* Pneumonia was first recognized by Hippocrates. It was first identified and described by Laennec in 1819.<ref name="Mackenzie2016">{{cite journal|last1=Mackenzie|first1=Grant|title=The definition and classification of pneumonia|journal=Pneumonia|volume=8|issue=1|year=2016|issn=2200-6133|doi=10.1186/s41479-016-0012-z}}</ref>
* Pneumonia was first recognized by Hippocrates. It was first identified and described by Laennec in 1819.
* In 1842, Rokitansky differentiated Pneumonia into Bronchopneumonia and Lobar Pneumonia.<ref name="Mackenzie20162">{{cite journal|last1=Mackenzie|first1=Grant|title=The definition and classification of pneumonia|journal=Pneumonia|volume=8|issue=1|year=2016|issn=2200-6133|doi=10.1186/s41479-016-0012-z}}</ref>
* In 1842, Rokitansky differentiated Pneumonia into Bronchopneumonia and Lobar Pneumonia.
== Classification[edit | edit source] ==
== Classification[edit | edit source] ==
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** Lobular (Bronchopneumonia)
** Lobular (Bronchopneumonia)
== Pathophysiology[edit | edit source] ==
== Pathophysiology[edit | edit source] ==
* The pathogenesis of Bronchopneumonia is characterized by inflammation of lung parenchyma.<ref name="Mackenzie20163">{{cite journal|last1=Mackenzie|first1=Grant|title=The definition and classification of pneumonia|journal=Pneumonia|volume=8|issue=1|year=2016|issn=2200-6133|doi=10.1186/s41479-016-0012-z}}</ref>
* The pathogenesis of Bronchopneumonia is characterized by inflammation of lung parenchyma.
* On gross pathology, multiple foci of consolidation is a characteristic feature of Bronchopneumonia. They are present bilaterally, most commonly in the basal lobes. These lesions are 2-4 cm in diameter, grey-yellow, dry, often centered by a [[bronchia]], are poorly delimited and have the tendency to confluence, especially in children.
* On gross pathology, multiple foci of consolidation is a characteristic feature of Bronchopneumonia. They are present bilaterally, most commonly in the basal lobes. These lesions are 2-4 cm in diameter, grey-yellow, dry, often centered by a [[bronchia]], are poorly delimited and have the tendency to confluence, especially in children.
* On microscopic histopathological analysis, a focus of inflammatory condensation, centered by a bronchiola with acute bronchiolitis is a characteristic finding in Bronchopneumonia. In addition, alveolar lumens surrounding the bronchia are filled with neutrophils and suppurative exudate("leukocytic alveolitis"), massive congestion is present and inflammatory foci are separated by normal, aerated parenchyma..
* On microscopic histopathological analysis, a focus of inflammatory condensation, centered by a bronchiola with acute bronchiolitis is a characteristic finding in Bronchopneumonia. In addition, alveolar lumens surrounding the bronchia are filled with neutrophils and suppurative exudate("leukocytic alveolitis"), massive congestion is present and inflammatory foci are separated by normal, aerated parenchyma.
* Bronchopneumonia is most commonly caused by pneumococcal serotypes 3, 7,8,10,18 and 20.
* Bronchopneumonia is most commonly caused by pneumococcal serotypes 3, 7,8,10,18 and 20.
* Common mechanisms in development of pneumonia include, micro-aspiration, hematogenous spread, spread from a contiguous focus and macro-aspiration.
* Common mechanisms in development of pneumonia include, micro-aspiration, hematogenous spread, spread from a contiguous focus and macro-aspiration.
* Bronchopneumonia is usually associated with infections due to gram-negative bacteria, ''Staphylococcus aureus'' and some fungi.
== Clinical Features[edit | edit source] ==
== Clinical Features[edit | edit source] ==
* Common clinical findings in Bronchopneumonia include cough, fever, chills, dyspnea, pleuritic chest pain and sputum production. However, many of these features may be absent in older patients.<ref name="Mackenzie20164">{{cite journal|last1=Mackenzie|first1=Grant|title=The definition and classification of pneumonia|journal=Pneumonia|volume=8|issue=1|year=2016|issn=2200-6133|doi=10.1186/s41479-016-0012-z}}</ref>
* Common clinical findings in Bronchopneumonia include cough, fever, chills, dyspnea, pleuritic chest pain and sputum production. However, many of these features may be absent in older patients.
* Bronchopneumonia can also case Gastrointestinal symptoms such as nausea, vomiting and diarrhea.
