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'Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief:'Syed Ali Rizvi, M.B;B.S

Contact: syedrizvi555@gmail.com


Medical Education:

Sindh Medical College.Karachi Pakistan


Membership and Certification:

Member of Association of Physicians of Pakistani Descent of North America.2017- Present

Member of Pakistan Medical Council.2007-Present

Overview

The Coronavirus disease-2019 (COVID-19), is caused by severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2). SARS-CoV-2 forms a distinct lineage with Bat-SARS-like coronaviruses . The virus is closely related (96.3%) to bat coronavirus RaTG13, based on phylogenetic analysis, that belong to the order Nidovirales, family Coronaviridae, genus Betacoronavirus, and subgenus Sarbecovirus [1]. Coronaviruses are enveloped, single-stranded RNA viruses that can infect a wide range of hosts including avian, wild, domestic mammalian species, and humans. Coronaviruses are well known for their ability to mutate rapidly, alter tissue tropism, cross the species barrier, and adapt to different epidemiological situations.[2] Six human coronaviruses have been reported since the 1960s; OC43, 229E, NL63, HKU1, severe acute respiratory syndrome coronavirus (SARS-CoV) and Middle East respiratory syndrome coronavirus (MERS-CoV. First case of COVID-19 was reported in Wuhan, Hubei province, China, in December 2019, associated with the Huanan Seafood Wholesale Market. On March 11, 2020 the Novel Coronavirus Disease, COVID-19, was declared a pandemic by the World Health Organization


Taxonomy


  • SARS-CoV-2 belong to the order nidovirale, family coronaviridae.
  • Coronaviridae is classified into two subfamilies.
    • Torovirinae
    • Coronavirinae
  • Coronavirinae is further classified on the basis of phylogenetic analysis and genome structure into four genera:
    • Alpha coronavirus (αCoV).
    • Beta coronavirus (βCoV).
    • Gamma coronavirus (γCoV).
    • Delta coronavirus (δCoV), which contain 17, 12, 2, and 7 unique species, respectively (ICTV 2018).
  • CoV-2 falls under beta coronavirus.

https://www.wikidoc.org/index.php/File:Taxonomy_of_CoV-2.jpg


Biology

Structure

  • Coronaviruses are enveloped, icosahedral symmetric particles, approximately 80–220 nm in diameter containing a non-segmented, single-strand, positive-sense RNA genome of about 26–32 kb in size. [3]
  • Corona in Latin means crown, and this name was attributed to the virus due to the presence of spike projections from the virus envelope that give it the shape of a crown under the electron microscope.
  • Nido means nest and refers to the ability of the viruses of this order to make a nested set of subgenomic mRNA

Envelope

Structural Proteins

  • Spike (S) Protein
    • Cell entry of coronaviruses depends on binding of the viral spike (S) proteins to cellular receptors and on S protein priming by host cell proteases.
    • Early studies indicate that SARS-CoV-2 uses the SARS-CoV receptor angiotensin-converting enzyme 2 (ACE2) for entry and transmembrane protease serine 2 (TMPRSS2) for S protein priming.[4]
    • The spike (S) glycoprotein is a type I transmembrane glycoprotein that plays an important role in mediating viral infection.
    • The S proteins consist of two subunits, S1 and S2.
    • The S1 subunit binds the cellular receptor through its receptor-binding domain (RBD), followed by conformational changes in the S2 subunit, which allows the fusion peptide to insert into the host target cell membrane.[5]
  • Envelope (E) Protein
    • The CoV envelope (E) protein is a small, integral membrane protein involved in several aspects of the virus’ life cycle, such as assembly, budding, envelope formation, and pathogenesis.
    • Recent studies have expanded on its structural motifs and topology, its functions as an ion-channelling viroporin, and its interactions with both other CoV proteins and host cell proteins.
    • Recombinant CoVs lacking E exhibit significantly reduced viral titres, crippled viral maturation, or yield propagation incompetent progeny, demonstrating the importance of E in virus production and maturation.[6]
  • Membrane (M) Protein
    • The CoV membrane (M) protein is a component of the viral envelope that plays a central role in virus morphogenesis and assembly via its interactions with other viral proteins.
    • M is located among the S proteins in the virus envelope along with small amounts of E and is the primary driver of the virus budding process.
    • During assembly of the authentic virion M interacts with itself, with the nucleocapsid protein N, with E and with the S protein.
    • The M protein has dominant cellular immunogenicity and elicits a strong humoral response which suggests it could serve as a potential target in vaccine design.[7] [8]
  • Nucleocapsid (N) Protein
    • The primary function of the nucleocapsid (N) protein is to package the viral RNA genome within the viral envelope into a ribonucleoprotein (RNP) complex called the capsid.
    • Ribonucleocapsid packaging is a fundamental part of viral self-assembly and replication.
    • Additionally, the N-protein of the SARS-CoV-2 affects host cell responses and may serve regulatory roles during its viral life cycle.

Corona Virus Life Cycle:

Attachment and Entry:

  • The attachment of the virion to the host cell is associated with the interactions between the S protein and its receptor.
  • The sites of receptor binding domains (RBD) within the S1 region of a coronavirus (SARS-CoV-2) S protein is at the C Terminus.[9]
  • SARS-CoV use angiotensin-converting enzyme 2 (ACE2) as their receptor[10]
  • After binding to the receptor, the virus next step is to gain access to the host cell cytosol.
  • This is generally done by cathepsin,TMPRRS2 or some other protease. This is followed by fusion of the viral and cellular membranes.
  • S protein cleavage occurs at two sites within the S2 portion of the protein, with the first cleavage important for separating the RBD (Receptor binding domain) and fusion domains of the S protein [11] and the second for exposing the fusion peptide (cleavage at S2′).
  • Fusion occurs within acidified endosomes.
  • Cleavage at S2′ exposes a fusion peptide that inserts into the membrane, which is followed by joining of two heptad repeats in S2 forming an antiparallel six-helix bundle[12].The formation of this bundle allows for the mixing of viral and cellular membranes, resulting in fusion and ultimately release of the viral genome into the cytoplasm.

RNA Replicase Protein Expression:

  • The next step in the coronavirus lifecycle is translation and assembly of the viral replicase complexes from the virion genomic RNA.


Replication and Transcription:

  • The translation and assembly of the viral replicase complexes is followed by viral RNA synthesis.
  • Viral RNA synthesis produces both genomic and sub-genomic RNAs. Sub-genomic RNAs serve as mRNAs for the structural and accessory genes which reside downstream of the replicase polyproteins. All positive-sense sub-genomic RNAs are 3′ co-terminal with the full-length viral genome and thus form a set of nested RNAs, a distinctive property of the order Nidovirales. Both genomic and sub-genomic RNAs are produced through negative-strand intermediates. These negative-strand intermediates are only about 1 % as abundant as their positive-sense counterparts and contain both poly-uridylate and anti-leader sequences.[13]

Tropism

  • Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) preferentially infects cells in the respiratory tract[14] .
  • SARS-CoV-2 can be detected in multiple organs, including the lungs, heart, liver, brain, pharynx and kidneys.[15]
  • In a study, it shows that highest levels of SARS-CoV-2 copies per cell were detected in the respiratory tract, and lower levels were detected the kidneys, liver, heart, brain, and blood. These findings indicate a broad organotropism of SARS-CoV-2.[16]

Natural Reservoir


References

Taxonomy[edit | edit source]

Insert full Linnaean taxonomy here

Biology[edit | edit source]

Structure[edit | edit source]

Tropism[edit | edit source]

Natural Reservoir[edit | edit source]

References

Post heart transplant Arrhythmia's


Overview

Historical Perspective

[Disease name] was first discovered by [name of scientist], a [nationality + occupation], in [year]/during/following [event].

The association between [important risk factor/cause] and [disease name] was made in/during [year/event].

In [year], [scientist] was the first to discover the association between [risk factor] and the development of [disease name].

In [year], [gene] mutations were first implicated in the pathogenesis of [disease name].

There have been several outbreaks of [disease name], including -----.

In [year], [diagnostic test/therapy] was developed by [scientist] to treat/diagnose [disease name].


Primary (idiopathic) is when the disorder is not a related medical condition, or Secondary (iatrogenic) is when side effects of medications, neurological or developmental disorders are causing the behavior.8 Primary bruxism is further divided into two types: awake and sleep bruxism. Clenching or grinding of the teeth is a common activity that can occur both during the day and at night.

Awake bruxism happens during the day with clenching being more prominent. It is defined as awareness of jaw clenching and appears to be semi-voluntary. It is usually correlated with high anxiety and stress. Awake bruxism is relatively common involving 20% of the adult population and 18% of children. It effects females more than males.1 Awake bruxism symptoms usually worsen throughout the day. Clenching during the day increases the risks of clenching or grinding at night.

Sleep bruxism occurs at night while sleeping with grinding being more prominent. It is defined as a sleep-related movement and is involuntary. It occurs in about 8%-10% of the population, with a lack of awareness from about 80% of the bruxers.; It effects both males and females equally.1,8 Sleep bruxism symptoms are usually worse in the morning, especially upon waking, and improve during the day.

One study reported sleep arousals induced sensory stimulation, which triggered episodes of sleep bruxism. Sleep arousals are a sudden change in the depth of the sleep stage and may also be accompanied by increased heart rate, respiratory changes and muscular activity, such as leg movements. It has been shown the majority (86%) of sleep bruxism episodes occur during periods of sleep arousal as a person goes from a deeper stage of sleep to a lighter stage of sleep.9==Classification==


There is no established system for the classification of [disease name].

