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Overview
Historical Perspective
Classification
Pathophysiology
Causes
Epidemiology and Demographics
Risk factors
Natural History, Complications, and Prognosis
Diagnosis
Treatment
Prevention

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Latest revision as of 21:06, 24 February 2021

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Ifeoma Anaya, M.D.[2]

Synonyms and keywords: Acrocyanosis; central cyanosis

Overview

Cyanosis is derived from the word kuaneos which is Greek for dark blue. It is categorized into two major types: peripheral and central cyanosis. Cyanosis is observed with an increase in the absolute concentration of deoxygenated hemoglobin to a level of 3-5g/dl. A structured way of grouping the common causes of cyanosis in newborns is by using the ABC which stands for Airway, Breathing, and Circulation. Persistent pulmonary hypertension of the newborn and congenital heart diseases (CHD) are the common causes of newborn cyanosis. Common risk factors in the development of cyanosis in newborns are evident in the pregnancy and labor period. Prompt recognition, and administration of treatment modalities, with appropriate referral to the ideal hospital setting equipped to manage the diagnosis, can improve the prognosis. The primary symptom is the bluish/dark colored lips, mucous membrane, and/or hands and feet. Patients can have breathing difficulties which can be seen as nasal flaring and chest retractions. Findings from exam include lethargy, conjunctival injection, features of shock, and tachypnea. Laboratory findings include a complete blood count, and differentials showing packed cell volume (PCV) suggesting polycythemia, and white cell count (septicemia). ECG is used seldomly, however, it may aid in the diagnosis of arrhythmias and dextrocardia. X-rays can show pulmonary causes such as pulmonary hypoplasia and increased lung vascular markings in pulmonary edema, and bronchopneumonia. Echocardiography can be used when the diagnosis is equivocal or when physical exam findings and/or failed hyperoxia test suggests the presence of congenital heart disease. There are other imaging techniques used as adjuncts to making diagnoses. The immediate priority is to optimize the neonate, especially in severe cyanosis. Surgery is employed for more definitive treatment. The preventive measures that can be adopted include pre-conceptual counseling for expectant mothers especially women who are above the age of 35 years, routine prenatal and postnatal care for early detection of congenital anomalies, and adequate preparedness for its management during pregnancy, labor, and delivery.

Historical Perspective

Cyanosis is derived from the word kuaneos which is Greek for dark blue. This is a result of the bluish discoloration of the skin or mucous membranes depending on the etiology.^[1]

Classification

Cyanosis is classified into two major types:^[2]
- Peripheral Cyanosis (acrocyanosis) seen on the hands and feet and mostly physiological.
- Central cyanosis, considered to be pathological requiring prompt evaluation.

Pathophysiology

Central cyanosis occurs as a result of an increase in the absolute concentration of deoxygenated hemoglobin to 3-5 g/dl. Deoxygenated hemoglobin is dusky blue or purple, which causes the discoloration seen in skin and mucous membranes as compared to the bright red oxyhemoglobin.^[1]
Oxygen is transported in blood predominantly attached to hemoglobin while an insignificant amount is transported dissolved in plasma. Sufficient tissue perfusion relies on the concentration of saturated hemoglobin.
With high hemoglobin concentrations (normal relative polycythemia,14-20 g/dl) seen in normal infants, cyanosis becomes apparent at higher PaO2 (partial pressure of oxygen) compared to the setting of severe anemia, whereas a far lower PaO2 leads to clinically recognizable cyanosis due to very low hemoglobin concentration. Therefore, cyanosis depends on the concentration of deoxygenated hemoglobin and not merely oxygen saturation. As an example, a neonate with a hemoglobin concentration of 24 g/dl exhibits signs of central cyanosis at 88% arterial saturation (SaO2) while cyanosis isn't clinically obvious in an anemic infant until SaO2 falls to about 62%.^[1]^[3]
Oxygen binding capacities differ between fetal and adult hemoglobin. If a newborn has mostly adult hemoglobin, cyanosis would be observed at an elevated PaO2 of 42-53 mmHg which is comparable to SaO2 of 75%-85% as opposed to the predominantly fetal hemoglobin (PaO2 of 32-42 mmHg); infants have varied proportions of adult and fetal hemoglobin. Therefore, a major reduction in PaO2 would have set in before cyanosis becomes apparent in a newborn with elevated fetal hemoglobin, a setting that shifts the oxygen-hemoglobin dissociation curve to the left.^[3]
Several changes occur in the newborn from the first breath. Blood flow resistance decreases within the pulmonary vasculature as a result of a rise in oxygen tension; this increase in oxygen tension and pulmonary circulation causes functional closure of the patent ductus arteriosus (PDA). Raised left atrial pressures closes the foramen ovale. The events resulting in the closures of these shunts invariably abolishes the right-to-left shunts of the precedent fetal circulation. The first breath also causes a net absorption of the fluid from the lungs, causing its expansion and successfully initiates the gaseous exchange. Furthermore, removal of the low-pressure placental bed causes a rise in blood flow resistance of the systemic vasculature. These are the traditional physiological changes observed in a normal neonate after birth.^[1]
Deviations from these may result in pathological conditions requiring immediate interventions; infants, especially those born prematurely, would require medical assistance for this phenomenal transition.^[4]
In peripheral cyanosis, there's normal SaO2 with a rise in oxygen uptake by the tissues leading to a wide arteriovenous difference within the venous aspect of the capillaries. Vasoconstriction could be a cause. This kind of cyanosis is seen majorly at the extremities.

Causes

A structured way of grouping the common causes of cyanosis in newborns is by using the ABC which stands for Airway, Breathing, and Circulation.

Causes of cyanosis in newborns

Airway

Breathing

Circulation

• Cystic hygroma
• Hemangioma
• Choanal atresia
• Micrognathia
• Laryngomalacia
• Tracheal stenosis
• Vascular rings
• Vocal cord paralysis
• Pierre Robin sequence

• Phrenic nerve palsy
• Congenital diaphragmatic hernia
• Perinatal asphyxia
• Pulmonary hypoplasia
• Inborn errors of metabolism
• Central nervous system and muscle congenital anomalies
• Neonatal sepsis
• Neonatal botulism
• Congenital cystic adenomatoid malformation
• Pneumonia

• Congenital heart diseases
Tetralogy of Fallot (TOF)
Tricuspid atresia
Pulmonary atresia
Pulmonary stenosis
Ebstein's anomaly
Transposition of great arteries (TGA)
Hypoplastic left heart syndrome
Atrioventricular canal defect
Total anomalous pulmonary venous return (TAPVR)
• Anemia
• Methemoglobinemia
• Polycythemia
• Persistent pulmonary hypertension

Epidemiology and Demographics

Persistent pulmonary hypertension of the newborn and Congenital heart diseases (CHD) are the common causes of newborn cyanosis. Common in older kids are respiratory diseases.^[5]^[6]
Tetralogy of Fallot (TOF) followed closely by the Transposition of Great Arteries (TGA) are the commonest causes of CHD.^[6]

Age

Newborns are more prone to cyanosis due to the peculiarities of birth and the changes that occur during the transition from fetal to neonatal life and/or due to congenital or acquired disorders.

