Monday, January 29, 2018

Postpartum Endometritis

Any postpartum women presenting with persistent fever of >38.0C should be assumed to have a genital tract infection until proven otherwise. Other common sources of fever include respiratory tract infection, UTIs, mastitis, and thrombophlebitis. However, Pelvic infection is the most common serious complication of the puerperium.

Risk factors of Postpartum Endometritis

  • Cesarean Section
  • Multiple Gestation
  • Younger maternal age
  • Prolonged labour and PROM
  • Internal fetal monitoring
  • Digital examination 
  • Immunocompromised state


Common Bugs (reside in the bowel and colonize the perineum, vagina, and cervix) 
  • Gram-positive and gram-negative aerobes, anaerobes
  • Chlamydia trachomatis, and Neisseria gonorrhoea
  • Gardnerella vaginalis is isolated more often in younger women. 
  • MRSA

Many infections are polymicrobial
Clinical Presentation
  • Fever 38.0C 
  • Foul-smelling loch
  • Leukocytosis
  • Tachycardia
  • Uterine tenderness

ED Management
  • ABC
  • General Sepsis Care (Fluids, Antibiotics, Cultures, Septic Screen). Combination of Ampicillin or Clindamycin plus gentamicin is sufficient for 90% of patients
  • Drainage of abscesses and purulent material or debridement of necrotic tissue 
  • OBGYN Consultation 
Complications of endometritis include parametrical spread of infection, pelvic abscesses; infected hematomas; septic pelvic thrombophlebitis; necrotizing fasciitis; and peritonitis. 

Posted by:

              
     Lakshay Chanana
     
     Speciality Doctor
     Northwick Park Hospital
     Department of Emergency Medicine
     England

     @EMDidactic

  

Monday, January 22, 2018

Acute Aortic Syndromes

Background
Acute aortic dissection is part of a spectrum of diseases referred to as Acute Aortic Syndromes which basically encompasses 3 related conditions: 

(1) Aortic dissection
(2) Intramural hematoma (lacks blood flow in the false lumen or its lack of an intimal flap or entry point. Believed to originate from a rupture of the vasa vasorum within the medial layer; or from microscopic intimal tears )
(3) Penetrating atherosclerotic ulcer (typically seen in older population and often found incidentally, may progress to intramural hematoma)


The pathology, diagnosis, and treatment of these three entities are similar

Presentation
While aortic dissection usually presents with severe pain, its presentation can be more subtle and should be considered in anyone with chest pain, back pain or abdominal pain and pain with either syncope or focal neurological deficits.  Aortic dissection can also present as an acute stroke. There are 2 main anatomic classification systems: 




Stanford type B dissections are further classified as:
1. Complicated - Radiographic evidence of thoracic aortic rupture (eg, blood outside the aortic wall); ischemia involving the viscera, kidneys, spinal cord, or lower extremities; persistent pain; or rapid expansion in the distal arch or proximal descending aorta to a total aortic diameter of > 4.5 cm. These findings require immediate intervention due to the threat to life and limb.
2. Uncomplicated


The dissection creates a new false lumen, which separates the media from the adventitia and can extend either anterograde or retrograde involving the aortic root, arch, or any of the main aortic branches. The false lumen may compress the true lumen and compromise blood flow to distal arteries and causing ischemic complications such as renal failure, stroke, spinal infarction, limb ischemia, and myocardial events.

Classically, aortic dissection will present with abrupt chest or back pain, but about  5% of patients with an acute aortic dissection will have no pain. 


Aortic dissection should always be considered in the differential diagnosis of patients with suspected acute coronary syndromes or pulmonary embolism. 

Atypical presentations can also occur. 
  • Syncope has been reported in up to about 20% of patients
  • Acute neurological deficits or coma occur in 30% of patients presenting with an acute type A dissection. Neurological findings can be associated with aortic dissections secondary to the extension of the dissection into the aortic branches. These branches can be occluded by either expansion of the false lumen occluding the true lumen or by emboli from an expanding thrombus. Deficits may occur from insults to the brain or spinal cord.