OR

[Disease name] may be classified according to [classification method] into [number] subtypes/groups: [group1], [group2], [group3], and [group4].

OR

[Disease name] may be classified into [large number > 6] subtypes based on [classification method 1], [classification method 2], and [classification method 3]. [Disease name] may be classified into several subtypes based on [classification method 1], [classification method 2], and [classification method 3].

OR

Based on the duration of symptoms, [disease name] may be classified as either acute or chronic.

OR

If the staging system involves specific and characteristic findings and features: According to the [staging system + reference], there are [number] stages of [malignancy name] based on the [finding1], [finding2], and [finding3]. Each stage is assigned a [letter/number1] and a [letter/number2] that designate the [feature1] and [feature2].

OR

The staging of [malignancy name] is based on the [staging system].

OR

There is no established system for the staging of [malignancy name].

Pathophysiology

The exact pathogenesis of [disease name] is not fully understood.

OR

It is thought that [disease name] is the result of / is mediated by / is produced by / is caused by either [hypothesis 1], [hypothesis 2], or [hypothesis 3].

OR

[Pathogen name] is usually transmitted via the [transmission route] route to the human host.

OR

Following transmission/ingestion, the [pathogen] uses the [entry site] to invade the [cell name] cell.

OR

[Disease or malignancy name] arises from [cell name]s, which are [cell type] cells that are normally involved in [function of cells].

OR

The progression to [disease name] usually involves the [molecular pathway].

OR

The pathophysiology of [disease/malignancy] depends on the histological subtype.

Causes

Disease name] may be caused by [cause1], [cause2], or [cause3].

OR

Common causes of [disease] include [cause1], [cause2], and [cause3].

OR

The most common cause of [disease name] is [cause 1]. Less common causes of [disease name] include [cause 2], [cause 3], and [cause 4].

OR

The cause of [disease name] has not been identified. To review risk factors for the development of [disease name], click here.

Differentiating ((Page name)) from other Diseases

[Disease name] must be differentiated from other diseases that cause [clinical feature 1], [clinical feature 2], and [clinical feature 3], such as [differential dx1], [differential dx2], and [differential dx3].

OR

[Disease name] must be differentiated from [[differential dx1], [differential dx2], and [differential dx3].

Epidemiology and Demographics

The incidence/prevalence of [disease name] is approximately [number range] per 100,000 individuals worldwide.

OR

In [year], the incidence/prevalence of [disease name] was estimated to be [number range] cases per 100,000 individuals worldwide.

OR

In [year], the incidence of [disease name] is approximately [number range] per 100,000 individuals with a case-fatality rate of [number range]%.

Patients of all age groups may develop [disease name].

OR

The incidence of [disease name] increases with age; the median age at diagnosis is [#] years.

OR

[Disease name] commonly affects individuals younger than/older than [number of years] years of age.

OR

[Chronic disease name] is usually first diagnosed among [age group].

OR

[Acute disease name] commonly affects [age group].

There is no racial predilection to [disease name].

OR

[Disease name] usually affects individuals of the [race 1] race. [Race 2] individuals are less likely to develop [disease name].

[Disease name] affects men and women equally.

OR

[Gender 1] are more commonly affected by [disease name] than [gender 2]. The [gender 1] to [gender 2] ratio is approximately [number > 1] to 1.

The majority of [disease name] cases are reported in [geographical region].

OR

[Disease name] is a common/rare disease that tends to affect [patient population 1] and [patient population 2].

Risk Factors

There are no established risk factors for [disease name].

OR

The most potent risk factor in the development of [disease name] is [risk factor 1]. Other risk factors include [risk factor 2], [risk factor 3], and [risk factor 4].

OR

Common risk factors in the development of [disease name] include [risk factor 1], [risk factor 2], [risk factor 3], and [risk factor 4].

OR

Common risk factors in the development of [disease name] may be occupational, environmental, genetic, and viral.

Screening

There is insufficient evidence to recommend routine screening for [disease/malignancy].

OR

According to the [guideline name], screening for [disease name] is not recommended.

OR

According to the [guideline name], screening for [disease name] by [test 1] is recommended every [duration] among patients with [condition 1], [condition 2], and [condition 3].

Natural History, Complications, and Prognosis

If left untreated, [#]% of patients with [disease name] may progress to develop [manifestation 1], [manifestation 2], and [manifestation 3].

OR

Common complications of [disease name] include [complication 1], [complication 2], and [complication 3].

OR

Prognosis is generally excellent/good/poor, and the 1/5/10-year mortality/survival rate of patients with [disease name] is approximately [#]%.

Diagnosis

Diagnostic Study of Choice

The diagnosis of [disease name] is made when at least [number] of the following [number] diagnostic criteria are met: [criterion 1], [criterion 2], [criterion 3], and [criterion 4].

OR

The diagnosis of [disease name] is based on the [criteria name] criteria, which include [criterion 1], [criterion 2], and [criterion 3].

OR

The diagnosis of [disease name] is based on the [definition name] definition, which includes [criterion 1], [criterion 2], and [criterion 3].

OR

There are no established criteria for the diagnosis of [disease name].

History and Symptoms

Acute or Chronic Pain

Fortunately, or unfortunately, bruxism aches and pains are a functional, healthy response. It is the body’s way of sending a message that something is not in sync and an adjustment needs to occur. Any injury to the body causes other muscles, ligaments or tendons to overcompensate for the injury. Over time, those compensations also become weak and unproductive. Common aches or pains can progress from mild to severe depending on the aggressiveness and repetitiveness of the bruxing.

Any of these pains can be acute (comes and goes) or chronic (comes but never goes). Teeth sensitivity can be very specific or generalized. Jaw pain can be from the muscles or joints and can feel over-worn, fatigued, stiff or throbbing. Headaches can be in the morning or night, constant or fluctuating and can range from a slight dull pain to an intense migraine. Cheeks can feel tired, worn or sore when chewing. The TMJ can have inflammation, become locked or have limited opening of the mouth. Earache pain can feel like a dull pain or an intense shooting pain leading into the ear. Neck and shoulder pain can feel dull, stiff, achy or intense.47

When grinding with the anterior teeth, there may not be any pain beyond those specific teeth. But when grinding the posterior teeth, the masseter and temporalis muscles are more involved, which can create more facial and head pain.4 Myalgia may worsen during function, along with tenderness on palpation.16

Sensitivity of the Teeth

Sensitivity can be localized, generalized, constant or sporadic. One of the first symptoms of bruxism is hot and cold sensitivity to the teeth. This is caused by the flexing that occurs when teeth are ground from side to side. Teeth were not designed to flex, so they deteriorate at the areas of bending above the gingiva.4 This area can become very sensitive with abfractions developing at the roots and causing receding gingiva. Many times, patients do not know which exact tooth is causing the sensitivity, or even if it is maxillary or mandibular. When there are not obvious signs of bruxism, treatment is usually desensitizing toothpaste, which temporarily resolves the problem.

Sensitivity related bruxism can be challenging to diagnose. The thinning of enamel can cause underlying dentinal sensitivity. The tooth may acclimate to the new conditions. Additional enamel loss and re-acclimation may lead to the “coming and going” symptoms of sensitivity.

Jaw Pain

A common symptom is pain in and around the TMJ. This pain is usually felt when opening and closing the mandible; however, it can also occur while the mandible is in the resting position. Discomfort can occur through hyperactivity, spasms or overworked muscles. As with any other muscle, when contracted for a long period of time, the muscle fibers start to present fatigue or inflammation that produce the pain. Overt tissue damage, injury or trauma and overloading stress of the jaw muscles and TMJ during bruxism can activate nociceptors (receptors for pain stimulated by various kinds of tissue injury and pain).4,47 These conditions can cause inflammation of the stressed areas and coincidentally cause pain as well. This type of pain is characterized as a fairly prolonged, deep dull ache, often similar to the discomfort associated with a nagging headache. A sharp, brief shooting pain or a feeling of numbness in the orofacial area is another symptom. Bruxism can cause stiffness in the TMJ and masseter muscles.

TMJ Discomfort

Changes that happen in the TMJ arise from pathologic processes more than physiologic adaptation, which can cause the entire dentition to undergo a continuous adaptation to functional wear. Adjustments in the orofacial region are constantly being supported by the wear caused by bruxing.48 Repetitive overloading of the TMJ through bruxing can be a factor in osteoarthritis. Bruxing pain in the TMJ area includes the retrodiscal pad, synovial membranes of the joint capsule and collateral ligaments of the disc-condyle complex.48 Bruxism can cause nightly bruising of the TMJ with a dislocated disk and can sometimes function as a sustaining factor in the cycle of pain and muscle tightness.48

Patients with Temporomandibular Disorder (TMD) often hear clicking, popping, or grating noises in their TMJ.4,47,48 The clicking noise commonly heard and palpated during opening or closing is a result of this disc slipping out of place, sticking, or malfunctioning. Although some clicking and popping sounds in the TMJ can be normal and insignificant, when the sound is grating or gravel like, the joint and disc may be breaking down (degenerating). This requires a more involved evaluation. Clicking sounds may occur in one or both joints when the bony joint and disc movement are not coordinated. The click may occur when opening or closing and with lateral movements as well. The jaw may shift to the side and may catch or lock during any of its movements.49 Although the disc can quickly reorient itself and normal jaw function can be restored, sometimes this problem can worsen. The disc wear can continue and result in a more severe displacement. Occasionally, this can be a painful event that results in a reflex contraction of the chewing muscles which locks the TMJ in an open dislocated position. This is referred to as an open lock.49 When these situations arise, a referral to a TMD dental specialist would be most beneficial for the patient.