Risk Factors

Common risk factors for the development of cyanosis in newborns are evident in the pregnancy and labor period.
Pregnancy-related risk factors include:
- Advanced age of the mother
- Pregnancy-induced hypertension
- Gestational diabetes
- Intake of Lithium (Ebstein's anomaly)
- Oligohydramnios
- Polyhydramnios
Labor and birth-related risk factors include:
- Cesarean section
- Preterm/prematurity
- Use of anesthetic drugs and/or sedatives
- Premature rupture of membranes (PROM)
- Meconium aspiration
- Difficult/assisted vaginal delivery

Natural History, Complications and Prognosis

Potential complications seen in these patients can include:
- Stroke
- Sudden Cardiac Arrest
- Repeated respiratory tract infections in infants with unrepaired heart defects which can be severe
- Developmental delays ranging from motor to cognitive
- Various forms of disabilities
- Arrhythmias
- Heart failure
Prompt recognition, and administration of treatment modalities, with appropriate referral to the ideal hospital setting equipped to manage the diagnosis, can improve the prognosis.
Mortality is high in newborns with critical CHD however, there has been an encouraging improvement in one-year survival to 75% following advances in treatment. 69% of these babies can survive to the age of 18 years.^[1]^[6]

Diagnosis

Symptoms

Primary symptom is the bluish/dark colored lips, mucous membranes, and/or hands and feet
Other symptoms include the following:
- Breathing difficulties evident as:
  - Nasal flaring
  - Chest retractions
  - Fast breathing
  - Slow breathing
  - Irregular breathing
  - History of momentary cessations of breathing
- Pausing/excessive sweating or crying while feeding
- Small volume of feeds
- Small for age/poor weight gain
- Large for age
- Fixed/immobile arms suggesting paralysis from birth trauma
- Increasing head circumference with\without scalp injuries resulting from a difficult delivery
- Hypo/hyperactive child

Physical Examination

Patients usually appear cyanotic.
Depending on the underlying etiology, other examination findings may include the following:
- Lethargy
- Conjunctival injection
- Features of shock
- Tachypnea
- Periodic breathing
- Apneic spells
- Use of accessory muscles of respiration
- Flaring of the alar nasa
- Tube or catheter carefully inserted into the nasal cavity if suspicion is high for choanal atresia
- Tachycardia
- Abnormal heart sounds/murmurs
- Weak peripheral pulses especially femoral pulse
- Fine crackles in lower lung fields
- Hepatomegaly
- Scaphoid abdomen (in diaphragmatic hernia)
- Erb's paralysis
- Scalp injuries
- Seizures

Laboratory Findings

Complete blood count and differentials:
- Increased packed cell volume (PCV)- polycythemia
- Increased white cell count- septicemia
Complete metabolic panel- electrolyte imbalance (metabolic acidosis)
Serum glucose- hypo or hyperglycemia
Hyperoxia Test- differentiates pulmonary from a cardiovascular cause. An increase in PaO2 to a 100 mmHg or more after administering 100% oxygen suggests a pulmonary etiology. Seldom used due to the availability of echocardiography.
Arterial Blood Gases (ABGs)
- PaCO2, ↑ suggests hypoventilation of CNS, pulmonary or cardiac etiology.
- PaO2, ↓ confirms cyanosis
- PH, a ↓ pH suggests hypoxemia,or/and sepsis
- 'Chocolate-brown' color of blood with normal levels of PaO2 and reduced SaO2 methemoglobinemia

Electrocardiogram

It is seldom used, however, may be helpful in the diagnosis of arrhythmias and dextrocardia to show a left axis deviation seen in tricuspid atresia due to left ventricular hypertrophy.
It could give a normal reading in very serious heart defects such as TGA.^[1]

X-ray

Can identify:
- Pulmonary causes such as pulmonary hypoplasia
- Increased lung vascular markings in pulmonary edema, bronchopneumonia
- Reduced pulmonary markings in pulmonary atresia, pulmonary stenosis, and persistent pulmonary hypertension of newborns
- Location of abdominal contents in diaphragmatic hernia
- Elevation of the affected hemidiaphragm in phrenic nerve injury
- Cystic adenomatoid malformation
Characteristic features of some congenital heart diseases may be seen such as:
- 'Snowman' or 'Figure 8' in TAPVR
- 'Boot-shaped heart' in TOF
- 'Egg-on-string' in TGA
- Cardiomegaly in Ebstein's anomaly

Echocardiography or Ultrasound

Can be used when the diagnosis is equivocal or when physical exam findings and/or failed hyperoxia test suggests the presence of congenital heart disease.
It is usually used with doppler to define the direction of shunts.^[6]

CT scan

Used as an adjunct to further define cardiac and other anatomical anomalies in preparation for the definitive management.

MRI

Used as an adjunct to further define cardiac and other anatomical anomalies in preparation for the definitive management.

Other Imaging Findings

Cardiac catheterization and angiography:
- Sometimes used as an adjunct to further define cardiac and other anatomical anomalies in preparation for the definitive management.

Other Diagnostic Studies

Pre-ductal and post-ductal PaO2 measurements.

Treatment

Medical Therapy

The immediate priority is to optimize the neonate, especially in severe cyanosis. This includes:
- Establishing assisted ventilation in respiratory distress.
- Keep infant in a radiant warmer.
- Stop all per oral feeds and give intravenous fluids through peripheral or central access such as umbilical vein.
- Give glucose for hypoglycemic infants and monitor serum glucose levels.
- Consult should be sent to the neonatologist.
- Oxygen administration should be done with caution. Care must be taken not to begin with very high concentrations of 100% due to damage to the lung tissue and pulmonary vessels.
- Prostaglandin E1 (PGE1) given as an infusion to keep the ductus patent for pulmonary blood flow in CHDs.
- Definitive treatment can be planned in stages once infant is optimized and a diagnosis has been made.
- Antibiotics coverage for sepsis if suspected, after blood samples are taken for culture and sensitivity, and urine samples have been collected.

Surgery

This a treatment modality for diagnoses associated with anatomic deformities in CHDs or airway obstructions.
Surgical treatment is tailored to the underlying cause of cyanosis that requires surgical intervention. An example is a Balloon Atrial Septostomy for acute TGA allowing for blood mixing.^[1]

Prevention

Prevention can be challenging as some of its causes are prevalent in-utero before the birth of child while others occur during the actual labor and birthing process.
The preventive measures that can be adopted include:
Counsel expectant mothers especially women who are above the age of 35 years.
Routine prenatal and postnatal care for early detection of congenital anomalies and adequate preparedness for its management during pregnancy, labor, and delivery.
Early detection and management of gestational diabetes and pregnancy-induced hypertension.
Parents of a child with congenital malformations should be counseled on the risk of having another child with the same or similar deformities.
Prophylaxis against respiratory syncytial virus (RSV).
Follow up for polycythemia, excessive dehydration, and iron-deficiency anemia.^[6]

References

↑ ^1.0 ^1.1 ^1.2 ^1.3 ^1.4 ^1.5 ^1.6 Steinhorn RH (2008). "Evaluation and management of the cyanotic neonate". Clin Pediatr Emerg Med. 9 (3): 169–175. doi:10.1016/j.cpem.2008.06.006. PMC 2598396. PMID 19727322.
↑ Izraelit A, Ten V, Krishnamurthy G, Ratner V (2011). "Neonatal cyanosis: diagnostic and management challenges". ISRN Pediatr. 2011: 175931. doi:10.5402/2011/175931. PMC 3317242. PMID 22482063.
↑ ^3.0 ^3.1 Lees MH, King DH (1987). "Cyanosis in the newborn". Pediatr Rev. 9 (2): 36–42. doi:10.1542/pir.9-2-36. PMID 3332361.
↑ Hooper SB, olglase GR, Roehr CC (2015). "Cardiopulmonary changes with aeration of the newborn lung". Paediatr Respir Rev. 16 (3): 147–50. doi:10.1016/j.prrv.2015.03.003. PMC 4526381. PMID 25870083.
↑ https://pediatriccare.solutions.aap.org/chapter.aspx?sectionid=108722941&bookid=1626
↑ ^6.0 ^6.1 ^6.2 ^6.3 ^6.4 "StatPearls". 2020. PMID 29763177.

