Monday, 27 March 2017

NEJM Week of 23rd February 2017 (#83)

Professor Brian Andrews NEJM Recommendations for Medical Students and Tutors
Week of 23rd February 2017 (#83)
University of Notre Dame Australia (Fremantle Campus)



Occasional Editorial Comment


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Must Read Articles


ORIGINAL ARTICLE

Assessing the Risks Associated with MRI in Patients with a Pacemaker or Defibrillator


A total of 1500 nonthoracic MRI examinations were performed on patients with a non–MRI-conditional pacemaker or ICD, after programming of the devices in accordance with a standardized protocol. No patient whose device was appropriately programmed had device or lead failure.

Over the past twenty years, pacemakers and implantable cardioverter-defibrillators (ICDs) have been designed to reduce the risks associated with MRI when used per defined protocol.

It is estimated that there are approximately eight million devices world-wide that are non-MRI-conditional or potentially not “MRI safe.” It is also estimated that approximately half of the patients with these devices will require an MRI in their lifetime.

1500 patients with non-MRI conditional devices were studied and received standard MRIs (77% for either the brain, cervical spine or lumbar spine). No MRIs were obtained of the thoracic cavity.  MRI machines with a magnetic field strength of 1.5 tesla were used.  Devices were programmed as per protocol before and after the MRI (MRIs were not performed on patients whose ICDs were pacing-dependent). During the study, there was no significant magnetic field-induced cardiac lead heating, although one patient experienced ICD failure, with the device needing to be replaced as protocol had not been followed with appropriate pre-MRI programming of the device. Otherwise no significant adverse events occurred. 



CLINICAL PRACTICE

Screening for Chlamydia trachomatis Infections in Women


Chlamydial infection may result in pelvic inflammatory disease, infertility, and ectopic pregnancy. Chlamydia screening is recommended in sexually active women younger than 25 years of age and other women at increased risk and can be performed on vaginal swabs or urine samples.

This is an excellent case-based review on chlamydial infections in women. The epidemiology, pathology and clinical presentations are defined followed by a discussion of screening strategies (see box insert for Key Clinical Points on screening). Treatment strategies and areas of uncertainty are outlined. This should be read by all medical students.

Recommended learning: Genital infections due to Chlamydia trachomatis.


IMAGES IN CLINICAL MEDICINE

Empyema Necessitatis


A 40-year-old man presented with fever, weight loss, dyspnea, and cough. Physical examination revealed a tender, bulging anterior thoracic mass.

This is an unusual complication of an empyema which, due to tuberculosis, tracks through the parietal pleura into the chest wall. There is an interesting clinical picture and CT scans.

Recommended learning: Review the pulmonary pathology of tuberculosis.



Articles Recommended for Medical Students



Perspective

Recreational Cannabis — Minimizing the Health Risks from Legalization


Twenty percent of the U.S. population now lives in states that have passed ballot initiatives to allow cannabis to be sold for recreational use. The net effect of cannabis legalization on public health is uncertain, and much will depend on how the laws are implemented.

This interesting Perspective summarises what is known and unknown regarding recreational cannabis use with respect to health effects, legalization, and public health policies. After reading this, I realized how much evidence based information needs to be gathered.




Important Articles Related to Mechanisms of Disease and Translational Research



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Other Articles which should interest medical students



ORIGINAL ARTICLE

Tight Glycemic Control in Critically Ill Children


Tight glycemic control has not improved outcomes in studies involving critically ill adults or children after cardiac surgery. A controlled study involving hyperglycemic critically ill children who had not undergone cardiac surgery showed no benefit of tight glycemic control.

After this study involving tight glycaemic control in critically ill children (lower-target group at 4.4 – 6.1 mmol/L and higher-target group at 8.3 – 10.0 mmol/L), it now appears that in most studies to date on critically ill adults and children that clinical outcomes are not improved with tight glycaemic control.  As this study demonstrates, patients in the lower-target group (tight control) had more health care-associated infections and more episodes of severe hypoglycaemia.



IMAGES IN CLINICAL MEDICINE

Gastric Gyri — Pediatric Ménétrier’s Disease


A 5-year-old boy presented with nausea, vomiting, and intermittent abdominal pain. Images showed giant cerebriform enlargement of rugal folds in the fundus and the body, which were suggestive of Ménétrier’s disease.

When considering the gastrointestinal causes of hypoalbuminemia, one of the rarer causes, Menetrier’s disease, may need to be considered.

Recommended learning: Review the mechanisms, clinical entities associated with and approach to the management of hypoalbuminemia.


CASE RECORDS OF THE MASSACHUSETTS GENERAL HOSPITAL

Case 6-2017 — A 57-Year-Old Woman with Fatigue, Sweats, Weight Loss, Headache, and Skin Lesions


A 57-year-old woman presented with fatigue, night sweats, weight loss, headache, abdominal pain, and skin lesions. Laboratory testing revealed hypergammaglobulinemia and hypocomplementemia. Diagnostic tests were performed.
This CPC provides an excellent differential diagnosis of a patient presenting with fatigue, night sweats, weight loss, headache, abdominal pain, and skin lesions.  This patient is also found to have lacrimal gland enlargement, hypergammaglobulinemia, hypocomplementemia and increased plasma cells on a biopsy. I would not have even considered giant cell arteritis in my DD. The diagnosis is an IgG4-related disease, the group of which also includes disorders such as autoimmune pancreatitis and idiopathic retroperitoneal fibrosis.
IgG4 related disorders have been previously discussed in issues # 64, http://www.nejm.org/doi/full/10.1056/NEJMcpc1610097  and #14 http://www.nejm.org/doi/full/10.1056/NEJMra1104650.