Muscles, Neck Pain and Headaches

Since the masseter muscle is considered one of the strongest single muscles in the body, when the muscle is worn and fatigued from bruxing, it can cause localized and referred pain.44,50 The masseter alone can be inflamed and fatigued, causing localized pain. The masseter attachment trigger points at the upper superficial layer can have referred pain points to the mandible, teeth and gingival area. The mass superficial layer can also have referred pain patterns to the mandible, teeth and gingival area. The attachment trigger point of the lower superficial layer refers pain to the mandible and above the eyebrows. The trigger point of the upper posterior deep layer below the TMJ refers pain to the ear area.50,51,52

Even if muscle pain does not occur, muscle hypertrophy can result.16 Bruxism involves excessive muscle use, which can lead to enlargement of the facial muscles. In long-term bruxers this enlargement can cause a square jaw appearance.53

Bruxism may lead to chronic headaches, although the correlation is not entirely clear. One perspective could be the aches and pains are from disturbed circulation in the muscles. Another suggestion is the tightening of the entire mandible and face during bruxing can cause headaches.5,51 Bruxers are three times more likely to experience headaches than non-bruxers.18 The use and tightness of the masseter muscles and the clamping down of the dentition connects with the neck muscles causing neck pain.52

Ear Pain

Ear pain can be a side effect of bruxism. It can either be referred or real. Since bruxism can cause TMJ issues, and the TMJ is located very close to the ear canal, pain in this area can be experienced.5


The majority of patients with [disease name] are asymptomatic.

OR

The hallmark of [disease name] is [finding]. A positive history of [finding 1] and [finding 2] is suggestive of [disease name]. The most common symptoms of [disease name] include [symptom 1], [symptom 2], and [symptom 3]. Common symptoms of [disease] include [symptom 1], [symptom 2], and [symptom 3]. Less common symptoms of [disease name] include [symptom 1], [symptom 2], and [symptom 3].

Physical Examination

Patients with [disease name] usually appear [general appearance]. Physical examination of patients with [disease name] is usually remarkable for [finding 1], [finding 2], and [finding 3].

OR

Common physical examination findings of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

The presence of [finding(s)] on physical examination is diagnostic of [disease name].

OR

The presence of [finding(s)] on physical examination is highly suggestive of [disease name].

Laboratory Findings

An elevated/reduced concentration of serum/blood/urinary/CSF/other [lab test] is diagnostic of [disease name].

OR

Laboratory findings consistent with the diagnosis of [disease name] include [abnormal test 1], [abnormal test 2], and [abnormal test 3].

OR

[Test] is usually normal among patients with [disease name].

OR

Some patients with [disease name] may have elevated/reduced concentration of [test], which is usually suggestive of [progression/complication].

OR

There are no diagnostic laboratory findings associated with [disease name].

Electrocardiogram

There are no ECG findings associated with [disease name].

OR

An ECG may be helpful in the diagnosis of [disease name]. Findings on an ECG suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

X-ray

There are no x-ray findings associated with [disease name].

OR

An x-ray may be helpful in the diagnosis of [disease name]. Findings on an x-ray suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

There are no x-ray findings associated with [disease name]. However, an x-ray may be helpful in the diagnosis of complications of [disease name], which include [complication 1], [complication 2], and [complication 3].

Echocardiography or Ultrasound

There are no echocardiography/ultrasound findings associated with [disease name].

OR

Echocardiography/ultrasound may be helpful in the diagnosis of [disease name]. Findings on an echocardiography/ultrasound suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

There are no echocardiography/ultrasound findings associated with [disease name]. However, an echocardiography/ultrasound may be helpful in the diagnosis of complications of [disease name], which include [complication 1], [complication 2], and [complication 3].

CT scan

There are no CT scan findings associated with [disease name].

OR

[Location] CT scan may be helpful in the diagnosis of [disease name]. Findings on CT scan suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

There are no CT scan findings associated with [disease name]. However, a CT scan may be helpful in the diagnosis of complications of [disease name], which include [complication 1], [complication 2], and [complication 3].

MRI

There are no MRI findings associated with [disease name].

OR

[Location] MRI may be helpful in the diagnosis of [disease name]. Findings on MRI suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

There are no MRI findings associated with [disease name]. However, a MRI may be helpful in the diagnosis of complications of [disease name], which include [complication 1], [complication 2], and [complication 3].

Other Imaging Findings

There are no other imaging findings associated with [disease name].

OR

[Imaging modality] may be helpful in the diagnosis of [disease name]. Findings on an [imaging modality] suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

Other Diagnostic Studies

There are no other diagnostic studies associated with [disease name].

OR

[Diagnostic study] may be helpful in the diagnosis of [disease name]. Findings suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

Other diagnostic studies for [disease name] include [diagnostic study 1], which demonstrates [finding 1], [finding 2], and [finding 3], and [diagnostic study 2], which demonstrates [finding 1], [finding 2], and [finding 3].

Treatment

Medical Therapy

There is no treatment for [disease name]; the mainstay of therapy is supportive care.

OR

Supportive therapy for [disease name] includes [therapy 1], [therapy 2], and [therapy 3].

OR

The majority of cases of [disease name] are self-limited and require only supportive care.

OR

[Disease name] is a medical emergency and requires prompt treatment.

OR

The mainstay of treatment for [disease name] is [therapy].

OR The optimal therapy for [malignancy name] depends on the stage at diagnosis.

OR

[Therapy] is recommended among all patients who develop [disease name].

OR

Pharmacologic medical therapy is recommended among patients with [disease subclass 1], [disease subclass 2], and [disease subclass 3].

OR

Pharmacologic medical therapies for [disease name] include (either) [therapy 1], [therapy 2], and/or [therapy 3].

OR

Empiric therapy for [disease name] depends on [disease factor 1] and [disease factor 2].

OR

Patients with [disease subclass 1] are treated with [therapy 1], whereas patients with [disease subclass 2] are treated with [therapy 2].

Surgery

Surgical intervention is not recommended for the management of [disease name].

OR

Surgery is not the first-line treatment option for patients with [disease name]. Surgery is usually reserved for patients with either [indication 1], [indication 2], and [indication 3]

OR

The mainstay of treatment for [disease name] is medical therapy. Surgery is usually reserved for patients with either [indication 1], [indication 2], and/or [indication 3].

OR

The feasibility of surgery depends on the stage of [malignancy] at diagnosis.

OR

Surgery is the mainstay of treatment for [disease or malignancy].

Primary Prevention

There are no established measures for the primary prevention of [disease name].

OR

There are no available vaccines against [disease name].

OR

Effective measures for the primary prevention of [disease name] include [measure1], [measure2], and [measure3].

OR

[Vaccine name] vaccine is recommended for [patient population] to prevent [disease name]. Other primary prevention strategies include [strategy 1], [strategy 2], and [strategy 3].

Secondary Prevention

There are no established measures for the secondary prevention of [disease name].

OR

Effective measures for the secondary prevention of [disease name] include [strategy 1], [strategy 2], and [strategy 3].

References

BRUXISM :

Overview

Bruxism is a condition in which you grind, gnash or clench your teeth. People may unconsciously clench their teeth when they are awake (awake bruxism) or clench or grind them during sleep (sleep bruxism).

Sleep bruxism is considered a sleep-related movement disorder. People who clench or grind their teeth (brux) during sleep are more likely to have other sleep disorders, such as snoring and pauses in breathing (sleep apnea).

Mild bruxism may not require treatment. However, in some people, bruxism can be frequent and severe enough to lead to jaw disorders, headaches, damaged teeth and other problems.

Because you may have sleep bruxism and be unaware of it until complications develop, it's important to know the signs and symptoms of bruxism and to seek regular dental care.



Historical Perspective

In the beginning of the twentieth century, Moritz Karolyi, a Viennese dentist, described bruxism as “traumatic neuralgia” and stated “it was the cause of a periodontal condition called pyorrhea (periodontitis).” In 1907 the French term “Bruxamine” was introduced by Marie and Pietkiewicz. In 1931 Bertrand Frohman, MD created the term bruxism, which comes from the Greek expression “brychien odontas.”4 Sigmund Freud, scholar and psychiatrist, also had a theory concerning bruxing in the oral cavity. He claimed it to be a prime significance in the psychosexual development and behavior of the individual. Between 1966 and 2007 research and treatment were focused on occlusal adjustments and oral splints. During the 1960s, a periodontist, Sigurd Peder, DDS, PhD,5 promoted the theory that occlusal factors were responsible for bruxism. While therapy centered on the removal of occlusal interference remained unsatisfactory, behavioral approaches in research also declined during 1966-1986.


[Disease name] was first discovered by [name of scientist], a [nationality + occupation], in [year]/during/following [event].

The association between [important risk factor/cause] and [disease name] was made in/during [year/event].

In [year], [scientist] was the first to discover the association between [risk factor] and the development of [disease name].

In [year], [gene] mutations were first implicated in the pathogenesis of [disease name].

There have been several outbreaks of [disease name], including -----.

In [year], [diagnostic test/therapy] was developed by [scientist] to treat/diagnose [disease name].