[pmid19727322-1] 1.0 ^1.1 ^1.2 ^1.3 ^1.4 ^1.5 ^1.6 Steinhorn RH (2008). "Evaluation and management of the cyanotic neonate". Clin Pediatr Emerg Med. 9 (3): 169–175. doi:10.1016/j.cpem.2008.06.006. PMC 2598396. PMID 19727322.

[pmid22482063-2] Izraelit A, Ten V, Krishnamurthy G, Ratner V (2011). "Neonatal cyanosis: diagnostic and management challenges". ISRN Pediatr. 2011: 175931. doi:10.5402/2011/175931. PMC 3317242. PMID 22482063.

[pmid3332361-3] 3.0 ^3.1 Lees MH, King DH (1987). "Cyanosis in the newborn". Pediatr Rev. 9 (2): 36–42. doi:10.1542/pir.9-2-36. PMID 3332361.

[pmid25870083-4] Hooper SB, olglase GR, Roehr CC (2015). "Cardiopulmonary changes with aeration of the newborn lung". Paediatr Respir Rev. 16 (3): 147–50. doi:10.1016/j.prrv.2015.03.003. PMC 4526381. PMID 25870083.

[5] ttps://pediatriccare.solutions.aap.org/chapter.aspx?sectionid=108722941&bookid=1626

[pmid29763177-6] 6.0 ^6.1 ^6.2 ^6.3 ^6.4 "StatPearls". 2020. PMID 29763177.

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[2]

[3]

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[5]