  • Patients may be hypertensive (49%), normo- tensive (35%) orhypotensive (8%), or in shock (8%). The presence of hypotension or shock is an ominous finding. 
  • Blood pressure discrepancy can occur when a dissection extends into a branch of the aorta occluding the subclavian artery. A difference of 20 mm Hg between arms is considered positive and can be suggestive of an aortic dissection (this finding cannot be used to rule out dissection); however, 20% of the population will have a blood pressure differential without an aortic dissection.
  • pulse deficit is defined as having weak or no pulse on the affected side. However, data from the IRAD database of 2538 patients founda pulse de cit or blood pressure differential in only 20% of patients.
  • An aortic dissection may extend retrograde and involve the aortic valve or coronary arteries. A diastolic murmur can be heard in about 1/3rd of patients with an aortic dissection and may represent severe aortic regurgitation but the presence of a diastolic murmur is neither sensi- tive nor specific for aortic dissection.
  • 2-5% of patients with aortic dissections will have concurrent myocardial ischemia. Proximal aortic dissections can dissect into the right coronary artery, causing occlusion, and can present with a STEMI. If clinical suspicion for aortic dissection is present, other diagnostic modalities should be used to evaluate for proximal aortic dissection prior to anticoagulation or thrombolytics. 

Risk Factors
  • Poorly controlled hypertension
  • Connective tissue disorders (eg, Marfan syndrome, Ehlers-Danlos syndrome)
  • Congenital valvular disorders (eg, bicuspid aortic valve)
  • Aortic coarctation
  • Homocystinuria
  • Previous cardiac surgery
  • Familial aortic dissections, aortic aneurysms
  • Pheochromocytoma
  • inflammatory vasculitis
  • Sympathomimetics (eg, cocaine)
  • Cardiac surgery (eg, aortic valve replacement, coronary artery bypass grafting) or percutaneous catheter placement (eg, cardiac catheterisation),

Diagnosis

D-Dimer
More and more evidence is accumulating in support of the use of D-dimer as a screening tool for aortic dissection but currently, only a few small studies have looked at the sensitivity of D-dimer in ruling out aortic dissection (need further validation). Also, Intramural hematoma or aortic dissections with a thrombosed false lumen can have a false negative D-dimer. If there is sufficient clinical suspicion for an acute aortic dissection, advanced imaging is indicated. 


A Negative D-dimer cannot rule out Aortic Dissection


Imaging Modalities for Acute Aortic Syndrome



CXR
Chest radiography can suggest an aortic dissection. Abnormalities are seen in approxi- lately about 88% of patients. A widened mediastinum is commonly associated with aortic dissection and is seen in approximately 60% of patients. 


A normal CXR cannot rule out an aortic dissection.


Treatment
  • ABCs
  • Adequate Pain Relief (Morphine or Fentanyl)
  • Target HR< 60 beats/min and Target SBP  between 100-120 mm Hg. Always start with Beta Blockers first (not vasodilators)
  • In case of cocaine toxicity, use benzodiazepines to decrease the sympathetic drive.
  • Type and Screen
  • If hypotensive with poor perfusion then use inotropes (can potentially worsen dissection due to increase in shearing forces) or consider pericardicentesis in cases of tamponade (poor prognosis)
  • Emergent Vascular Surgery Consultation - Type A acute aortic dissections require prompt surgical treatment. Definitive treatment of type B acute aortic dissections is unclear. Uncomplicated distal dissections have traditionally been treated with blood pressure control. Surgery has been reserved for patients who have persistent pain, uncontrolled hypertension, occlusion of a major arterial trunk, frank aortic leaking or rupture, or development of a localized aneurysm. 

Rationale for Beta-Blockers FirstAortic wall stress is directly affected by the velocity of ventricular contraction over time (dP/dt). Initiation of treatment to decrease these shear forces should occur as soon as the diagnosis is made or suspected.intravenous narcotics should also be given and titrated to pain control.  Beta-blocker therapy should be given prior to initiating intravenous vasodilators to prevent reflex tachycardia. However, in cases of severe aortic regurgitation, use of intravenous beta blockers or calcium-channel blockers with caution.  

Chronic Dissection
Patients who present with chronic aortic dissection have already survived their period of greatest mortality risk and are usually treated by blood pressure control and close monitoring unless complications mandate surgery. All patients who have sustained and survived an aortic dissection, regardless of the type of definitive therapy used, require careful long-term surveillance and treatment. 