Classification

Bruxism may be classified into two catogeries :

Primary (idiopathic) is when the disorder is not a related medical condition, or Secondary (iatrogenic) is when side effects of medications, neurological or developmental disorders are causing the behavior.8 Primary bruxism is further divided into two types: awake and sleep bruxism. Clenching or grinding of the teeth is a common activity that can occur both during the day and at night.

Awake bruxism happens during the day with clenching being more prominent. It is defined as awareness of jaw clenching and appears to be semi-voluntary. It is usually correlated with high anxiety and stress. Awake bruxism is relatively common involving 20% of the adult population and 18% of children. It effects females more than males.1 Awake bruxism symptoms usually worsen throughout the day. Clenching during the day increases the risks of clenching or grinding at night.

Sleep bruxism occurs at night while sleeping with grinding being more prominent. It is defined as a sleep-related movement and is involuntary. It occurs in about 8%-10% of the population, with a lack of awareness from about 80% of the bruxers.; It effects both males and females equally.1,8 Sleep bruxism symptoms are usually worse in the morning, especially upon waking, and improve during the day.

One study reported sleep arousals induced sensory stimulation, which triggered episodes of sleep bruxism. Sleep arousals are a sudden change in the depth of the sleep stage and may also be accompanied by increased heart rate, respiratory changes and muscular activity, such as leg movements. It has been shown the majority (86%) of sleep bruxism episodes occur during periods of sleep arousal as a person goes from a deeper stage of sleep to a lighter stage of sleep.9



There is no established system for the classification of [disease name].

OR

[Disease name] may be classified according to [classification method] into [number] subtypes/groups: [group1], [group2], [group3], and [group4].

OR

[Disease name] may be classified into [large number > 6] subtypes based on [classification method 1], [classification method 2], and [classification method 3]. [Disease name] may be classified into several subtypes based on [classification method 1], [classification method 2], and [classification method 3].

OR

Based on the duration of symptoms, [disease name] may be classified as either acute or chronic.

OR

If the staging system involves specific and characteristic findings and features: According to the [staging system + reference], there are [number] stages of [malignancy name] based on the [finding1], [finding2], and [finding3]. Each stage is assigned a [letter/number1] and a [letter/number2] that designate the [feature1] and [feature2].

OR

The staging of [malignancy name] is based on the [staging system].

OR

There is no established system for the staging of [malignancy name].

Pathophysiology

The exact pathogenesis of [disease name] is not fully understood.

OR

It is thought that [disease name] is the result of / is mediated by / is produced by / is caused by either [hypothesis 1], [hypothesis 2], or [hypothesis 3].

OR

[Pathogen name] is usually transmitted via the [transmission route] route to the human host.

OR

Following transmission/ingestion, the [pathogen] uses the [entry site] to invade the [cell name] cell.

OR

[Disease or malignancy name] arises from [cell name]s, which are [cell type] cells that are normally involved in [function of cells].

OR

The progression to [disease name] usually involves the [molecular pathway].

OR

The pathophysiology of [disease/malignancy] depends on the histological subtype.

Causes

Disease name] may be caused by [cause1], [cause2], or [cause3].

OR

Common causes of [disease] include [cause1], [cause2], and [cause3].

OR

The most common cause of [disease name] is [cause 1]. Less common causes of [disease name] include [cause 2], [cause 3], and [cause 4].

OR

The cause of [disease name] has not been identified. To review risk factors for the development of [disease name], click here.

Differentiating ((Page name)) from other Diseases

[Disease name] must be differentiated from other diseases that cause [clinical feature 1], [clinical feature 2], and [clinical feature 3], such as [differential dx1], [differential dx2], and [differential dx3].

OR

[Disease name] must be differentiated from [[differential dx1], [differential dx2], and [differential dx3].

Epidemiology and Demographics

The incidence/prevalence of [disease name] is approximately [number range] per 100,000 individuals worldwide.

OR

In [year], the incidence/prevalence of [disease name] was estimated to be [number range] cases per 100,000 individuals worldwide.

OR

In [year], the incidence of [disease name] is approximately [number range] per 100,000 individuals with a case-fatality rate of [number range]%.

Patients of all age groups may develop [disease name].

OR

The incidence of [disease name] increases with age; the median age at diagnosis is [#] years.

OR

[Disease name] commonly affects individuals younger than/older than [number of years] years of age.

OR

[Chronic disease name] is usually first diagnosed among [age group].

OR

[Acute disease name] commonly affects [age group].

There is no racial predilection to [disease name].

OR

[Disease name] usually affects individuals of the [race 1] race. [Race 2] individuals are less likely to develop [disease name].

[Disease name] affects men and women equally.

OR

[Gender 1] are more commonly affected by [disease name] than [gender 2]. The [gender 1] to [gender 2] ratio is approximately [number > 1] to 1.

The majority of [disease name] cases are reported in [geographical region].

OR

[Disease name] is a common/rare disease that tends to affect [patient population 1] and [patient population 2].

Risk Factors

There are no established risk factors for [disease name].

OR

The most potent risk factor in the development of [disease name] is [risk factor 1]. Other risk factors include [risk factor 2], [risk factor 3], and [risk factor 4].

OR

Common risk factors in the development of [disease name] include [risk factor 1], [risk factor 2], [risk factor 3], and [risk factor 4].

OR

Common risk factors in the development of [disease name] may be occupational, environmental, genetic, and viral.

Screening

There is insufficient evidence to recommend routine screening for [disease/malignancy].

OR

According to the [guideline name], screening for [disease name] is not recommended.

OR

According to the [guideline name], screening for [disease name] by [test 1] is recommended every [duration] among patients with [condition 1], [condition 2], and [condition 3].

Natural History, Complications, and Prognosis

If left untreated, [#]% of patients with [disease name] may progress to develop [manifestation 1], [manifestation 2], and [manifestation 3].

OR

Common complications of [disease name] include [complication 1], [complication 2], and [complication 3].

OR

Prognosis is generally excellent/good/poor, and the 1/5/10-year mortality/survival rate of patients with [disease name] is approximately [#]%.

Diagnosis

Diagnostic Study of Choice

Diagnosis initially starts with the patient’s concerns during a dental appointment. The common chief complaint is usually some level of pain, whether it is persistent or inconsistent, from slight sensitivity to intense pain. Patients will usually state generalized or localized hypersensitivity or pain in their teeth and/or jaw. The patient may also become aware of their clenching habits during times of stress or depression. They will sometimes know exactly which tooth. Other times they will know the area but are unable to pinpoint the exact tooth.

After determining decay is not the issue, diagnosing wear facets could be the confirmation of teeth grinding. Symptoms related to the mandible or face are: pain, soreness, tiredness, achiness, popping of the mandible upon opening and closing, tightness or stiffness usually from the pressure and overuse of the masseter muscles or TMJ. Headaches are another common symptom, especially when it is experienced after wakening. These headaches can be dull or intense, sometimes leading to migraines.17

Over the years, the accumulated toll of bruxing can produce a wide range of damage or oral changes. Duration, frequency and intensity of bruxing significantly contributes to the resulting effect.

The diagnosis of [disease name] is made when at least [number] of the following [number] diagnostic criteria are met: [criterion 1], [criterion 2], [criterion 3], and [criterion 4].

OR

The diagnosis of [disease name] is based on the [criteria name] criteria, which include [criterion 1], [criterion 2], and [criterion 3].

OR

The diagnosis of [disease name] is based on the [definition name] definition, which includes [criterion 1], [criterion 2], and [criterion 3].

OR

There are no established criteria for the diagnosis of [disease name].

History and Symptoms

Acute or Chronic Pain

Fortunately, or unfortunately, bruxism aches and pains are a functional, healthy response. It is the body’s way of sending a message that something is not in sync and an adjustment needs to occur. Any injury to the body causes other muscles, ligaments or tendons to overcompensate for the injury. Over time, those compensations also become weak and unproductive. Common aches or pains can progress from mild to severe depending on the aggressiveness and repetitiveness of the bruxing.

Any of these pains can be acute (comes and goes) or chronic (comes but never goes). Teeth sensitivity can be very specific or generalized. Jaw pain can be from the muscles or joints and can feel over-worn, fatigued, stiff or throbbing. Headaches can be in the morning or night, constant or fluctuating and can range from a slight dull pain to an intense migraine. Cheeks can feel tired, worn or sore when chewing. The TMJ can have inflammation, become locked or have limited opening of the mouth. Earache pain can feel like a dull pain or an intense shooting pain leading into the ear. Neck and shoulder pain can feel dull, stiff, achy or intense.47

When grinding with the anterior teeth, there may not be any pain beyond those specific teeth. But when grinding the posterior teeth, the masseter and temporalis muscles are more involved, which can create more facial and head pain.4 Myalgia may worsen during function, along with tenderness on palpation.16

Sensitivity of the Teeth

Sensitivity can be localized, generalized, constant or sporadic. One of the first symptoms of bruxism is hot and cold sensitivity to the teeth. This is caused by the flexing that occurs when teeth are ground from side to side. Teeth were not designed to flex, so they deteriorate at the areas of bending above the gingiva.4 This area can become very sensitive with abfractions developing at the roots and causing receding gingiva. Many times, patients do not know which exact tooth is causing the sensitivity, or even if it is maxillary or mandibular. When there are not obvious signs of bruxism, treatment is usually desensitizing toothpaste, which temporarily resolves the problem.