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@@ Line 82: / Line 82: @@
 ==Overview==
-[[Cyanosis]] is coined from the word '''''kuaneos''''' which is greek for '''dark blue'''. It is classified into two major types: peripheral and [[central cyanosis]]. [[Cyanosis]] results when there is an increase in the absolute [[concentration]] of deoxygenated [[hemoglobin]] to a level of 3-5g/dl. A systematic way of classifying the common causes of [[cyanosis]] in [[newborns]] is by using the '''ABC''' which stands for '''''[[Airway]]''''', '''''[[Breathing]]''''', and '''''[[Circulation]]'''''. [[Congenital heart diseases]] (CHD) affecting 8-9 per 1000 live births and Persistent [[pulmonary hypertension]] of the [[newborn]] are the common causes of [[newborn]] [[cyanosis]]. In older kids, [[respiratory]] [[diseases]] tend to be more common. Common [[risk factors]] in the development of [[cyanosis]] in [[newborns]] are evident in the [[pregnancy]] and [[labor]] period. [[Complications]] and [[prognosis]] are dependent on the actual cause of the [[cyanosis]], prompt recognition, and administration of [[treatment]] modalities with appropriate referral to the ideal [[hospital]] setting equipped to manage the [[diagnosis]]. The primary [[symptom]] is the bluish/dark colored lips, [[mucous membrane]], and/or hands and feet. [[Breathing]] difficulties such as [[nasal]] flaring, chest retractions. [[Physical examination|Exam]] findings include lethargy, [[conjunctival injection]], features of [[shock]], [[tachypnea]]. [[Laboratory findings]] include a [[Complete blood count]] and differentials showing ↑Packed cell volume([[PCV increased|PCV]]) suggesting [[polycythemia]], ↑[[White blood cells|White cell]] count ([[Septicemia]]). Although seldom helpful, an [[ECG]] may aid in the [[diagnosis]] of [[arrhythmias]] and [[dextrocardia]]. [[X-rays]] can show [[pulmonary]] causes like [[pulmonary]] [[hypoplasia]] and increased [[lung]] [[vascular]] markings in [[pulmonary edema]], [[bronchopneumonia]]. [[Echocardiography]] is employed when [[physical exam]] findings and/or failed [[hyperoxia]] test suggests the presence of [[congenital heart disease]] or when the [[diagnosis]] is uncertain. Other imaging modalities are used as adjuncts in making diagnoses. The priority in the immediate term will be to optimize the [[neonate]], especially in severe [[cyanosis]]. [[Surgery]] is employed for more definitive treatment. The following [[Preventive care|preventive]] measures can be adopted; pre-conceptual [[counseling]] for expectant mothers especially women who are above the age of 35 years, routine [[prenatal]] and [[postnatal]] care for early detection of [[congenital anomalies]], and adequate preparedness for its management during [[pregnancy]], [[labor]], and [[delivery]].
+[[Cyanosis]] is derived from the word '''''kuaneos''''' which is Greek for '''dark blue'''. It is categorized into two major types: [[Peripheral cyanosis|peripheral]] and [[central cyanosis]]. [[Cyanosis]] is observed with an increase in the absolute [[concentration]] of [[Deoxygenation|deoxygenated]] [[hemoglobin]] to a level of 3-5g/dl. A structured way of grouping the common [[causes]] of [[cyanosis]] in [[newborns]] is by using the '''ABC''' which stands for '''''[[Airway]]''''', '''''[[Breathing]]''''', and '''''[[Circulation]]'''''. Persistent [[pulmonary hypertension]] of the [[newborn]] and [[congenital heart diseases]] ([[CHD]]) are the common [[causes]] of [[newborn]] [[cyanosis]]. Common [[risk factors]] in the [[development]] of [[cyanosis]] in [[newborns]] are evident in the [[pregnancy]] and [[labor]] period. Prompt recognition, and administration of [[treatment]] modalities, with appropriate referral to the ideal [[hospital]] setting equipped to manage the [[diagnosis]], can improve the [[prognosis]]. The primary [[symptom]] is the [[Bluish lips|bluish]]/dark [[Color|colored]] [[lips]], [[mucous membrane]], and/or [[hands]] and [[feet]]. [[Patients]] can have [[breathing difficulties]] which can be seen as [[nasal]] flaring and [[chest]] retractions. Findings from [[physical examination|exam]] include [[lethargy]], [[conjunctival injection]], features of [[shock]], and [[tachypnea]]. [[Laboratory findings]] include a [[complete blood count]], and differentials showing [[Packed cell volume increased|packed cell volume]] ([[PCV increased|PCV]]) suggesting [[polycythemia]], and [[White blood cells|white cell]] count ([[septicemia]]). ECG is used seldomly, however, it may aid in the [[diagnosis]] of [[arrhythmias]] and [[dextrocardia]]. [[X-rays]] can show [[pulmonary]] [[causes]] such as [[pulmonary]] [[hypoplasia]] and increased [[lung]] [[vascular]] markings in [[pulmonary edema]], and [[bronchopneumonia]]. [[Echocardiography]] can be used when the [[diagnosis]] is equivocal or when [[physical exam]] findings and/or failed [[hyperoxia]] test suggests the presence of [[congenital heart disease]]. There are other [[Imaging studies|imaging techniques]] used as adjuncts to making [[Diagnosis|diagnoses]]. The immediate priority is to optimize the [[neonate]], especially in severe [[cyanosis]]. [[Surgery]] is employed for more definitive [[treatment]]. The [[preventive care|preventive]] [[Measure (mathematics)|measures]] that can be adopted include pre-conceptual [[counseling]] for expectant mothers especially [[women]] who are above the [[age]] of 35 [[Year|years]], routine [[prenatal]] and [[postnatal]] care for early [[Detection theory|detection]] of [[congenital anomalies]], and adequate preparedness for its management during [[pregnancy]], [[labor]], and [[delivery]].
 ==Historical Perspective==
-*[[Cyanosis]] is coined from the word '''''kuaneos''''' which is greek for '''''dark blue'''''. This is as a result of the bluish discoloration of the skin or [[mucous membranes]] depending on etiology. <ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
+*[[Cyanosis]] is derived from the word '''''kuaneos''''' which is Greek for '''''dark blue'''''. This is a [[result]] of the [[bluish discoloration of the skin]] or [[mucous membranes]] depending on the [[etiology]].<ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
 ==Classification==
 *[[Cyanosis]] is classified into two major types:<ref name="pmid22482063">{{cite journal| author=Izraelit A, Ten V, Krishnamurthy G, Ratner V| title=Neonatal cyanosis: diagnostic and management challenges. | journal=ISRN Pediatr | year= 2011 | volume= 2011 | issue=  | pages= 175931 | pmid=22482063 | doi=10.5402/2011/175931 | pmc=3317242 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=22482063  }} </ref>
-**Peripheral Cyanosis ([[acrocyanosis]]) which is located on the hands and feet. It is mostly physiological and relatively common.
+**Peripheral Cyanosis ([[acrocyanosis]]) seen on the hands and feet and mostly physiological.
-**[[Central cyanosis]] which is considered to be [[pathological]] and requiring immediate evaluation until proven otherwise.
+**[[Central cyanosis]], considered to be [[pathological]] requiring prompt evaluation.
 ==Pathophysiology==
-*[[Central cyanosis]] results when there is a rise in the absolute [[concentration]] of deoxygenated [[hemoglobin]] to a 3-5g/dl. Deoxygenated hemoglobin is dusky blue or purple which causes the discoloration seen in [[skin]] and [[mucous membranes]] compared to bright red [[oxyhemoglobin]].<ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
+*[[Central cyanosis]] occurs as a [[result]] of an increase in the absolute [[concentration]] of [[Deoxygenation|deoxygenated]] [[hemoglobin]] to 3-5 g/dl. [[Deoxygenation|Deoxygenated]] [[hemoglobin]] is dusky [[blue]] or [[Purple haze|purple]], which causes the discoloration seen in [[skin]] and [[mucous membranes]] as compared to the bright red [[oxyhemoglobin]].<ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