* Bronchopneumonia can also case Gastrointestinal symptoms such as nausea, vomiting and diarrhea.
* Older patients may also present with altered mental status.
* Older patients may also present with altered mental status.
== Differentiating [disease name] from other Diseases[edit | edit source] ==
== Differentiating [disease name] from other Diseases[edit | edit source] ==
* Lobular pneumonia must be differentiated from other diseases that cause similar clinical symptoms and interstitial infiltrates on chest x-ray such as:<ref name="WuytsCavazza2014">{{cite journal|last1=Wuyts|first1=W. A.|last2=Cavazza|first2=A.|last3=Rossi|first3=G.|last4=Bonella|first4=F.|last5=Sverzellati|first5=N.|last6=Spagnolo|first6=P.|title=Differential diagnosis of usual interstitial pneumonia: when is it truly idiopathic?|journal=European Respiratory Review|volume=23|issue=133|year=2014|pages=308–319|issn=0905-9180|doi=10.1183/09059180.00004914}}</ref>
* Lobular pneumonia must be differentiated from other diseases that cause similar clinical symptoms and interstitial infiltrates on chest x-ray such as:
:* Lobar pneumonia
:* Lobar pneumonia
:* Non-infectious lung conditions such as: Hypersensitivity pneumonitis, Collagen vascular disease, Asbestosis, Drug toxicities, Pulmonary fibrosis, Pulmonary edema, Pulmonary embolism and neoplastic lesions.
:* Non-infectious lung conditions such as: Hypersensitivity pneumonitis, Collagen vascular disease, Asbestosis, Drug toxicities, Pulmonary fibrosis, Pulmonary edema, Pulmonary embolism and neoplastic lesions.
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== Epidemiology and Demographics[edit | edit source] ==
== Epidemiology and Demographics[edit | edit source] ==
* The rate of Community acquired pneumonia is approximately 5.16-7.06 cases per 1000 individuals per year. <ref name="CillonizMartin-Loeches20162">{{cite journal|last1=Cilloniz|first1=Catia|last2=Martin-Loeches|first2=Ignacio|last3=Garcia-Vidal|first3=Carolina|last4=San Jose|first4=Alicia|last5=Torres|first5=Antoni|title=Microbial Etiology of Pneumonia: Epidemiology, Diagnosis and Resistance Patterns|journal=International Journal of Molecular Sciences|volume=17|issue=12|year=2016|pages=2120|issn=1422-0067|doi=10.3390/ijms17122120}}</ref>
* The rate of Community acquired pneumonia is approximately 5.16-7.06 cases per 1000 individuals per year.
=== Age[edit | edit source] ===
=== Age[edit | edit source] ===
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== Risk Factors[edit | edit source] ==
== Risk Factors[edit | edit source] ==
* Common risk factors in the development of Bronchopneumonia are Influenza infection, Alcohol abuse, Hyposplenism/splenectomy, smoking, COPD/Asthma and Immunocompromise. Additional risk factors include, homelessness, incarceration, pregnancy, crack cocaine use, opioid use and occupational welding.<ref name="pmid107068972">{{cite journal |vauthors=Nuorti JP, Butler JC, Farley MM, Harrison LH, McGeer A, Kolczak MS, Breiman RF |title=Cigarette smoking and invasive pneumococcal disease. Active Bacterial Core Surveillance Team |journal=N. Engl. J. Med. |volume=342 |issue=10 |pages=681–9 |date=March 2000 |pmid=10706897 |doi=10.1056/NEJM200003093421002 |url=}}</ref>
* Common risk factors in the development of Bronchopneumonia are Influenza infection, Alcohol abuse, Hyposplenism/splenectomy, smoking, COPD/Asthma and Immunocompromise. Additional risk factors include, homelessness, incarceration, pregnancy, crack cocaine use, opioid use and occupational welding.
* Risk factors for a complicated course include, older age, preexisting lung condition, immunodeficiency/AIDS, and acquisition of a nosocomial infection.
* Risk factors for a complicated course include, older age, preexisting lung condition, immunodeficiency/AIDS, and acquisition of a nosocomial infection.
== Natural History, Complications and Prognosis[edit | edit source] ==
== Natural History, Complications and Prognosis[edit | edit source] ==
* Early clinical features include sudden fever, chills, cough and chest pain.
* Early clinical features include sudden fever, chills, cough and chest pain.<ref name="Mackenzie20165" />
* If left untreated, patients with Bronchopneumonia may progress to develop tachypnea and increasing systemic toxicity. They may also progress to develop Lobar pneumonia.