Sensitivity related bruxism can be challenging to diagnose. The thinning of enamel can cause underlying dentinal sensitivity. The tooth may acclimate to the new conditions. Additional enamel loss and re-acclimation may lead to the “coming and going” symptoms of sensitivity.

Jaw Pain

A common symptom is pain in and around the TMJ. This pain is usually felt when opening and closing the mandible; however, it can also occur while the mandible is in the resting position. Discomfort can occur through hyperactivity, spasms or overworked muscles. As with any other muscle, when contracted for a long period of time, the muscle fibers start to present fatigue or inflammation that produce the pain. Overt tissue damage, injury or trauma and overloading stress of the jaw muscles and TMJ during bruxism can activate nociceptors (receptors for pain stimulated by various kinds of tissue injury and pain).4,47 These conditions can cause inflammation of the stressed areas and coincidentally cause pain as well. This type of pain is characterized as a fairly prolonged, deep dull ache, often similar to the discomfort associated with a nagging headache. A sharp, brief shooting pain or a feeling of numbness in the orofacial area is another symptom. Bruxism can cause stiffness in the TMJ and masseter muscles.

TMJ Discomfort

Changes that happen in the TMJ arise from pathologic processes more than physiologic adaptation, which can cause the entire dentition to undergo a continuous adaptation to functional wear. Adjustments in the orofacial region are constantly being supported by the wear caused by bruxing.48 Repetitive overloading of the TMJ through bruxing can be a factor in osteoarthritis. Bruxing pain in the TMJ area includes the retrodiscal pad, synovial membranes of the joint capsule and collateral ligaments of the disc-condyle complex.48 Bruxism can cause nightly bruising of the TMJ with a dislocated disk and can sometimes function as a sustaining factor in the cycle of pain and muscle tightness.48

Patients with Temporomandibular Disorder (TMD) often hear clicking, popping, or grating noises in their TMJ.4,47,48 The clicking noise commonly heard and palpated during opening or closing is a result of this disc slipping out of place, sticking, or malfunctioning. Although some clicking and popping sounds in the TMJ can be normal and insignificant, when the sound is grating or gravel like, the joint and disc may be breaking down (degenerating). This requires a more involved evaluation. Clicking sounds may occur in one or both joints when the bony joint and disc movement are not coordinated. The click may occur when opening or closing and with lateral movements as well. The jaw may shift to the side and may catch or lock during any of its movements.49 Although the disc can quickly reorient itself and normal jaw function can be restored, sometimes this problem can worsen. The disc wear can continue and result in a more severe displacement. Occasionally, this can be a painful event that results in a reflex contraction of the chewing muscles which locks the TMJ in an open dislocated position. This is referred to as an open lock.49 When these situations arise, a referral to a TMD dental specialist would be most beneficial for the patient.

Muscles, Neck Pain and Headaches

Since the masseter muscle is considered one of the strongest single muscles in the body, when the muscle is worn and fatigued from bruxing, it can cause localized and referred pain.44,50 The masseter alone can be inflamed and fatigued, causing localized pain. The masseter attachment trigger points at the upper superficial layer can have referred pain points to the mandible, teeth and gingival area. The mass superficial layer can also have referred pain patterns to the mandible, teeth and gingival area. The attachment trigger point of the lower superficial layer refers pain to the mandible and above the eyebrows. The trigger point of the upper posterior deep layer below the TMJ refers pain to the ear area.50,51,52

Even if muscle pain does not occur, muscle hypertrophy can result.16 Bruxism involves excessive muscle use, which can lead to enlargement of the facial muscles. In long-term bruxers this enlargement can cause a square jaw appearance.53

Bruxism may lead to chronic headaches, although the correlation is not entirely clear. One perspective could be the aches and pains are from disturbed circulation in the muscles. Another suggestion is the tightening of the entire mandible and face during bruxing can cause headaches.5,51 Bruxers are three times more likely to experience headaches than non-bruxers.18 The use and tightness of the masseter muscles and the clamping down of the dentition connects with the neck muscles causing neck pain.52

Ear Pain

Ear pain can be a side effect of bruxism. It can either be referred or real. Since bruxism can cause TMJ issues, and the TMJ is located very close to the ear canal, pain in this area can be experienced.5




The majority of patients with [disease name] are asymptomatic.

OR

The hallmark of [disease name] is [finding]. A positive history of [finding 1] and [finding 2] is suggestive of [disease name]. The most common symptoms of [disease name] include [symptom 1], [symptom 2], and [symptom 3]. Common symptoms of [disease] include [symptom 1], [symptom 2], and [symptom 3]. Less common symptoms of [disease name] include [symptom 1], [symptom 2], and [symptom 3].

Physical Examination

Patients with [disease name] usually appear [general appearance]. Physical examination of patients with [disease name] is usually remarkable for [finding 1], [finding 2], and [finding 3].

OR

Common physical examination findings of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

The presence of [finding(s)] on physical examination is diagnostic of [disease name].

OR

The presence of [finding(s)] on physical examination is highly suggestive of [disease name].

Laboratory Findings

An elevated/reduced concentration of serum/blood/urinary/CSF/other [lab test] is diagnostic of [disease name].

OR

Laboratory findings consistent with the diagnosis of [disease name] include [abnormal test 1], [abnormal test 2], and [abnormal test 3].

OR

[Test] is usually normal among patients with [disease name].

OR

Some patients with [disease name] may have elevated/reduced concentration of [test], which is usually suggestive of [progression/complication].

OR

There are no diagnostic laboratory findings associated with [disease name].

Electrocardiogram

There are no ECG findings associated with [disease name].

OR

An ECG may be helpful in the diagnosis of [disease name]. Findings on an ECG suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

X-ray

There are no x-ray findings associated with [disease name].

OR

An x-ray may be helpful in the diagnosis of [disease name]. Findings on an x-ray suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

There are no x-ray findings associated with [disease name]. However, an x-ray may be helpful in the diagnosis of complications of [disease name], which include [complication 1], [complication 2], and [complication 3].

Echocardiography or Ultrasound

There are no echocardiography/ultrasound findings associated with [disease name].

OR

Echocardiography/ultrasound may be helpful in the diagnosis of [disease name]. Findings on an echocardiography/ultrasound suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

There are no echocardiography/ultrasound findings associated with [disease name]. However, an echocardiography/ultrasound may be helpful in the diagnosis of complications of [disease name], which include [complication 1], [complication 2], and [complication 3].

CT scan

There are no CT scan findings associated with [disease name].

OR

[Location] CT scan may be helpful in the diagnosis of [disease name]. Findings on CT scan suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

There are no CT scan findings associated with [disease name]. However, a CT scan may be helpful in the diagnosis of complications of [disease name], which include [complication 1], [complication 2], and [complication 3].

MRI

There are no MRI findings associated with [disease name].

OR

[Location] MRI may be helpful in the diagnosis of [disease name]. Findings on MRI suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

There are no MRI findings associated with [disease name]. However, a MRI may be helpful in the diagnosis of complications of [disease name], which include [complication 1], [complication 2], and [complication 3].

Other Imaging Findings

There are no other imaging findings associated with [disease name].

OR

[Imaging modality] may be helpful in the diagnosis of [disease name]. Findings on an [imaging modality] suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

Other Diagnostic Studies

There are no other diagnostic studies associated with [disease name].

OR

[Diagnostic study] may be helpful in the diagnosis of [disease name]. Findings suggestive of/diagnostic of [disease name] include [finding 1], [finding 2], and [finding 3].

OR

Other diagnostic studies for [disease name] include [diagnostic study 1], which demonstrates [finding 1], [finding 2], and [finding 3], and [diagnostic study 2], which demonstrates [finding 1], [finding 2], and [finding 3].

Treatment

Medical Therapy

There is no treatment for [disease name]; the mainstay of therapy is supportive care.

OR

Supportive therapy for [disease name] includes [therapy 1], [therapy 2], and [therapy 3].

OR

The majority of cases of [disease name] are self-limited and require only supportive care.

OR

[Disease name] is a medical emergency and requires prompt treatment.

OR

The mainstay of treatment for [disease name] is [therapy].

OR The optimal therapy for [malignancy name] depends on the stage at diagnosis.

OR

[Therapy] is recommended among all patients who develop [disease name].

OR

Pharmacologic medical therapy is recommended among patients with [disease subclass 1], [disease subclass 2], and [disease subclass 3].

OR

Pharmacologic medical therapies for [disease name] include (either) [therapy 1], [therapy 2], and/or [therapy 3].

OR

Empiric therapy for [disease name] depends on [disease factor 1] and [disease factor 2].

OR

Patients with [disease subclass 1] are treated with [therapy 1], whereas patients with [disease subclass 2] are treated with [therapy 2].

Surgery

Surgical intervention is not recommended for the management of [disease name].

OR

Surgery is not the first-line treatment option for patients with [disease name]. Surgery is usually reserved for patients with either [indication 1], [indication 2], and [indication 3]

OR

The mainstay of treatment for [disease name] is medical therapy. Surgery is usually reserved for patients with either [indication 1], [indication 2], and/or [indication 3].

OR

The feasibility of surgery depends on the stage of [malignancy] at diagnosis.

OR

Surgery is the mainstay of treatment for [disease or malignancy].

Primary Prevention

There are no established measures for the primary prevention of [disease name].

OR

There are no available vaccines against [disease name].

OR

Effective measures for the primary prevention of [disease name] include [measure1], [measure2], and [measure3].