-*[[Oxygen]] is transported in [[blood]] predominantly attached to [[hemoglobin]] while an insignificant amount is transported [[Dissolved oxygen|dissolved]] in [[plasma]]. Sufficient [[tissue]] [[perfusion]] relies on the concentration of [[saturated]] [[hemoglobin]].
+*[[Oxygen]] is transported in [[blood]] predominantly attached to [[hemoglobin]] while an insignificant amount is transported [[Dissolved oxygen|dissolved]] in [[plasma]]. Sufficient [[tissue]] [[perfusion]] relies on the [[concentration]] of [[saturated]] [[hemoglobin]].
-*With high [[hemoglobin]] concentrations (normal relative [[polycythemia]], 14-20g/dl) seen in normal [[infants]], [[cyanosis]] becomes apparent at higher [[PaO2]] (partial pressure of oxygen) compared to the setting of severe [[anemia]] where a far lower [[PaO2]] would lead to clinically recognizable [[cyanosis]] from very low [[hemoglobin]] concentration. Therefore, [[cyanosis]] depends on the concentration of deoxygenated [[hemoglobin]] and not merely [[oxygen saturation]]. As an example, a [[neonate]] with a [[hemoglobin]] concentration of 24g/dl exhibits signs of [[central cyanosis]] at 88% [[arterial]] [[saturation]] (SaO2) while [[cyanosis]] isn't clinically obvious in an [[anemic]] [[infant]] until SaO2 falls to about 62%. <ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref> <ref name="pmid3332361">{{cite journal| author=Lees MH, King DH| title=Cyanosis in the newborn. | journal=Pediatr Rev | year= 1987 | volume= 9 | issue= 2 | pages= 36-42 | pmid=3332361 | doi=10.1542/pir.9-2-36 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=3332361  }} </ref>
+*With high [[hemoglobin]] [[concentrations]] (normal relative [[polycythemia]],14-20 g/dl) seen in normal [[infants]], [[cyanosis]] becomes apparent at higher [[PaO2]] ([[partial pressure]] of [[oxygen]]) compared to the setting of severe [[anemia]], whereas a far lower [[PaO2]] leads to clinically recognizable [[cyanosis]] due to very low [[hemoglobin]] [[concentration]]. Therefore, [[cyanosis]] depends on the [[concentration]] of [[Deoxygenation|deoxygenated]] [[hemoglobin]] and not merely [[oxygen saturation]]. As an example, a [[neonate]] with a [[hemoglobin]] [[concentration]] of 24 g/dl exhibits [[signs]] of [[central cyanosis]] at 88% [[arterial]] [[saturation]] (SaO2) while [[cyanosis]] isn't clinically obvious in an [[anemic]] [[infant]] until SaO2 falls to about 62%.<ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref><ref name="pmid3332361">{{cite journal| author=Lees MH, King DH| title=Cyanosis in the newborn. | journal=Pediatr Rev | year= 1987 | volume= 9 | issue= 2 | pages= 36-42 | pmid=3332361 | doi=10.1542/pir.9-2-36 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=3332361  }} </ref>
-*[[Fetal]] and [[adult hemoglobin]] possess different capabilities of [[oxygen]] binding. If a [[newborn]] has mostly adult [[hemoglobin]], [[cyanosis]] would be observed at an elevated [[PaO2]] 42-53mmHg which is comparable to an SaO2 of 75%-85% as opposed to predominantly [[fetal hemoglobin]]([[PaO2]] of 32-42mmHg); [[infants]] have varied proportions of [[adult]] and [[fetal hemoglobin]]. Therefore, a major reduction in [[PaO2]] would have set in before [[cyanosis]] becomes apparent in a [[newborn]] with elevated [[fetal hemoglobin]], a setting that shifts the [[oxygen-hemoglobin dissociation curve]] to the left. <ref name="pmid3332361">{{cite journal| author=Lees MH, King DH| title=Cyanosis in the newborn. | journal=Pediatr Rev | year= 1987 | volume= 9 | issue= 2 | pages= 36-42 | pmid=3332361 | doi=10.1542/pir.9-2-36 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=3332361  }} </ref>
+*[[Oxygen]] binding capacities differ between [[fetal]] and [[adult hemoglobin]]. If a [[newborn]] has mostly adult [[hemoglobin]], [[cyanosis]] would be observed at an elevated [[PaO2]] of 42-53 mmHg which is comparable to SaO2 of 75%-85% as opposed to the predominantly [[fetal hemoglobin]] ([[PaO2]] of 32-42 mmHg); [[infants]] have varied proportions of [[adult]] and [[fetal hemoglobin]]. Therefore, a major reduction in [[PaO2]] would have set in before [[cyanosis]] becomes apparent in a [[newborn]] with elevated [[fetal hemoglobin]], a setting that shifts the [[oxygen-hemoglobin dissociation curve]] to the left.<ref name="pmid3332361">{{cite journal| author=Lees MH, King DH| title=Cyanosis in the newborn. | journal=Pediatr Rev | year= 1987 | volume= 9 | issue= 2 | pages= 36-42 | pmid=3332361 | doi=10.1542/pir.9-2-36 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=3332361  }} </ref>
-*Several changes occur in the [[newborn]] from the first [[breath]]. Blood flow [[resistance]] decreases within the [[pulmonary vasculature]] as a result of a rise in [[oxygen]] tension; this increase in [[oxygen]] tension and [[pulmonary circulation]] causes functional closure of the blood vessel, [[patent ductus arteriosus (PDA)]]. Also, the [[foramen ovale]] closes from raised left [[atrial]] pressures. The events resulting in the closures of those [[shunts]] invariably abolishes the right-to-left shunts of the precedent [[fetal circulation]]. The first breath also causes a net [[absorption]] of the [[fluid]] from the [[lungs]], causing its expansion and successfully initiates the [[gaseous]] exchange. Furthermore, removal of the low-[[pressure]] [[placental]] bed causes a rise in [[blood]] flow [[resistance]] of the [[systemic]] [[vasculature]]. These are the traditional [[physiological]] changes observed within the normal [[neonate]] after [[birth]]. <ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
+*Several changes occur in the [[newborn]] from the first [[breath]]. [[Blood flow]] [[resistance]] decreases within the [[pulmonary vasculature]] as a result of a rise in [[oxygen]] tension; this increase in [[oxygen]] tension and [[pulmonary circulation]] causes functional closure of the [[patent ductus arteriosus (PDA)]]. Raised left [[atrial]] pressures closes the [[foramen ovale]]. The events resulting in the closures of these [[shunts]] invariably abolishes the right-to-left shunts of the precedent [[fetal circulation]]. The first breath also [[causes]] a net [[absorption]] of the [[fluid]] from the [[lungs]], causing its expansion and successfully initiates the [[gaseous]] [[Exchange interaction|exchange]]. Furthermore, removal of the low-[[pressure]] [[placental]] bed causes a rise in [[blood]] flow [[resistance]] of the [[systemic]] [[vasculature]]. These are the traditional [[physiological]] changes observed in a normal [[neonate]] after [[birth]].<ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
-*Deviations from these may result in [[pathological]] [[conditions]] requiring immediate [[interventions]]; [[infants]], especially those born prematurely would require medical assistance for this phenomenal transition. <ref name="pmid25870083">{{cite journal| author=Hooper SB, olglase GR, Roehr CC| title=Cardiopulmonary changes with aeration of the newborn lung. | journal=Paediatr Respir Rev | year= 2015 | volume= 16 | issue= 3 | pages= 147-50 | pmid=25870083 | doi=10.1016/j.prrv.2015.03.003 | pmc=4526381 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=25870083  }} </ref>
+*Deviations from these may result in [[pathological]] [[conditions]] requiring immediate [[interventions]]; [[infants]], especially those born prematurely, would require medical assistance for this phenomenal transition.<ref name="pmid25870083">{{cite journal| author=Hooper SB, olglase GR, Roehr CC| title=Cardiopulmonary changes with aeration of the newborn lung. | journal=Paediatr Respir Rev | year= 2015 | volume= 16 | issue= 3 | pages= 147-50 | pmid=25870083 | doi=10.1016/j.prrv.2015.03.003 | pmc=4526381 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=25870083  }} </ref>