* If left untreated, patients with Bronchopneumonia may progress to develop tachypnea and increasing systemic toxicity. They may also progress to develop Lobar pneumonia.
* Common complications of Bronchopneumonia include parapneumonic effusion, empyema, necrotizing pneumonia, lung abscess and metastatic infections such as endocarditis, septic arthritis, peritonitis, pericarditis and meningitis, and other cardiac complications.
* Common complications of Bronchopneumonia include parapneumonic effusion, empyema, necrotizing pneumonia, lung abscess and metastatic infections such as endocarditis, septic arthritis, peritonitis, pericarditis and meningitis, and other cardiac complications.
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* The diagnosis is made when clinical and radiological evidence suggests the presence of Bronchopneumonia.
* The diagnosis is made when clinical and radiological evidence suggests the presence of Bronchopneumonia.
=== Symptoms[edit | edit source] ===
=== Symptoms[edit | edit source] ===
*Symptoms of Bronchopneumonia may include the following:<ref name="Mackenzie20165">{{cite journal|last1=Mackenzie|first1=Grant|title=The definition and classification of pneumonia|journal=Pneumonia|volume=8|issue=1|year=2016|issn=2200-6133|doi=10.1186/s41479-016-0012-z}}</ref>
*Symptoms of Bronchopneumonia may include the following:
** Fever
** Fever
** Chills
** Chills
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** Shortness of breath
** Shortness of breath
=== Physical Examination[edit | edit source] ===
=== Physical Examination[edit | edit source] ===
* Physical examination may be remarkable for: <ref name="EvertsenBaumgardner2010">{{cite journal|last1=Evertsen|first1=Jennifer|last2=Baumgardner|first2=Dennis J|last3=Regnery|first3=Ann|last4=Banerjee|first4=Indrani|title=Diagnosis and management of pneumonia and bronchitis in outpatient primary care practices|journal=Primary Care Respiratory Journal|volume=19|issue=3|year=2010|pages=237–241|issn=1471-4418|doi=10.4104/pcrj.2010.00024}}</ref>
* Physical examination may be remarkable for:
** Fever
** Fever
** Respiratory rate >24 breaths/min (Tachypnea)
** Respiratory rate >24 breaths/min (Tachypnea)
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=== Imaging Findings[edit | edit source] ===
=== Imaging Findings[edit | edit source] ===
* Chest x-ray is the imaging modality of choice for Bronchopneumonia.
* Chest x-ray is the imaging modality of choice for Bronchopneumonia.
* On chest x-ray, Bronchopneumonia is characterized by multiple foci of isolated, acute consolidation, affecting one or more [[pulmonary]] lobes.
* On chest x-ray, Bronchopneumonia is characterized by peribronchial thickening and poorly defined air-space opacities. Inhomogeneous patchy areas of consolidation involving several lobes reflect more severe disease. When confluent, bronchopneumonia may resemble lobar pneumonia. <ref>{{Cite book|Muller NL, Fraser RS, Coleman NC, Pare PD. Radiologic Diagnosis of Diseases of the Chest. Philadelphia: WB Saunders Co; 2001.=}}</ref>
* In the case of a negative chest x-ray and a high clinical suspicion, HRCT scan may be used to confirm the diagnosis as it has a higher sensitivity and accuracy in detecting lesions and anatomical changes.
* In the case of a negative chest x-ray and a high clinical suspicion, HRCT scan may be used to confirm the diagnosis as it has a higher sensitivity and accuracy in detecting lesions and anatomical changes.
* In case of emergency where chest x-ray and HRCT cannot be performed, lung ultrasound performed by an experienced physician can yield findings.
*[[File:Bronchopneumonia caused by aspergillus.jpg|thumb|Posteroanterior chest radiograph reveals bilateral nonsegmental consolidations in the lingula and in the right upper and lower lobes. ''Aspergillus fumigatus'' was recovered from the sputum. <ref>{{Cite web|url=https://erj.ersjournals.com/content/18/1/196|title=Imaging of pneumonia: trends and algorithms|last=Franquet|first=T.|date=|website=|archive-url=|archive-date=|dead-url=|access-date=}}</ref>]]In case of emergency where chest x-ray and HRCT cannot be performed, lung ultrasound performed by an experienced physician can yield findings.