OR

[Vaccine name] vaccine is recommended for [patient population] to prevent [disease name]. Other primary prevention strategies include [strategy 1], [strategy 2], and [strategy 3].

Secondary Prevention

There are no established measures for the secondary prevention of [disease name].

OR

Effective measures for the secondary prevention of [disease name] include [strategy 1], [strategy 2], and [strategy 3].

References

  1. Zhou, Peng; Yang, Xing-Lou; Wang, Xian-Guang; Hu, Ben; Zhang, Lei; Zhang, Wei; Si, Hao-Rui; Zhu, Yan; Li, Bei; Huang, Chao-Lin; Chen, Hui-Dong; Chen, Jing; Luo, Yun; Guo, Hua; Jiang, Ren-Di; Liu, Mei-Qin; Chen, Ying; Shen, Xu-Rui; Wang, Xi; Zheng, Xiao-Shuang; Zhao, Kai; Chen, Quan-Jiao; Deng, Fei; Liu, Lin-Lin; Yan, Bing; Zhan, Fa-Xian; Wang, Yan-Yi; Xiao, Geng-Fu; Shi, Zheng-Li (2020). "A pneumonia outbreak associated with a new coronavirus of probable bat origin". Nature. 579 (7798): 270–273. doi:10.1038/s41586-020-2012-7. ISSN 0028-0836.
  2. Decaro N, Mari V, Elia G, Addie DD, Camero M, Lucente MS, Martella V, Buonavoglia C (January 2010). "Recombinant canine coronaviruses in dogs, Europe". Emerging Infect. Dis. 16 (1): 41–7. doi:10.3201/eid1601.090726. PMC 2874359. PMID 20031041.
  3. Weiss SR, Navas-Martin S (December 2005). "Coronavirus pathogenesis and the emerging pathogen severe acute respiratory syndrome coronavirus". Microbiol. Mol. Biol. Rev. 69 (4): 635–64. doi:10.1128/MMBR.69.4.635-664.2005. PMC 1306801. PMID 16339739.
  4. Zhou, Peng; Yang, Xing-Lou; Wang, Xian-Guang; Hu, Ben; Zhang, Lei; Zhang, Wei; Si, Hao-Rui; Zhu, Yan; Li, Bei; Huang, Chao-Lin; Chen, Hui-Dong; Chen, Jing; Luo, Yun; Guo, Hua; Jiang, Ren-Di; Liu, Mei-Qin; Chen, Ying; Shen, Xu-Rui; Wang, Xi; Zheng, Xiao-Shuang; Zhao, Kai; Chen, Quan-Jiao; Deng, Fei; Liu, Lin-Lin; Yan, Bing; Zhan, Fa-Xian; Wang, Yan-Yi; Xiao, Geng-Fu; Shi, Zheng-Li (2020). "A pneumonia outbreak associated with a new coronavirus of probable bat origin". Nature. 579 (7798): 270–273. doi:10.1038/s41586-020-2012-7. ISSN 0028-0836.
  5. Nieva, José; Carrasco, Luis (2015). "Viroporins: Structures and functions beyond cell membrane permeabilization". Viruses. 7 (10): 5169–5171. doi:10.3390/v7102866. ISSN 1999-4915.
  6. Schoeman, Dewald; Fielding, Burtram C. (2019). "Coronavirus envelope protein: current knowledge". Virology Journal. 16 (1). doi:10.1186/s12985-019-1182-0. ISSN 1743-422X.
  7. Siu, Y. L.; Teoh, K. T.; Lo, J.; Chan, C. M.; Kien, F.; Escriou, N.; Tsao, S. W.; Nicholls, J. M.; Altmeyer, R.; Peiris, J. S. M.; Bruzzone, R.; Nal, B. (2008). "The M, E, and N Structural Proteins of the Severe Acute Respiratory Syndrome Coronavirus Are Required for Efficient Assembly, Trafficking, and Release of Virus-Like Particles". Journal of Virology. 82 (22): 11318–11330. doi:10.1128/JVI.01052-08. ISSN 0022-538X.
  8. Tooze J, Tooze S, Warren G (March 1984). "Replication of coronavirus MHV-A59 in sac- cells: determination of the first site of budding of progeny virions". Eur. J. Cell Biol. 33 (2): 281–93. PMID 6325194.
  9. Kubo H, Yamada YK, Taguchi F (September 1994). "Localization of neutralizing epitopes and the receptor-binding site within the amino-terminal 330 amino acids of the murine coronavirus spike protein". J. Virol. 68 (9): 5403–10. PMC 236940. PMID 7520090.
  10. Zhou, Peng; Yang, Xing-Lou; Wang, Xian-Guang; Hu, Ben; Zhang, Lei; Zhang, Wei; Si, Hao-Rui; Zhu, Yan; Li, Bei; Huang, Chao-Lin; Chen, Hui-Dong; Chen, Jing; Luo, Yun; Guo, Hua; Jiang, Ren-Di; Liu, Mei-Qin; Chen, Ying; Shen, Xu-Rui; Wang, Xi; Zheng, Xiao-Shuang; Zhao, Kai; Chen, Quan-Jiao; Deng, Fei; Liu, Lin-Lin; Yan, Bing; Zhan, Fa-Xian; Wang, Yan-Yi; Xiao, Geng-Fu; Shi, Zheng-Li (2020). "A pneumonia outbreak associated with a new coronavirus of probable bat origin". Nature. 579 (7798): 270–273. doi:10.1038/s41586-020-2012-7. ISSN 0028-0836.
  11. Belouzard S, Chu VC, Whittaker GR (April 2009). "Activation of the SARS coronavirus spike protein via sequential proteolytic cleavage at two distinct sites". Proc. Natl. Acad. Sci. U.S.A. 106 (14): 5871–6. doi:10.1073/pnas.0809524106. PMC 2660061. PMID 19321428.
  12. Knuhtsen S, Holst JJ, Schwartz TW, Jensen SL, Nielsen OV (May 1987). "The effect of gastrin-releasing peptide on the endocrine pancreas". Regul. Pept. 17 (5): 269–76. doi:10.1016/0167-0115(87)90284-9. PMID 2885899.
  13. Sethna PB, Hofmann MA, Brian DA (January 1991). "Minus-strand copies of replicating coronavirus mRNAs contain antileaders". J. Virol. 65 (1): 320–5. PMC 240520. PMID 1985203.
  14. Zou L, Ruan F, Huang M, Liang L, Huang H, Hong Z, Yu J, Kang M, Song Y, Xia J, Guo Q, Song T, He J, Yen HL, Peiris M, Wu J (March 2020). "SARS-CoV-2 Viral Load in Upper Respiratory Specimens of Infected Patients". N. Engl. J. Med. 382 (12): 1177–1179. doi:10.1056/NEJMc2001737. PMC 7121626 Check |pmc= value (help). PMID 32074444 Check |pmid= value (help).
  15. Puelles VG, Lütgehetmann M, Lindenmeyer MT, Sperhake JP, Wong MN, Allweiss L, Chilla S, Heinemann A, Wanner N, Liu S, Braun F, Lu S, Pfefferle S, Schröder AS, Edler C, Gross O, Glatzel M, Wichmann D, Wiech T, Kluge S, Pueschel K, Aepfelbacher M, Huber TB (May 2020). "Multiorgan and Renal Tropism of SARS-CoV-2". N. Engl. J. Med. doi:10.1056/NEJMc2011400. PMC 7240771 Check |pmc= value (help). PMID 32402155 Check |pmid= value (help).
  16. Puelles VG, Lütgehetmann M, Lindenmeyer MT, Sperhake JP, Wong MN, Allweiss L, Chilla S, Heinemann A, Wanner N, Liu S, Braun F, Lu S, Pfefferle S, Schröder AS, Edler C, Gross O, Glatzel M, Wichmann D, Wiech T, Kluge S, Pueschel K, Aepfelbacher M, Huber TB (May 2020). "Multiorgan and Renal Tropism of SARS-CoV-2". N. Engl. J. Med. doi:10.1056/NEJMc2011400. PMC 7240771 Check |pmc= value (help). PMID 32402155 Check |pmid= value (help).

Template:WikiDoc Sources




ACUTE MYOCARDIAL INJURY:


Overview

Acute myocardial injury may be defined across studies as any of the following

Coronavirus disease 2019 (COVID-19) is a rapidly expanding global pandemic which is caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) , resulting in significant morbidity and mortality. Some hospitalized patients can develop an acute COVID-19 myocardial injury, which can manifest with a variety of clinical presentations but often presents as an acute cardiac injury with cardiomyopathy, ventricular arrhythmias, and hemodynamic instability, acute coronary syndrome, cardiogenic shock. patents with preexisting cardiovascular disease have higher morbidity and mortality.

Historical Perspective

  • One of the first reports of myocardial injury associated with SARS-CoV-2 was a study of 41 patients diagnosed with COVID-19 in Wuhan, China, wherein 5 patients (12%) had a high-sensitivity troponin I above the threshold of 28 pg/mL [5]

Classification

There is no established system for the classification of Acute myocardial injury.