Documentation:
  • Document HPI with pertinent negative findings
  • Presence of Absence of risk factors
  • Listen for bruits
  • Pulsate Mass, BP difference in lies or any pulse deficits
  • Neuro Exam and CXR, ECHO findings

Take Home
  • Use your gestalt to work up dissections. Read more here on ADvISED Trial.   Currently, no validated clinical decision rule exists to rule out an acute aortic dissection. Historical and physical exam can be used to increase or decrease probability, but atypical presentations are common. 
  • Aortic dissection should always be in the differential for patients with chest pain, back pain, or abdominal pain.
  • Once the diagnosis is made or strongly suspected, ED Management is limited to pain relief, HTN and BP control and urgent Vascular surgery consulnation.
  • D-dimer and CXR alone should not be used to “rule out” aortic dissection. POCUS can be helpful in unstable patients but it should not be relied upon to rule out an aortic dissection. 

   References and Further Reading:
  1. Friado FJ. Aortic dissection: a 250-year perspective. Tex Heart Inst J. 2011;38(6):694-700. (Review)
  2. Hagan PG, Nienaber CA, Isselbacher EM, et al. The Inter- national Registry of Acute Aortic Dissection (IRAD): new insights into an old disease. JAMA. 2000;283(7):897-903. (Retrospective; 464 patients)
  3. 2010 ACCF/AHA/AATS/ACR/ASA/SCA/SCAI/SIR/ STS/SVM guidelines for the diagnosis and management of patients with thoracic aortic disease: a report of the Ameri- can College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines, American As- sociation for Thoracic Surgery, American College of Radiol- ogy, American Stroke Association, Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and Interventions, Society of Interventional Radiology, Soci- ety of Thoracic Surgeons, and Society for Vascular Medicine. Circulation. 2010;121(13):1544-1579. (Guideline) 
  4. Mancini MC. Aortic dissection. Medscape. Available at: http://emedicine.medscape.com/article/2062452-overview.
  5. Accessed June 10, 2013. (Review)
  6. Hardie AD, Wineman RW, Nandalur KR. The natural his- tory of acute non-traumatic aortic diseases. Emerg Radiol. 2009;16(2):87-95. (Review) 
  7. Collins JS, Evangelista A, Nienaber CA, et al. Differences in clinical presentation, management, and outcomes of acute type A aortic dissection in patients with and without previ- ous cardiac surgery. Circulation. 2004;110(11 suppl 1):II237- II242. (Retrospective; 617 patients) 
  8. Bossone E, Rampoldi V, Nienaber CA, et al. Usefulness of pulse de cit to predict inhospital complications and mortal- ity in patients with acute type A aortic dissection. Am J Cardiol. 2002;89(7):851-855. (Retrospective; 513 patients) Rogers AM, Hermann LK, Booher AM, et al. Sensitivity of the aortic dissection detection risk score, a novel guideline- based tool for identi cation of acute aortic dissection at initial presentation: results from the international registry of acute aortic dissection. Circulation. 2011;123(20):2213-2218.
  9. Lo BM. An evidence-based approach to acute aortic syndromes. Emergency medicine practice. 2013 Dec 1;15(12):1-23.

Posted by:

              
     Lakshay Chanana
     
     Speciality Doctor
     Northwick Park Hospital
     Department of Emergency Medicine
     England

     @EMDidactic

  

Monday, January 15, 2018

The "qRBBB" pattern

Presence of qRBBB in the setting of acute coronary syndrome signifies proximal occlusion of left descending coronary artery with compromise of circulation in the septal arteries supplying the bundle branches. Anterior STEMi with RBBB is associated with a higher risk of death when compared with that of patients with normal conduction. 

qRBBB with LAFBInstead of the rSR pattern (seen in RBBB), there is qRBBB pattern in V1 because the initial r wave has been knocked off by anterior wall myocardial infarction. 


Due to anterior location of the right ventricle than that of the left ventricle, activation of the right ventricular free wall can neutralize the abnormal septal forces associated with an anteroseptal MI. Therefore, in most patients with an anteroseptal infarction, abnormal Q waves in right precordial leads is mostly manifest during RBBB showing the classical qRBBB pattern, due to delayed activation of the right ventricle. 






Understanding RBBB

RBBB causes delayed depolarisation of right Ventricle as depolarisation spreads across the septum (instead of the Right Bundle) taking longer than usual. This produces characteristic ECG changes described below in the diagnostic criteria. Left Ventricle depolarisation remains normal i.e normal early part of QRS complex. 