=== Other Diagnostic Studies[edit | edit source] ===
=== Other Diagnostic Studies[edit | edit source] ===
* Microbial analysis in Bronchopneumonia can be performed using techniques such as Blood culture, Sputum analysis, PCR and Urine antigen detection, however, pathogens are not commonly identified and empiric treatment should be started once the diagnosis is made.<ref name="CillonizMartin-Loeches2016">{{cite journal|last1=Cilloniz|first1=Catia|last2=Martin-Loeches|first2=Ignacio|last3=Garcia-Vidal|first3=Carolina|last4=San Jose|first4=Alicia|last5=Torres|first5=Antoni|title=Microbial Etiology of Pneumonia: Epidemiology, Diagnosis and Resistance Patterns|journal=International Journal of Molecular Sciences|volume=17|issue=12|year=2016|pages=2120|issn=1422-0067|doi=10.3390/ijms17122120}}</ref>
* Microbial analysis in Bronchopneumonia can be performed using techniques such as Blood culture, Sputum analysis, PCR and Urine antigen detection, however, pathogens are not commonly identified and empiric treatment should be started once the diagnosis is made.
== Treatment[edit | edit source] ==
== Treatment[edit | edit source] ==
=== Medical Therapy[edit | edit source] ===
=== Medical Therapy[edit | edit source] ===
* The mainstay of therapy for Bronchopneumonia is antibiotics and supportive care.<ref name="pmid17278083">{{cite journal |vauthors=Mandell LA, Wunderink RG, Anzueto A, Bartlett JG, Campbell GD, Dean NC, Dowell SF, File TM, Musher DM, Niederman MS, Torres A, Whitney CG |title=Infectious Diseases Society of America/American Thoracic Society consensus guidelines on the management of community-acquired pneumonia in adults |journal=Clin. Infect. Dis. |volume=44 Suppl 2 |issue= |pages=S27–72 |date=March 2007 |pmid=17278083 |doi=10.1086/511159 |url=}}</ref>
* The mainstay of therapy for Bronchopneumonia is antibiotics and supportive care.
* Choice of antibiotics is dependent on epidemiology of microbes, resistance and patients' co-morbidities and severity of illness.<ref name="pmid172780832">{{cite journal |vauthors=Mandell LA, Wunderink RG, Anzueto A, Bartlett JG, Campbell GD, Dean NC, Dowell SF, File TM, Musher DM, Niederman MS, Torres A, Whitney CG |title=Infectious Diseases Society of America/American Thoracic Society consensus guidelines on the management of community-acquired pneumonia in adults |journal=Clin. Infect. Dis. |volume=44 Suppl 2 |issue= |pages=S27–72 |date=March 2007 |pmid=17278083 |doi=10.1086/511159 |url=}}</ref>
* Choice of antibiotics is dependent on epidemiology of microbes, resistance and patients' co-morbidities and severity of illness.
* In patients without co-morbidities Macrolides such as Azithromycin and Clarithromycin can be used. In the case of Macrolide resistant pneumonias and patients with multiple co-morbidities, Doxycycline, Amoxicillin-Clavulanate, and Cephalosporins such as Cefpodoxime and Cefuroxime may be used.<ref name="pmid172780833">{{cite journal |vauthors=Mandell LA, Wunderink RG, Anzueto A, Bartlett JG, Campbell GD, Dean NC, Dowell SF, File TM, Musher DM, Niederman MS, Torres A, Whitney CG |title=Infectious Diseases Society of America/American Thoracic Society consensus guidelines on the management of community-acquired pneumonia in adults |journal=Clin. Infect. Dis. |volume=44 Suppl 2 |issue= |pages=S27–72 |date=March 2007 |pmid=17278083 |doi=10.1086/511159 |url=}}</ref>
* In patients without co-morbidities Macrolides such as Azithromycin and Clarithromycin can be used. In the case of Macrolide resistant pneumonias and patients with multiple co-morbidities, Doxycycline, Amoxicillin-Clavulanate, and Cephalosporins such as Cefpodoxime and Cefuroxime may be used.