Pathophysiology

  • The pathophysiology of myocardial injury include,
    • Hyperinflammation and cytokine storm mediated through pathologic T-cells and monocytes leading to myocarditis[6]
    • Respiratory failure and hypoxemia resulting in damage to cardiac myocytes[7]
    • Down regulation of ACE2 expression and subsequent protective signaling pathways in cardiac myocytes
    • Hypercoagulability and development of coronary microvascular thrombosis[8]
    • Diffuse endothelial injury and ‘endotheliitis’ in several organs, including the heart as a direct consequence of SARS-CoV-2 viral involvement and/or resulting from host inflammatory response.[9]
    • inflammation and/or stress causing coronary plaque rupture or supply-demand mismatch leading to myocardial ischemia/infarction.[10]
    • Electrolyte imbalances and adverse medication effects may disproportionately challenge a diseased heart, with special consideration for the regimen of hydroxychloroquine and azithromycin treatment due to the potential for QTc prolongation [11]
    • Direct invasion of the cardiac tissue by COVID-19.[12]

Hyperinflammation and cytokine storm:

  • Immune dysregulation, including T cell and immune signaling dysfunction, recognized as an important factor in the pathogenesis of vascular disease, may also adversely affect the body's response to SARS-CoV-2 infection[13]
  • The role of CD4(+)CD25(+)FOXP3(+) regulatory T (TREG) cells in the modulation of inflammation and immunity has received increasing attention. Given the important role of TREG cells in the induction and maintenance of immune homeostasis and tolerance, dysregulation in the generation or function of TREG cells can trigger abnormal immune responses and lead to pathology.
  • Evidence from experimental and clinical studies has indicated that TREG cells might have an important role in protecting against cardiovascular disease, in particular atherosclerosis and abdominal aortic aneurysm.
  • The role of TREG cells is evident in the pathogenesis of a number of cardiovascular diseases, including atherosclerosis, hypertension, ischaemic stroke, abdominal aortic aneurysm, Kawasaki disease, pulmonary arterial hypertension, myocardial infarction and remodelling, postischaemic neovascularization, myocarditis and dilated cardiomyopathy, and heart failure.[14]

Role of ACE Receptor :

  • ACE-2 is a membrane-bound aminopeptidate receptor expressed on the epithelial cells of the lungs, intestines, kidneys and blood vessels. It has important immune and cardiovascular roles. Angiotensin-converting enzyme (ACE) cleaves angiotensin I to generate angiotensin II (Ang II), which binds to and activates AT1R, thus promoting vasoconstriction.
  • ACE-2 cleaves angiotensin II and generates angiotensin 1–7, a powerful vasodilator acting through Mas receptors.
  • SARS-CoV-2 has a spike protein receptor-binding domain, similar to SARS-CoV-1, which interacts with the ACE-2 receptor and acts as the primary functional receptor for pathogenicity and human-to-human transmission.[15] Furthermore, SARS-CoV-2 binding to ACE-2 leads to its down regulation and increases angiotensin II,a pro-inflammatory factor in the lung.
  • This subsequently leads to lower amount of angiotensin 1–7. Thus loss of protective signaling pathway in cardiac myocytes. The detrimental effect of ACE-2 downregulation would impede cardioprotective effects of angiotensin 1–7 leading to increased TNFα production, other cytokines release that can result in acute respiratory syndrome, acute cardiac injury and multiorgan dysfunction.[16]

Causes

  • Acute respiratory distress syndrome. (ARDS)
  • Pneumonia.
  • Hypercoagulability and plaque rupture.
  • Hyperinflammation and cytokine storm.
  • Electrolyte imbalances and adverse medication effects
  • Direct invasion of the cardiac tissue by COVID-19.
  • Myocarditis and myocyte necrosis.

Epidemiology and Demographics

  • A summary of 44,672 COVID-19 cases documented by the Chinese Center for Disease Control and Prevention demonstrated a case fatality rate of 10.5% with comorbid CVD ( cardiovascular disease) compared to a 2.4% overall case fatality rate[17]
  • The frequency of myocardial injury (as reflected by elevation in cardiac troponin levels) is variable among hospitalized patients with COVID-19, with reported frequencies of 7 to 28 percent[18] [19]. Some studies have identified greater frequency and magnitude of troponin elevations in hospitalized patients with more severe disease and worse outcomes [20]
  • In a series of 416 patients with COVID-19 who were hospitalized in Wuhan, China, 19.7 percent had high-sensitivity troponin I (hs-TnI) above the 99th percentile upper reference limit on admission [21]. Patients with this marker of myocardial injury were older and had more comorbidities (including chronic heart failure in 14.6 versus 1.5 percent), greater laboratory abnormalities (including higher levels of C-reactive protein, procalcitonin, and aspartate aminotransferase), more lung radiographic abnormalities, and more complications compared with those without myocardial injury. The mortality rate was also higher in those with myocardial injury (51.2 versus 4.5 percent). The risk of death starting from the time of symptom onset was more than four times higher in patients with evidence of myocardial injury on admission.

Risk Factors

A meta-analysis of 6 studies inclusive of 1,527 patients with COVID-19 examined the prevalence of cardio vascular disease (CVD) and reported the prevalence of hypertension, cardiac and cerebrovascular disease, and diabetes to be 17.1%, 16.4%, and 9.7%, respectively [22]

Screening

  • There is insufficient evidence to recommend routine screening for acute myocardial injury in COVID-19 patients.

Natural History, Complications, and Prognosis

  • The disease also contributes to cardiovascular complications, including
    • Acute coronary syndromes
    • Arrhythmias
    • Myocarditis
    • Pericarditis
    • Heart failure
    • Cardiogenic shock
    • Death.
  • Older patients with preexisting cardiovascular comorbidities and diabetes are prone to develop a higher acuity of illness after contracting SARS-CoV-2 associated with higher risk of myocardial injury and a markedly higher short-term mortality rate.[23]

Diagnosis

Diagnostic Study of Choice

  • Cardiac Biomarkers and Acute Cardiac Injury
    • he upper reference limit for the high-sensitivity troponin I (hs-TnI) test (0.04ng/mL), based on the 99th percentile of measurements reported in healthy population without the occlusion of coronary arteries.
    • In the recently published retrospective study of 191 COVID-19 patients from two separate hospitals in China, the incidence of elevation in high-sensitivity cardiac troponin I (cTnI) (>28 pg/ml) was 17%, and it was significantly higher among non-survivors (46% versus 1%, p<0.001).10 Furthermore, elevation of this biomarker was noted to be a predictor of in-hospital death (univariable OR 80.07, 95% CI [10.34–620.36], p<0.0001). The most abrupt increase in cTnI in non-survivors was noted beyond day 16 after the onset of disease. In the same study, the incidence of acute cardiac injury was 17% among all-comers, but significantly higher among non-survivors (59% versus 1%, p<0.0001).[24]
    • CK-MB >2.2 ng/mL
    • Guo et al11 provide additional novel insights that TnT levels are significantly associated with levels of C-reactive protein and N-terminal pro-B-type natriuretic peptide (NT-proBNP), thus linking myocardial injury to severity of inflammation and ventricular dysfunction[25]

History and Symptoms

  • Patients with COVID-19 can present with the typical symptoms and signs of SARS-CoV-2 nfection such as fever, cough, dyspnea, and bilateral infiltrates on chest imaging can present with chest pain, dyspnea, dysarrhythmia, and acute left ventricular dysfunction [26] [27]

Physical Examination

Laboratory Findings

Electrocardiogram

  • The electrocardiogram (ECG) can demonstrate a range of findings
    • In some cases mimicking acute coronary syndrome (ACS).
    • The ECG abnormalities result from myocardial inflammation and include non-specific ST segment-T wave abnormalities.
    • T wave inversion.
    • PR segment and ST segment deviations (depression and elevation)