-*In [[peripheral cyanosis]], there's normal SaO2 with a rise in [[oxygen]] uptake by tissues leading to a wide arteriovenous difference within the [[venous]] aspect of the [[capillaries]]. [[Vasoconstriction]] could be a cause. This kind of [[cyanosis]] is seen majorly at the [[extremities]].
+*In [[peripheral cyanosis]], there's normal SaO2 with a rise in [[oxygen]] uptake by the [[tissues]] leading to a wide arteriovenous difference within the [[venous]] aspect of the [[capillaries]]. [[Vasoconstriction]] could be a [[Causes|cause]]. This kind of [[cyanosis]] is seen majorly at the [[extremities]].
 ==Causes==
-*A systematic way of classifying the common causes of cyanosis in newborns is by using the '''ABC''' which stands for '''''[[Airway]]''''', '''''[[Breathing]]''''', and '''''[[Circulation]]'''''.
+*A structured way of grouping the common [[causes]] of [[cyanosis in newborns]] is by using the '''ABC''' which stands for '''''[[Airway]]''''', '''''[[Breathing]]''''', and '''''[[Circulation]]'''''.
 {{familytree/start}}
-{{familytree | | | | | | A01 | | | | | | | | | | | | | | |A01=Causes of [[cyanosis]] in [[newborns]]}}
+{{familytree | | | | | | A01 | | | | | | | | | | | | | | |A01=[[Causes]] of [[cyanosis]] in [[newborns]]}}
 {{familytree | |,|-|-|-|-|+|-|-|-|-|.| | | | | | | | | |}}
 {{familytree | B01 | | | B02 | | | B03 | | | | | | | | | | | |B01=[[Airway]]|B02=[[Breathing]]|B03=[[Circulation]]}}
 {{familytree | |!| | | | |!| | | | |!| | | | | | | | | |}}
-{{familytree | C01 | | | C02 | | | C03 | | | | | | | | | | | |C01=• [[Cystic hygroma]]<br>• [[Hemangioma]]<br>• [[Choanal atresia]]<br>• [[Micrognathia]]<br>• [[Laryngomalacia]]<br>• Tracheal [[stenosis]]<br>• [[Vascular rings]]<br>• [[Vocal cord]] [[paralysis]]<br>• Pierre Robin sequence|C02=• [[Phrenic nerve]] [[palsy]]<br>• [[Congenital diaphragmatic hernia]]<br>• Perinatal [[asphyxia]]<br>• Pulmonary hypoplasia<br>• Inborn errors of [[metabolism]]<br>• [[Central nervous system]] and muscle [[congenital anomalies]]<br>• [[Neonatal sepsis]]<br>• Neonatal [[botulism]]<br>• [[Congenital cystic adenomatoid malformation]]<br>• [[Pneumonia]]|C03=• [[Congenital heart diseases]]<br> [[Tetralogy of Fallot]]
+{{familytree | C01 | | | C02 | | | C03 | | | | | | | | | | | |C01=• [[Cystic hygroma]]<br>• [[Hemangioma]]<br>• [[Choanal atresia]]<br>• [[Micrognathia]]<br>• [[Laryngomalacia]]<br>• Tracheal [[stenosis]]<br>• [[Vascular rings]]<br>• [[Vocal cord]] [[paralysis]]<br>• [[Pierre Robin]] sequence|C02=• [[Phrenic nerve]] [[palsy]]<br>• [[Congenital diaphragmatic hernia]]<br>• [[Perinatal]] [[asphyxia]]<br>• [[Pulmonary]] [[hypoplasia]]<br>• [[Inborn errors of metabolism]]<br>• [[Central nervous system]] and [[muscle]] [[congenital anomalies]]<br>• [[Neonatal sepsis]]<br>• [[Neonatal]] [[botulism]]<br>• [[Congenital cystic adenomatoid malformation]]<br>• [[Pneumonia]]|C03=• [[Congenital heart diseases]]<br> [[Tetralogy of Fallot]]
-  (TOF)<br> [[Tricuspid atresia]]<br> [[Pulmonary atresia]]<br> [[Pulmonary stenosis]]<br> [[Ebstein's anomaly]]<br> [[Transposition of great arteries]] (TGA)<br> [[Hypoplastic left heart syndrome]]<br> [[Atrioventricular]] canal defect<br> Total anomalous pulmonary [[venous return]] (TAPVR)<br>• [[Anemia]]<br>• [[Methemoglobinemia]]<br>• [[Polycythemia]]<br>• Persistent [[pulmonary hypertension]]}}
+  ([[TOF]])<br> [[Tricuspid atresia]]<br> [[Pulmonary atresia]]<br> [[Pulmonary stenosis]]<br> [[Ebstein's anomaly]]<br> [[Transposition of great arteries]] ([[TGA]])<br> [[Hypoplastic left heart syndrome]]<br> [[Atrioventricular]] canal defect<br> Total anomalous [[pulmonary]] [[venous return]] (TAPVR)<br>• [[Anemia]]<br>• [[Methemoglobinemia]]<br>• [[Polycythemia]]<br>• Persistent [[pulmonary hypertension]]}}
 {{familytree | | | | | | | | | | | | | | | | | | | | | |}}
 {{familytree/end}}
@@ Line 120: / Line 120: @@
 ==Epidemiology and Demographics==
-*Persistent [[pulmonary hypertension]] of the [[newborn]] and [[Congenital heart diseases]] (CHD) are the common causes of [[newborn]] [[cyanosis]]. Common in older kids are [[respiratory]] [[diseases]]. <ref>https://pediatriccare.solutions.aap.org/chapter.aspx?sectionid=108722941&bookid=1626</ref> <ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
+*Persistent [[pulmonary hypertension]] of the [[newborn]] and [[Congenital heart diseases]] ([[CHD]]) are the common [[causes]] of [[newborn]] [[cyanosis]]. Common in older kids are [[respiratory]] [[diseases]].<ref>https://pediatriccare.solutions.aap.org/chapter.aspx?sectionid=108722941&bookid=1626</ref><ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
-*[[Tetralogy of Fallot]] (TOF) followed closely by the Transposition of Great Arteries ([[TGA]]) are the commonest causes of CHD.<ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
+*[[Tetralogy of Fallot]] ([[Tetralogy of Fallot|TOF]]) followed closely by the [[Transposition of the Great Arteries|Transposition of Great Arteries]] ([[TGA]]) are the commonest [[causes]] of [[CHD]].<ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
 ===Age===
-*[[Newborns]] are more prone to cyanosis due to the peculiarities of [[birth]] and the changes that occur during the [[transition]] from [[fetal]] to neonatal life and/or due to [[congenital]] or [[acquired]] [[disorders]].
+*[[Newborns]] are more prone to [[cyanosis]] due to the peculiarities of [[birth]] and the changes that occur during the [[transition]] from [[fetal]] to [[neonatal]] life and/or due to [[congenital]] or [[acquired]] [[disorders]].
-===Gender===
-*No documented evidence of gender predilection.
-===Race===
-*No particular racial tendency for [[cyanosis]] in [[newborns]].
 ==Risk Factors==
-*Common [[risk factors]] in the development of [[cyanosis]] in [[newborns]] are evident in the [[pregnancy]] and [[labor]] period. <ref>https://learn.pediatrics.ubc.ca/body-systems/neonate/approach-to-neonatal-cyanosis/</ref>
+*Common [[risk factors]] for the [[development]] of [[cyanosis]] in [[newborns]] are evident in the [[pregnancy]] and [[labor]] period.
-*[[Pregnancy]]-related [[risk factors]] are:
+*[[Pregnancy]]-related [[risk factors]] include:
-**Advanced age of the mother
+**Advanced [[age]] of the mother
 **[[Pregnancy-induced hypertension]]
 **[[Gestational diabetes]]
@@ Line 145: / Line 137: @@
 **[[Oligohydramnios]]
 **[[Polyhydramnios]]
-*[[Labor]] and [[birth]]-related risk factors are:
+*[[Labor]] and [[birth]]-related [[risk factors]] include:
 **[[Cesarean section]]
 **[[Preterm]]/[[prematurity]]
-**Use of [[Anesthetic agents|anesthetic]] drugs and/or [[sedatives]]
+**Use of [[Anesthetic agents|anesthetic]] [[drugs]] and/or [[sedatives]]
 **[[Premature rupture of membranes]] ([[PROM]])
 **[[Meconium aspiration syndrome|Meconium aspiration]]
-**Difficult/assisted vaginal delivery
+**Difficult/assisted [[vaginal]] [[delivery]]
 ==Natural History, Complications and Prognosis==
@@ Line 158: / Line 150: @@
 **[[Stroke]]
 **[[Sudden Cardiac Arrest]]
-**Repeated [[respiratory tract infections]] in [[infants]] with unrepaired [[heart defects]] which can be severe.
+**Repeated [[respiratory tract infections]] in [[infants]] with unrepaired [[heart defects]] which can be severe
 **[[Developmental delays]] ranging from [[Motor skill|motor]] to [[cognitive]]
-**Various forms of disabilities
+**Various forms of [[Disability|disabilities]]