Diagnostic Criteria 

  • Broad QRS > 120 ms
  • RSR’ pattern in V1-3 (‘M-shaped’ QRS complex) or a broad monophonic r wave or a qR complex
  • Wide, slurred S wave in the lateral leads (I, aVL, V5-6
  • Delayed intrinsicoid deflection time 


RBBB (Image from LIFTL)
RBBB often shows STD and TWI in V1-3 due to secondary depolarisation abnormalities 

Causes
  • Ischemic Heat Disease
  • Acute Pulmonary HTN (PE)
  • Chronic Pulmonary HTN (Cor Pulmonale)
  • Valvular Heart Disease
  • Myocarditis
  • Degenerative Diseases of conduction system
  • Congenital Heart Disease
  • Overdose of Na Channel Blockers
  • Idiopathic
  • Transient and Rate Related 

RBBB should NOT have any ST Elevation. Look for the qRBBB pattern and RBBB with LAFB (Leftward Axis, qR in lead I, aVL, rS in lead III) pattern. 

qRBBB in V1-4 with STE (Image from TheECGinAcuteMI)
Take Home:
  • Remember the qRBBB pattern morphology
  • RBBB should never have any ST elevation 
  • When in doubt, do serial ECGs and screening bedside ECHO to look for RWMA

References and Further Reading:
  1. Mishra, V., Sinha, S. K., & Razi, M. (2016). Right Bundle Branch Block: A Masquerader in Acute Coronary Syndrome. North American Journal of Medical Sciences8(2), 121–122. http://doi.org/10.4103/1947-2714.177347
  2. 2. Widimsky P, Rohác F, Stásek J, Kala P, Rokyta R, Kuzmanov B, et al. Primary angioplasty in acute myocardial infarction with right bundle branch block: Should new onset right bundle branch block be added to future guidelines as an indication for reperfusion therapy? Eur Heart J. 2012;33:86–95.
  3. Ganesan S, Kannan K, Victor A, Selvan KT, Arun R, Majella JC, Kumar RS, Aravind A, Viswanathan N, District V. QRBBB in acute coronary syndrome: Does it matter in modern era? Angiographic correlation. Indian Heart Journal. 2015 Dec 1;67:S38.
  4. Wong CK, Stewart RA, Gao W, French JK, Raffel C, White HD. Prognostic differences between different types of bundle branch block during the early phase of acute myocardial infarction: Insights from the Hirulog and Early Reperfusion or Occlusion (HERO)-2 trial. Eur Heart J. 2006;27:21–8. 
  5. http://hqmeded-ecg.blogspot.co.uk/2010/01/right-bundle-branch-block-with-subtle.html
  6. http://hqmeded-ecg.blogspot.co.uk/2017/04/rbbb-with-transient-st-elevation.html
  7. http://hqmeded-ecg.blogspot.co.uk/2010/11/wide-complex-tachycardia-its-really.html
  8. http://hqmeded-ecg.blogspot.co.uk/2014/03/elderly-woman-in-shock-ekg-from.html
  9. https://emcrit.org/wp-content/uploads/2015/03/Who-to-PCI-by-Smith-and-Weingart.pdf
  10. https://lifeinthefastlane.com/ecg-library/basics/right-bundle-branch-block/

Posted by:

              
     Lakshay Chanana
     
     Speciality Doctor
     Northwick Park Hospital
     Department of Emergency Medicine
     England

     @EMDidactic

Monday, January 8, 2018

Croup - Laryngotracheobronchitis

Viral Laryngotracheobronchitis (Croup) is the most common cause of stridor commonly affecting children between 6 months to 6 years old, with a peak in the fall and early winter months. Croup is acquired through inhalation of the virus. 

Possible agents could be parainfluenza virus (most common), rhinovirus. enterovirus, respiratory syncytial virus, influenza virus and human metapneumovirus.


Clinical Presentation 
Typically, symptoms begin after 1 to 3 days of URTI symptoms (nasal congestion, rhinorrhea, cough, and low-grade fever). Classic symptoms include a harsh barking cough, hoarse voice, and stridor. Symptoms often tend to be worse at night and the severity of symptoms is related to the amount of edema and inflammation of the airway. 