* Response to antibiotics can be monitored with clinical improvement, serum inflammatory markers and chest x-ray findings. However, most non-complicated pneumonias are treated out-patient and only require two follow up treatments to clinically determine improvement and resolution of the pneumonia, respectively. Follow-up chest x-rays are only required in male patients over the age of 50 years and smokers.<ref name="pmid172780834">{{cite journal |vauthors=Mandell LA, Wunderink RG, Anzueto A, Bartlett JG, Campbell GD, Dean NC, Dowell SF, File TM, Musher DM, Niederman MS, Torres A, Whitney CG |title=Infectious Diseases Society of America/American Thoracic Society consensus guidelines on the management of community-acquired pneumonia in adults |journal=Clin. Infect. Dis. |volume=44 Suppl 2 |issue= |pages=S27–72 |date=March 2007 |pmid=17278083 |doi=10.1086/511159 |url=}}</ref>
* Response to antibiotics can be monitored with clinical improvement, serum inflammatory markers and chest x-ray findings. However, most non-complicated pneumonias are treated out-patient and only require two follow up treatments to clinically determine improvement and resolution of the pneumonia, respectively. Follow-up chest x-rays are only required in male patients over the age of 50 years and smokers.
=== Prevention[edit | edit source] ===
=== Prevention[edit | edit source] ===
* Effective measures for the primary prevention of Bronchopneumonia include vaccination against influenza and pneumococcal antigens, and smoking cessation. Pneumococcal vaccination is indicated in patients over the age of 65 years. <ref name="pmid10706897">{{cite journal |vauthors=Nuorti JP, Butler JC, Farley MM, Harrison LH, McGeer A, Kolczak MS, Breiman RF |title=Cigarette smoking and invasive pneumococcal disease. Active Bacterial Core Surveillance Team |journal=N. Engl. J. Med. |volume=342 |issue=10 |pages=681–9 |date=March 2000 |pmid=10706897 |doi=10.1056/NEJM200003093421002 |url=}}</ref>
* Effective measures for the primary prevention of Bronchopneumonia include vaccination against influenza and pneumococcal antigens, and smoking cessation. Pneumococcal vaccination is indicated in patients over the age of 65 years.
== References[edit | edit source] ==
* Abbas, Abul K, Kumar, Vinay and Fausto, Nelson. Robbins and Coltran Pathologic Basis of Disease, 7th ed. Philadelphia: Elsevier Saunders, 2005.
Pneumonia was first recognized by Hippocrates. It was first identified and described by Laennec in 1819.
In 1842, Rokitansky differentiated Pneumonia into Bronchopneumonia and Lobar Pneumonia.
Classification[edit | edit source]
Pneumonia may be classified according to anatomic distribution of consolidation into two subtypes/groups:
Lobar
Lobular (Bronchopneumonia)
Pathophysiology[edit | edit source]
The pathogenesis of Bronchopneumonia is characterized by inflammation of lung parenchyma.
On gross pathology, multiple foci of consolidation is a characteristic feature of Bronchopneumonia. They are present bilaterally, most commonly in the basal lobes. These lesions are 2-4 cm in diameter, grey-yellow, dry, often centered by a bronchia, are poorly delimited and have the tendency to confluence, especially in children.
On microscopic histopathological analysis, a focus of inflammatory condensation, centered by a bronchiola with acute bronchiolitis is a characteristic finding in Bronchopneumonia. In addition, alveolar lumens surrounding the bronchia are filled with neutrophils and suppurative exudate("leukocytic alveolitis"), massive congestion is present and inflammatory foci are separated by normal, aerated parenchyma.
Bronchopneumonia is most commonly caused by pneumococcal serotypes 3, 7,8,10,18 and 20.
Common mechanisms in development of pneumonia include, micro-aspiration, hematogenous spread, spread from a contiguous focus and macro-aspiration.
Bronchopneumonia is usually associated with infections due to gram-negative bacteria, Staphylococcus aureus and some fungi.
Clinical Features[edit | edit source]
Common clinical findings in Bronchopneumonia include cough, fever, chills, dyspnea, pleuritic chest pain and sputum production. However, many of these features may be absent in older patients.
Bronchopneumonia can also case Gastrointestinal symptoms such as nausea, vomiting and diarrhea.
Older patients may also present with altered mental status.
Differentiating [disease name] from other Diseases[edit | edit source]
Lobular pneumonia must be differentiated from other diseases that cause similar clinical symptoms and interstitial infiltrates on chest x-ray such as:
Lobar pneumonia
Non-infectious lung conditions such as: Hypersensitivity pneumonitis, Collagen vascular disease, Asbestosis, Drug toxicities, Pulmonary fibrosis, Pulmonary edema, Pulmonary embolism and neoplastic lesions.
Other types of pneumonias such as: cryptogenic pneumonia.
Epidemiology and Demographics[edit | edit source]
The rate of Community acquired pneumonia is approximately 5.16-7.06 cases per 1000 individuals per year.
Age[edit | edit source]
Patients of all age groups may develop Bronchopneumonia.