 **[[Arrhythmias]]
 **[[Heart failure]]
-*Prompt recognition, and administration of [[treatment]] modalities, with appropriate referral to the ideal [[hospital]] setting equipped to manage the [[diagnosis]], can improve prognosis.
+*Prompt recognition, and administration of [[treatment]] modalities, with appropriate referral to the ideal [[hospital]] setting equipped to manage the [[diagnosis]], can improve the [[prognosis]].
-*[[Mortality]] is high in [[newborns]] with critical CHD however, there has been an encouraging improvement in one-year survival to 75% following advances in [[treatment]]. 69% of these [[babies]] can survive to the age of 18 years. <ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref><ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
+*[[Mortality]] is high in [[newborns]] with critical [[CHD]] however, there has been an encouraging improvement in one-year survival to 75% following advances in [[treatment]]. 69% of these [[babies]] can survive to the [[age]] of 18 [[Year|years]].<ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref><ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
 ==Diagnosis==
@@ Line 170: / Line 162: @@
 ===Symptoms===
-*Primary [[symptom]] is the bluish/dark colored lips, [[mucous membranes]], and/or hands and feet.
+*Primary [[symptom]] is the [[Bluish color of the lips or skin|bluish/dark colored lips]], [[mucous membranes]], and/or [[hands]] and [[feet]]
 *Other [[symptoms]] include the following:
-**Breathing difficulties such as:
+**[[Breathing difficulties]] evident as:
-***Nasal flaring
+***[[Nasal]] flaring
-***Chest retractions
+***[[Chest]] [[Retraction|retractions]]
 ***Fast [[breathing]]
-***Slow breathing
+***Slow [[breathing]]
-***[[Irregular]] breathing
+***[[Irregular]] [[breathing]]
-***History of momentary cessations of breathing
+***History of momentary cessations of [[breathing]]
 **Pausing/excessive [[sweating]] or [[crying]] while [[feeding]]
-**Small volume of feeds
+**Small [[volume]] of [[Feeding|feeds]]
-**Small for age/poor [[weight gain]]
+**Small for [[age]]/poor [[weight gain]]
-**Large for age
+**Large for [[age]]
-**Fixed/immobile arms suggesting [[paralysis]] from [[birth trauma]]
+**[[Fixation|Fixed]]/immobile [[Arm|arms]] suggesting [[paralysis]] from [[birth trauma]]
-**Increasing head cicumference with\without [[scalp]] [[injuries]] from a difficult [[delivery]]
+**Increasing [[head]] circumference with\without [[scalp]] [[injuries]] resulting from a difficult [[delivery]]
 **Hypo/[[hyperactive]] [[child]]
 ===Physical Examination===
-*[[Patients]] usually appear [[cyanotic]]
+*[[Patients]] usually [[Appearance|appear]] [[cyanotic]].
-*Other [[examination]] findings relates to the etiology which can include:
+*Depending on the underlying [[etiology]], other [[examination]] findings may include the following:
 **[[Lethargy]]
-**[[Conjunctival]] injection
+**[[Conjunctival]] [[injection]]
 **Features of [[shock]]
 **[[Tachypnea]]
-**Periodic breathing
+**Periodic [[breathing]]
-**Apneic spells
+**[[Apnea|Apneic]] spells
-**Use of accessory [[muscles]] of [[respiration]]
+**Use of [[accessory]] [[muscles]] of [[respiration]]
-**Flaring of the alar nasa
+**Flaring of the [[alar]] [[Nasal|nasa]]
-**Tube or [[catheter]] carefully inserted into the nasal cavity if suspicion is high for [[Choanal atresia]]
+**Tube or [[catheter]] carefully [[Insert|inserted]] into the [[nasal cavity]] if suspicion is high for [[choanal atresia]]
 **[[Tachycardia]]
-**Abnormal [[heart sounds]]/[[murmurs]]
+**[[Abnormal]] [[heart sounds]]/[[murmurs]]
-**Weak peripheral [[pulses]] especially [[femoral]]
+**[[Weak (thready) pulse|Weak peripheral pulses]] especially [[femoral]] [[pulse]]
 **Fine [[crackles]] in lower [[lung]] fields
 **[[Hepatomegaly]]
-**[[Scaphoid]] [[abdomen]](in [[diaphragmatic hernia]])
+**[[Scaphoid]] [[abdomen]] (in [[diaphragmatic hernia]])
-**Erb's [[paralysis]]
+**[[Erb's palsy|Erb's paralysis]]
 **[[Scalp]] [[injuries]]
 **[[Seizures]]
@@ Line 212: / Line 204: @@
 ===Laboratory Findings===
-*[[Complete blood count]] and differentials
+*[[Complete blood count]] and differentials:
-**↑Packed cell volume([[PCV increased|PCV]])- [[Polycythemia]]
+**[[Packed cell volume increased|Increased packed cell volume]] ([[PCV increased|PCV]])- [[polycythemia]]
-**↑[[White blood cells|White cell]] count- [[Septicemia]]
+**Increased [[White blood cells|white cell]] count- [[septicemia]]
 *Complete metabolic panel- [[electrolyte imbalance]] ([[metabolic acidosis]])
 *[[Serum glucose]]- hypo or [[hyperglycemia]]
-*[[Hyperoxia]] Test- differentiates [[pulmonary]] from a [[cardiovascular]] cause. An increase in [[PaO2]] to 100mmHg or more after administering 100% [[oxygen]] suggests a [[pulmonary]] [[etiology]]. Seldom used due to the availability of [[echocardiography]].
+*[[Hyperoxia]] Test- differentiates [[pulmonary]] from a [[cardiovascular]] cause. An increase in [[PaO2]] to a 100 mmHg or more after administering 100% [[oxygen]] suggests a [[pulmonary]] [[etiology]]. Seldom used due to the availability of [[echocardiography]].
-*[[Arterial]] [[Blood]] [[Gases]] (ABGs)
+*[[Arterial]] [[Blood]] [[Gases]] ([[ABG|ABGs]])
 **[[PaCO2]], ↑ suggests [[hypoventilation]] of [[CNS Disease|CNS]], [[pulmonary]] or [[cardiac]] [[etiology]].
 **[[PaO2]], ↓ confirms [[cyanosis]]
-**PH, a ↓ suggests [[hypoxemia]], [[sepsis]]
+**[[PH]], a ↓ pH suggests [[hypoxemia]],or/and [[sepsis]]
-**'Chocolate-brown' color of blood with normal levels of PaO2 and reduced SaO2 [[Methemoglobinemia]]
+**'[[Chocolate]]-[[brown]]' [[color]] of [[blood]] with [[normal]] levels of [[PaO2]] and reduced SaO2 [[methemoglobinemia]]
 ===Electrocardiogram===
-*It is seldom used however, may be helpful in the [[diagnosis]] of [[arrhythmias]] and [[dextrocardia]] to show a [[left axis deviation]] seen in [[Tricuspid atresia]] due to [[left ventricular hypertrophy]].
+*It is seldom used, however, may be helpful in the [[diagnosis]] of [[arrhythmias]] and [[dextrocardia]] to show a [[left axis deviation]] seen in [[tricuspid atresia]] due to [[left ventricular hypertrophy]].
-*It could give a normal reading in very serious heart defects like [[TGA]]. <ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
+*It could give a normal reading in very serious heart defects such as [[TGA]].<ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
 ===X-ray===
 *Can identify:
-**[[Pulmonary]] causes like [[pulmonary]] [[hypoplasia]]
+**[[Pulmonary]] [[causes]] such as [[pulmonary]] [[hypoplasia]]
 **Increased [[lung]] [[vascular]] markings in [[pulmonary edema]], [[bronchopneumonia]]
-**Reduced [[pulmonary]] markings in [[pulmonary atresia]], [[Pulmonary stenosis]], and persistent [[pulmonary hypertension]] of [[newborns]]
+**Reduced [[pulmonary]] markings in [[pulmonary atresia]], [[pulmonary stenosis]], and persistent [[pulmonary hypertension]] of [[newborns]]
 **Location of [[abdominal]] contents in [[diaphragmatic hernia]]
-**Elevation of the affected [[hemidiaphragm]] in [[phrenic nerve injury]]
+**Elevation of the affected hemidiaphragm in [[phrenic nerve]] [[injury]]
 **[[Cystic]] adenomatoid [[malformation]]
-*Characteristic features of some [[congenital heart diseases]] can be observed like:
+*Characteristic [[Features (pattern recognition)|features]] of some [[congenital heart diseases]] may be seen such as:
 **'Snowman' or 'Figure 8' in TAPVR
-**'Boot-shaped heart' in TOF
+**'Boot-shaped [[heart]]' in [[Tetralogy of Fallot|TOF]]
-**'Egg-on-string' in [[TGA]]
+**'[[Egg (biology)|Egg]]-on-string' in [[TGA]]
 **[[Cardiomegaly]] in [[Ebstein's anomaly]]
-[[File:Boot-shaped heart.jpg|thumb|300px|none| Boot-shaped heart in Tetralogy of Fallot. [https://medpix.nlm.nih.gov/search?allen=true&allt=true&alli=true&query=boot%20shaped%20heart]]]