X-ray

Echocardiography or Ultrasound

CT scan

MRI

Other Imaging Findings

Other Diagnostic Studies

Treatment

Treatment of Acute myocardial injury depends upon the complication the

References

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  15. Wan, Yushun; Shang, Jian; Graham, Rachel; Baric, Ralph S.; Li, Fang; Gallagher, Tom (2020). "Receptor Recognition by the Novel Coronavirus from Wuhan: an Analysis Based on Decade-Long Structural Studies of SARS Coronavirus". Journal of Virology. 94 (7). doi:10.1128/JVI.00127-20. ISSN 0022-538X.
  16. Zhou, Peng; Yang, Xing-Lou; Wang, Xian-Guang; Hu, Ben; Zhang, Lei; Zhang, Wei; Si, Hao-Rui; Zhu, Yan; Li, Bei; Huang, Chao-Lin; Chen, Hui-Dong; Chen, Jing; Luo, Yun; Guo, Hua; Jiang, Ren-Di; Liu, Mei-Qin; Chen, Ying; Shen, Xu-Rui; Wang, Xi; Zheng, Xiao-Shuang; Zhao, Kai; Chen, Quan-Jiao; Deng, Fei; Liu, Lin-Lin; Yan, Bing; Zhan, Fa-Xian; Wang, Yan-Yi; Xiao, Geng-Fu; Shi, Zheng-Li (2020). "A pneumonia outbreak associated with a new coronavirus of probable bat origin". Nature. 579 (7798): 270–273. doi:10.1038/s41586-020-2012-7. ISSN 0028-0836.
  17. Bodini G, Demarzo MG, Casagrande E, De Maria C, Kayali S, Ziola S, Giannini EG (May 2020). "Concerns related to COVID-19 pandemic among patients with inflammatory bowel disease and its influence on patient management". Eur. J. Clin. Invest. 50 (5): e13233. doi:10.1111/eci.13233. PMC 7235524 Check |pmc= value (help). PMID 32294238 Check |pmid= value (help).
  18. Shi S, Qin M, Shen B, Cai Y, Liu T, Yang F, Gong W, Liu X, Liang J, Zhao Q, Huang H, Yang B, Huang C (March 2020). "Association of Cardiac Injury With Mortality in Hospitalized Patients With COVID-19 in Wuhan, China". JAMA Cardiol. doi:10.1001/jamacardio.2020.0950. PMC 7097841 Check |pmc= value (help). PMID 32211816 Check |pmid= value (help).
  19. Lippi G, Lavie CJ, Sanchis-Gomar F (March 2020). "Cardiac troponin I in patients with coronavirus disease 2019 (COVID-19): Evidence from a meta-analysis". Prog Cardiovasc Dis. doi:10.1016/j.pcad.2020.03.001. PMC 7127395 Check |pmc= value (help). PMID 32169400 Check |pmid= value (help).
  20. Shi S, Qin M, Shen B, Cai Y, Liu T, Yang F, Gong W, Liu X, Liang J, Zhao Q, Huang H, Yang B, Huang C (March 2020). "Association of Cardiac Injury With Mortality in Hospitalized Patients With COVID-19 in Wuhan, China". JAMA Cardiol. doi:10.1001/jamacardio.2020.0950. PMC 7097841 Check |pmc= value (help). PMID 32211816 Check |pmid= value (help).
  21. Shi S, Qin M, Shen B, Cai Y, Liu T, Yang F, Gong W, Liu X, Liang J, Zhao Q, Huang H, Yang B, Huang C (March 2020). "Association of Cardiac Injury With Mortality in Hospitalized Patients With COVID-19 in Wuhan, China". JAMA Cardiol. doi:10.1001/jamacardio.2020.0950. PMC 7097841 Check |pmc= value (help). PMID 32211816 Check |pmid= value (help).
  22. Li, Bo; Yang, Jing; Zhao, Faming; Zhi, Lili; Wang, Xiqian; Liu, Lin; Bi, Zhaohui; Zhao, Yunhe (2020). "Prevalence and impact of cardiovascular metabolic diseases on COVID-19 in China". Clinical Research in Cardiology. 109 (5): 531–538. doi:10.1007/s00392-020-01626-9. ISSN 1861-0684.
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COVID 19


For the main page on coronavirus infection, please click here

The novel coronavirus (SARS-CoV-2), also known as the Wuhan coronavirus, is a contagious virus that causes respiratory infection and has shown evidence of human-to-human transmission, first identified by authorities in Wuhan, Hubei, China, as the cause of the ongoing 2019–20 Wuhan coronavirus outbreak. Genomic sequencing has shown that it is a positive-sense, single-stranded RNA coronavirus.

Due to reports that the initial cases had epidemiological links to a large seafood and animal market, the virus is thought to have a zoonotic origin, though this has not been confirmed. Comparisons of genetic sequences between this virus and other existing virus samples have shown similarities to SARS-CoV (79.5%) and bat coronaviruses (96%),[1] with a likely origin in bats being theorized.

Epidemiology

Main article: 2019–20 Wuhan coronavirus outbreak

The first known human infection occurred in early December 2019. Molecular clock approaches suggest a similar, or slightly earlier, date of origin.

An outbreak of SARS-CoV-2 was first detected in Wuhan, China, in mid-December 2019. The virus subsequently spread to other provinces of Mainland China and other countries, including Thailand, Japan, Taiwan, South Korea, Australia, France, and the United States.

As of 29 January 2020 (04:00 UTC), there were 6,057 confirmed cases of infection, of which 5,970 were within mainland China. Cases outside China, to date, were people who have either travelled from Wuhan, or were in direct contact with someone who travelled from the area. The number of deaths was 132 as of 29 January 2020 (04:00 UTC).[2] Human-to-human spread was first confirmed in Guangdong, China, on 20 January 2020.

Treatment

No specific treatment is currently available, so treatment is focused on alleviation of symptoms, which include fever, fatigue, dry cough, and shortness of breath, or pneumonia and kidney failure in severe cases. The Chinese Center for Disease Control and Prevention (CCDC) is testing existing pneumonia treatments for efficacy in treating coronavirus-related pneumonia.

Existing anti-virals are being studied,[3] including protease inhibitors like indinavir, saquinavir, remdesivir, lopinavir/ritonavir and interferon beta. The effectiveness of previously identified monoclonal antibodies (mAbs) is also under investigation.

Virology

Infection

Human-to-human transmission of the virus has been confirmed.[4] Reports have emerged that the virus is infectious even during the incubation period, although as of 27 January 2020 officials at the Centers for Disease Control and Prevention (CDC) in the United States stated they "don't have any evidence of patients being infectious prior to symptom onset."

Research groups have estimated the basic reproduction number (<math>R_0</math>, pronounced R-nought) of the virus to be between 1.4 and 5, with most estimates below 3.8. This means that, when unchecked, the virus typically results in 1.4 to 3.8 new cases per established infection. It has been established that the virus is able to transmit along a chain of at least four people.

Reservoir

Animals sold for food are suspected to be the reservoir or the intermediary because many of the first identified infected individuals were workers at the Huanan Seafood Market. Consequently, they were exposed to greater contact with animals.[5] A market selling live animals for food was also blamed in the SARS epidemic in 2003; such markets are considered to be incubators for novel pathogens. The outbreak has prompted a temporary ban on the trade and consumption of wild animals in China.

With a sufficient number of sequenced genomes, it is possible to reconstruct a phylogenetic tree of the mutation history of a family of viruses. During 17 years of research on the origin of the SARS 2003 epidemic, many SARS-like bat coronaviruses were isolated and sequenced, most of them originating from the Rhinolophus genus of bats. SARS-CoV-2 has been found to fall into this category of SARS-related coronaviruses. Two genome sequences from Rhinolophus sinicus published in 2015 and 2017 show a resemblance of 80% to SARS-CoV-2.[6][7] A third unpublished virus genome from Rhinolophus affinis, "RaTG13", is said to have a 96% resemblance to SARS-CoV-2. For comparison, this amount of variation among viruses is similar to the amount of mutation observed over ten years in the H3N2 human flu virus strain.

Phylogenetics and taxonomy

Genomic information
File:2019-nCoV genome.svg
Genome organisation (click to enlarge)
NCBI genome IDMN908947
Genome size29,903 bases
Year of completion2020

SARS-CoV-2 belongs to the broad family of viruses known as coronaviruses. Other coronaviruses are capable of causing illnesses ranging from the common cold to more severe diseases such as the Middle East respiratory syndrome (MERS) and severe acute respiratory syndrome (SARS). It is the seventh known coronavirus to infect people, after 229E, NL63, OC43, HKU1, MERS-CoV, and SARS-CoV.

Though genetically distinct from other coronaviruses that infect humans, it is, like SARS-CoV, a member of the subgenus Sarbecovirus (Beta-CoV lineage B).[5] Its RNA sequence is approximately 30 kb in length.[8]

By 12 January, five genomes of the novel coronavirus had been isolated from Wuhan and reported by the Chinese Center for Disease Control and Prevention and other institutions;[8] the number of genomes increased to 28 by 26 January. Except for the earliest GenBank genome, the genomes are under an embargo at GISAID. A phylogenic analysis for the samples is available through Nextstrain.

Structural biology

File:Coronavirus 2019-nCoV.3.png
Innophore Phyre2 ribbon diagram of the SARS-CoV-2 M(pro) protease, a prospective target for antiviral drugs

The publications of the genome led to several protein modeling experiments on the receptor binding protein (RBD) of the nCoV spike (S) protein suggesting that the S protein retained sufficient affinity to the Angiotensin converting enzyme 2 (ACE2) receptor to use it as a mechanism of cell entry. On 22 January, a group in China working with the full virus and a group in the U.S. working with reverse genetics independently and experimentally demonstrated ACE2 as the receptor for SARS-CoV-2.

To look for potential protease inhibitors, the viral 3C-like protease M(pro) from the Orf1a polyprotein was also modeled for drug docking experiments. Innophore has produced two computational models based on SARS protease,[9] and the Chinese Academy of Sciences has produced an unpublished experimental structure of a recombinant SARS-CoV-2 protease.

Vaccine research

In January 2020, several organizations and institutions began work on creating vaccines for 2019 n-CoV based on the published genome.

In China, the Chinese Center for Disease Control and Prevention is developing a vaccine against the novel coronavirus.[10] The team of Yuen Kwok-yung at the University of Hong Kong, which previously participated in work on the SARS coronavirus during its 2003 outbreak, has also announced that a vaccine is under development there but has yet to proceed to animal testing.

Elsewhere, three vaccine projects are being supported by the Coalition for Epidemic Preparedness Innovations (CEPI), including one project by the biotechnology company Moderna and another by the University of Queensland. The United States National Institutes of Health (NIH) is cooperating with Moderna to create an RNA vaccine matching a spike of the coronavirus surface, and is hoping to start production by May 2020. In Australia, the University of Queensland is investigating the potential of a molecular clamp vaccine that would genetically modify viral proteins to make them mimic the coronavirus and stimulate an immune reaction.

In an independent project, the Public Health Agency of Canada has granted permission to the International Vaccine Centre (VIDO-InterVac) at the University of Saskatchewan to begin work on a vaccine. VIDO-InterVac aims to start production and animal testing in March 2020, and human testing in 2021.


  5. 5.0 5.1
  8. 8.0 8.1
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