Diagnosis and Assessment of Severity 
Look for tachypnea, stridor at rest, nasal flaring, retractions, lethargy or agitation, and oxygen desaturation. Symptoms are most severe on 3rd or 4th day of illness. Agitation and crying increase oxygen demand and may worsen airway compromise. Bloods and imaging are only required in children who fail to respond to conventional therapy. X Rays may demonstrate “steeple sign” (subglottic narrowing)


Steeple Sign
Croup is a clinical diagnosis
Steeple sign may be present in normal children and can be absent in up to half of those with croup






















Management 
Treatment is directed at decreasing airway obstruction and keeping the child comfortable 
  • CorticosteroidsAll patients with croup get steroids as a one- time dose (PO/IM/IV). Steroids reduce the severity and duration of symptoms and result in a decrease in return visits and hospital length of stay. The long half-life of dexamethasone (36-54 h) often allows for a single injection. Studies have shown that dexamethasone dosed at 0.15 mg/kg is as effective as 0.3 mg/kg or 0.6 mg/kg (with a maximum daily dose of 10 mg). Effects can be seen within 1 hour of oral administration. Nebulized budesonide 2 mg as a single dose and IM dexamethasone (0.6mg/kg) are alternatives to PO dexamethasone in children who are vomiting.
Treatment of croup: Nebulized epinephrine for moderate to severe croup and corticosteroids for all



  • EpinephrineEpinephrine comes as two different forms: racemic, which is composed of equal parts of L- and D-isomers, and L-epinephrine, which is the drug routinely used in acute situations in concentrations of 1:1000 and 1:10,000. 
  • L-Epinephrine (1:1000): 0.5 ml/kg neb or 5ml maximum  
  • Racemic Epinephrine (2.25%): 0.05ml/kg neb or max 0.5ml
Mild croup generally does not require epinephrine. For those with moderate or severe croup who receive nebulized epinephrine, observe in the ED for at least 3 hours before considering discharge. Epinephrine decreases airway edema through vasoconstrictive alpha effects and acts wishing 10-min lasting up to 2 hours. The use of Adrenaline decreases the number of children with croup requiring intubation, ITU admissions, and admission to the hospital. 

Observation for about 3 hours is recommended because an increase in croup scores can occur between doses of epinephrine nebulisation

  • Intubation is reserved for cases of severe croup not responding to medical treatment. When intubation is necessary, use endotracheal tubes smaller than recommended for patient size and age to avoid traumatizing the inflamed mucosa. 

Treatment options with limited evidence: 
  • Cool Mist: Humidified air was used to treat croup, but they are no longer recommended as studies have consistently failed to show clinical improvement with these interventions.
  • Heliox (70% helium/30% oxygen): Despite its theoretical benefits, studies show no definitive advantage of heliox over conventional treatment.24-28
  • Beta 2 Agonists: Insufficient data. Concerns about risk of worsening upper airway obstruction as Î²-receptors on the vasculature cause vasodilation (as compared to the vasoconstrictive α effects of epinephrine), which might worsen upper airway edema in croup, and there is no smooth muscle in the upper airway. Therefore, β-agonists are not recommended for treatment of croup.
  • Antibiotics have no role in uncomplicated croup 
  • Antitussives have no proven effect on the course or severity of croup and may increase sedation


Differential Diagnosis (Consider if no relief with Rx)
  • Bacterial tracheitis
  • Laryngomalacia
  • Tracheomalacia
  • Vascular rings
  • Epiglottitis (unlikely if vaccinated)
  • Foreign body aspiration
  • Peritonsillar abscess
  • Retropharyngeal abscess
  • Tracheo-esophageal fistula

Admit 
  • Moderate to Severe Croup
  • Looking toxic and not tolerating oral fluids
  • Comorbidities 
  • Social Issues
  • Persistent stridor at rest, tachypnea, retractions, and hypoxia

Discharge Advice 

  • Advise the parents/carers to use either paracetamol or ibuprofen to treat a child who is distressed due to fever. 
  • Encourage the child to take fluids regularly.
  • To check on the child regularly, including through the night.

References and Further Reading :
  1. https://cks.nice.org.uk/croup#!scenario
  2. http://www.ebmedicine.net/topics.php?paction=showTopic&topic_id=334
  3. Russell KF, Liang Y, O’Gorman K, Johnson DW, Klassen TP. Glucocorticoids for croup. Cochrane Database of Systematic Reviews 2011, Issue 1. Art. No.: CD001955.
  4. Johnson DW. Croup. BMJ Clin Evid. 2009; 2009: 0321.
  5. Bjornson, C.L. and and Johnson, D.W. (2013)  Croup in children. CMAJ. 185(15), 1317-1323

    Posted by:

                  
         Lakshay Chanana
         
         Speciality Doctor
         Northwick Park Hospital
         Department of Emergency Medicine
         England

         @EMDidactic