Bronchopneumonia is more commonly observed among elderly patients.
Gender[edit | edit source]
Brochopneumonia is more commonly observed in men than women.
Race[edit | edit source]
Bronchopneumonia is more commonly observed in Black persons than caucasians.
Risk Factors[edit | edit source]
Common risk factors in the development of Bronchopneumonia are Influenza infection, Alcohol abuse, Hyposplenism/splenectomy, smoking, COPD/Asthma and Immunocompromise. Additional risk factors include, homelessness, incarceration, pregnancy, crack cocaine use, opioid use and occupational welding.
Risk factors for a complicated course include, older age, preexisting lung condition, immunodeficiency/AIDS, and acquisition of a nosocomial infection.
Natural History, Complications and Prognosis[edit | edit source]
Early clinical features include sudden fever, chills, cough and chest pain.[1]
If left untreated, patients with Bronchopneumonia may progress to develop tachypnea and increasing systemic toxicity. They may also progress to develop Lobar pneumonia.
Common complications of Bronchopneumonia include parapneumonic effusion, empyema, necrotizing pneumonia, lung abscess and metastatic infections such as endocarditis, septic arthritis, peritonitis, pericarditis and meningitis, and other cardiac complications.
Diagnosis[edit | edit source]
Diagnostic Criteria[edit | edit source]
The diagnosis is made when clinical and radiological evidence suggests the presence of Bronchopneumonia.
Symptoms[edit | edit source]
Symptoms of Bronchopneumonia may include the following:
Fever
Chills
Cough
Chest Pain
Shortness of breath
Physical Examination[edit | edit source]
Physical examination may be remarkable for:
Fever
Respiratory rate >24 breaths/min (Tachypnea)
Tachycardia
Chest Examination:
Audible crackles
Decreased or bronchial breath sounds
Dullness to percussion in areas of consolidation
Tactile fremitus
Egophony
Laboratory Findings[edit | edit source]
There are no specific laboratory findings associated with Bronchopneumonia.
A Leukocytosis (15000-30000 per mm3) with a left ward shift on a blood test can aid in diagnosis of Bronchopneumonia.
An elevated concentration of ESR or CRP is a non-specific indication of inflammation in the body.
Imaging Findings[edit | edit source]
Chest x-ray is the imaging modality of choice for Bronchopneumonia.
On chest x-ray, Bronchopneumonia is characterized by peribronchial thickening and poorly defined air-space opacities. Inhomogeneous patchy areas of consolidation involving several lobes reflect more severe disease. When confluent, bronchopneumonia may resemble lobar pneumonia. [2]
In the case of a negative chest x-ray and a high clinical suspicion, HRCT scan may be used to confirm the diagnosis as it has a higher sensitivity and accuracy in detecting lesions and anatomical changes.
Posteroanterior chest radiograph reveals bilateral nonsegmental consolidations in the lingula and in the right upper and lower lobes. Aspergillus fumigatus was recovered from the sputum. [3]In case of emergency where chest x-ray and HRCT cannot be performed, lung ultrasound performed by an experienced physician can yield findings.
Other Diagnostic Studies[edit | edit source]
Microbial analysis in Bronchopneumonia can be performed using techniques such as Blood culture, Sputum analysis, PCR and Urine antigen detection, however, pathogens are not commonly identified and empiric treatment should be started once the diagnosis is made.
Treatment[edit | edit source]
Medical Therapy[edit | edit source]
The mainstay of therapy for Bronchopneumonia is antibiotics and supportive care.
Choice of antibiotics is dependent on epidemiology of microbes, resistance and patients' co-morbidities and severity of illness.
In patients without co-morbidities Macrolides such as Azithromycin and Clarithromycin can be used. In the case of Macrolide resistant pneumonias and patients with multiple co-morbidities, Doxycycline, Amoxicillin-Clavulanate, and Cephalosporins such as Cefpodoxime and Cefuroxime may be used.
Response to antibiotics can be monitored with clinical improvement, serum inflammatory markers and chest x-ray findings. However, most non-complicated pneumonias are treated out-patient and only require two follow up treatments to clinically determine improvement and resolution of the pneumonia, respectively. Follow-up chest x-rays are only required in male patients over the age of 50 years and smokers.
Prevention[edit | edit source]
Effective measures for the primary prevention of Bronchopneumonia include vaccination against influenza and pneumococcal antigens, and smoking cessation. Pneumococcal vaccination is indicated in patients over the age of 65 years.