 ===Echocardiography or Ultrasound===
-*Can be used when the diagnosis is equivocal or when [[physical exam]] findings and/or failed [[hyperoxia]] test suggests the presence of [[congenital heart disease]].
+*Can be used when the [[diagnosis]] is equivocal or when [[physical exam]] findings and/or failed [[hyperoxia]] test suggests the presence of [[congenital heart disease]].
-*It usually used with [[doppler]] to define the direction of [[shunts]]. <ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
+*It is usually used with [[doppler]] to define the [[direction]] of [[shunts]].<ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
 ===CT scan===
-*Used as an adjunct to further define [[cardiac]] and other [[anatomical]] anomalies in preparation for definitive management.
+*[[Usage analysis|Used]] as an adjunct to further define [[cardiac]] and other [[anatomical]] anomalies in [[Preparedness|preparation]] for the definitive management.
 ===MRI===
-*Used as an adjunct to further define [[cardiac]] and other  [[anatomical]] anomalies in preparation for definitive management.
+*Used as an adjunct to further define [[cardiac]] and other [[anatomical]] anomalies in [[Preparedness|preparation]] for the definitive management.
 ===Other Imaging Findings===
 *[[Cardiac catheterization]] and [[angiography]]:
-**Sometimes as an adjunct to further define [[cardiac]] and other [[anatomical]] anomalies in preparation for definitive management.
+**Sometimes used as an adjunct to further define [[cardiac]] and other [[anatomical]] anomalies in [[Preparedness (learning)|preparation]] for the definitive management.
 ===Other Diagnostic Studies===
-*Pre-ductal and post-ductal [[PaO2]] measurements
+*Pre-[[Duct (anatomy)|ductal]] and post-[[Duct (anatomy)|ductal]] [[PaO2]] measurements.
 ==Treatment==
 ===Medical Therapy===
-*The priority in the immediate term will be to optimize the [[neonate]], especially in severe [[cyanosis]]. This includes:
+*The immediate priority is to [[Optimization (mathematics)|optimize]] the [[neonate]], especially in severe [[cyanosis]]. This includes:
-**Establishing assisted [[ventilation]] in [[respiratory distress]]
+**Establishing assisted [[ventilation]] in [[respiratory distress]].
-**Keep [[infant]] in a radiant warmer
+**Keep [[infant]] in a [[Radiant energy|radiant]] warmer.
-**Stop all per oral feeds and give [[intravenous fluids]] through peripheral or central access like the [[umbilical vein]]
+**Stop all per [[oral]] [[Feeding|feeds]] and give [[intravenous fluids]] through peripheral or [[central]] [[Accessibility|access]] such as [[umbilical vein]].
-**Give [[glucose]] for [[hypoglycemic]] [[infants]] and monitor [[serum glucose]] levels
+**Give [[glucose]] for [[hypoglycemic]] [[infants]] and monitor [[serum glucose]] levels.
-**Consult should be sent to the [[Neonatologist]]
+**[[Consultation|Consult]] should be sent to the [[neonatologist]].
-**[[Oxygen]] administration should be done with caution. Care must be taken not to begin with very high [[concentrations]] of 100% due to damage to the [[lung]] tissue and [[pulmonary vessels]]
+**[[Oxygen]] administration should be done with caution. Care must be taken not to begin with very high [[concentrations]] of 100% due to damage to the [[lung]] tissue and [[pulmonary vessels]].
-**[[Prostaglandin]] E1([[PGE1]]) given as an infusion to keep the ductus patent for [[pulmonary]] [[blood]] flow in CHDs
+**[[Prostaglandin]] E1 ([[PGE1]]) given as an [[infusion]] to keep the [[Ductus arteriosus|ductus]] [[patent]] for [[pulmonary]] [[blood]] flow in [[CHD|CHDs]].
 **Definitive [[treatment]] can be planned in stages once [[infant]] is optimized and a [[diagnosis]] has been made.
-**[[Antibiotics]] coverage for [[sepsis]] if suspected. Give after [[blood]] samples are taken for [[Culture collection|culture]] and [[Sensitivity (tests)|sensitivity]], [[urine]] samples have been collected.
+**[[Antibiotics]] coverage for [[sepsis]] if suspected, after [[blood]] samples are taken for [[Culture collection|culture]] and [[Sensitivity (tests)|sensitivity]], and [[urine]] samples have been collected.
 ===Surgery===
-*This a [[treatment]] modality for diagnoses associated with [[anatomic]] [[deformities]] in CHDs or [[airway]] obstructions.
+*This a [[treatment]] modality for [[Diagnosis|diagnoses]] [[Association (statistics)|associated]] with [[anatomic]] [[deformities]] in [[CHD|CHDs]] or [[airway]] [[Obstruction|obstructions]].
-*[[Surgical]] [[treatment]] is tailored to the cause of the [[cyanosis]] that requires [[surgical]] intervention. An example is a Balloon Atrial Septostomy for acute [[TGA]] allowing for [[blood]] mixing. <ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
+*[[Surgical]] [[treatment]] is tailored to the underlying [[Causes|cause]] of [[cyanosis]] that requires [[surgical]] [[Intervention (counseling)|intervention]]. An example is a [[Balloon septostomy|Balloon Atrial Septostomy]] for [[acute]] [[TGA]] allowing for [[blood]] mixing.<ref name="pmid19727322">{{cite journal| author=Steinhorn RH| title=Evaluation and management of the cyanotic neonate. | journal=Clin Pediatr Emerg Med | year= 2008 | volume= 9 | issue= 3 | pages= 169-175 | pmid=19727322 | doi=10.1016/j.cpem.2008.06.006 | pmc=2598396 | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19727322  }} </ref>
 ===Prevention===
-*[[Prevention]] can be challenging as some of its [[causes]] would have been prevalent in-utero before the [[birth]] of the child while others occur during the actual [[labor]] and birthing process.
+*[[Prevention]] can be challenging as some of its [[causes]] are prevalent in-[[Uterus|utero]] before the [[birth]] of [[child]] while others occur during the actual [[labor]] and [[Birth|birthing]] [[Process (anatomy)|process]].
-*The following preventive measures can be adopted:
+*The [[Preventive care|preventive measures]] that can be adopted include:
-*[[Counsel]] [[expectant mothers]] especially women who are above the age of 35 years.
+*[[Counsel]] [[expectant mothers]] especially [[women]] who are above the [[age]] of 35 [[Year|years]].
-*Routine [[prenatal]] and [[postnatal]] care for early detection of [[congenital anomalies]] and adequate preparedness for its management during [[pregnancy]], [[labor]], and [[delivery]].
+*Routine [[prenatal]] and [[postnatal]] [[Care centers|care]] for early [[Detection theory|detection]] of [[congenital anomalies]] and adequate [[preparedness]] for its management during [[pregnancy]], [[labor]], and [[delivery]].
-*Early detection and management of [[gestational diabetes]] and [[pregnancy-induced hypertension]].
+*Early [[Detection theory|detection]] and management of [[gestational diabetes]] and [[pregnancy-induced hypertension]].
-*Parents of a child with [[congenital malformations]] should be counseled on the risk of having another child with the same or similar [[deformities]].
+*[[Parenting|Parents]] of a [[child]] with [[congenital malformations]] should be counseled on the [[RiskMetrics|risk]] of having another [[child]] with the same or similar [[deformities]].
-*[[Prophylaxis]] against [[Respiratory syncytial virus]]([[Human respiratory syncytial virus|RSV]]).
+*[[Prophylaxis]] against [[respiratory syncytial virus]] ([[Human respiratory syncytial virus|RSV]]).
 *Follow up for [[polycythemia]], excessive [[dehydration]], and [[iron-deficiency anemia]].<ref name="pmid29763177">{{cite journal| author=| title=StatPearls | journal= | year= 2020 | volume=  | issue=  | pages=  | pmid=29763177 | doi= | pmc= | url= }} </ref>
@@ Line 302: / Line 292: @@
 [[Category:Pediatrics]]
+[[Category:Primary care]]
+[[Category:Up-To-Date]]