New and Novel Therapies



ORIGINAL ARTICLE

Inhibiting Plasma Kallikrein for Hereditary Angioedema Prophylaxis


In patients with hereditary angioedema with C1 inhibitor deficiency, swelling episodes are related to the release of bradykinin from high-molecular-weight kininogen from kallikrein action. Lanadelumab, which inhibits kallikrein action, reduced the rate of attacks of angioedema.

EDITORIAL

Kallikrein Inhibition for Hereditary Angioedema


Hereditary angioedema (HA), due to a functional deficiency in C1 (esterase) inhibitor (types I and II), is a rare disorder and is usually autosomal dominant in inheritance.  Deficient function of C1INH results in ongoing activation of the classical complement system with reduced C4 levels, activation of the coagulation system and activation of the kallikrein-kinin system (Fletcher factor deficiency is a rare congenital absence of prekallikrein which does not produce any significant clinical manifestations). Kallikrein generation from prekallikrein leads to excessive proteolysis of high MW kininogen and formation of bradykinin which results in vasodilation, vascular leakage, oedema and pain.  80% of patients with HA exhibit reduced production of C1INH, while 20% have functional inhibition of C1INH usually due to autoantibodies (SLE and B cell lymphomas).

The clinical manifestations of HA result from intermittent subcutaneous oedema of the hands, feet, face and abdominal wall and from submucosal oedema of the mouth, airways, GIT and genitourinary system.  There is no urticaria or pruritus associated with this condition. Patients usually present with recurrent painful swelling of lips, tongue, and airways compromising breathing and abdominal pain.

This study employs the prophylactic use of a monoclonal antibody (lanadelumab) against kallikrein, resulting in reduced cleavage of high MW kininogen and reduced plasma levels of bradykinin, which leads to fewer episodes of clinical angioedema.

The prophylactic use of this monoclonal antibody was effective and produced no significant adverse events in this brief six week, phase 1b study.  This is really an “appetiser study” responsible in part for some of the literature pollution that occurs. If this study had not been performed at the MGH in Boston, it would not have been published in the Journal. As the authors indicate in their discussion, the full phase 3 six-month (24 week) study is under way and had undoubtedly been completed at the time of submission and subsequent publication of this study. Maybe the results of another agent for treating HA are soon to be published in the Journal.



Articles Some Medical Students Found Interesting




Perspective

HISTORY OF MEDICINE

The Death of Animals in Medical School

Although live animals had been used in medical education for millennia, with recent changes at Johns Hopkins and the University of Tennessee, every core U.S. medical school curriculum has now ceased this practice. It is worth considering the causes and implications of this milestone.

This is an interesting historical review of the use of live animals in medical education in the US.


ORIGINAL ARTICLE

Genetic Drivers of Kidney Defects in the DiGeorge Syndrome


A third of patients with the DiGeorge syndrome have congenital kidney and urinary tract anomalies. This study provides evidence that haploinsufficiency of CRKL is associated with such anomalies in the DiGeorge syndrome and in sporadic congenital kidney and urinary tract anomalies.

I found this to be a fascinating study, though none of the medical students in my groups felt the same, until we discussed the article in some detail.

This is a truly an extensive and elegant study involving 2080 patients with congenital kidney and urinary tract abnormalities and 22,094 controls. The authors performed a genome wide search for structural variants in 22q11.2 in the above two cohorts.

This article illustrates the following:

1.     30% of patients with DiGeorge syndrome have congenital renal and urinary tract abnormalities.  They also exhibit the more well-characterized thymic aplasia with profound T cell immunodeficiency, hypoparathyroidism leading to hypocalcaemia, congenital cardiac malformations frequently requiring early surgery and facial and neck abnormalities.

2.     Most non-renal manifestations of the DiGeorge syndrome are associated with small deletions in chromosome 22, resulting in loss of function in TBX1 (the tbx1 gene translates the T-box 1 protein).

3.     The T-box 1 protein appears to be necessary for the normal development of large arteries that carry blood out of the heartmuscles and bones of the face and neck, and glands such as the thymus and parathyroid (Wikipedia).

4.     The hypothesis was generated that if renal abnormalities in DiGeorge syndrome were not attributable to deletions involving the tbx1 gene on 22q11.2, could another deletion in a nearby area of 22q11.2 on chromosome 22 be responsible?

5.     The authors identified a heterozygous 370 kB deletion in 22q11.2 containing a series of nine genes that when absent were associated with the renal defects in the DiGeorge syndrome. Further characterization of these genes identified the three important responsible genes, snap29, aifm3 and crkl.  However, absence of the crkl gene alone resulted in renal agenesis or hypodysplasia.

6.     CRKL encodes an adapter protein that regulates intracellular signalling transduction from multiple growth factors, including the fibroblast growth factors, which are key regulators of kidney and urinary tract development (article).

7.     In zebra fish embryos, the authors produced a crkl loss of function mutation which resulted in renal defects. In a mouse model, inactivation of crkl resulted in similar renal abnormalities to those in humans.

8.     In 1.1% of the 2080 humans with congenital renal abnormalities and in 0.01% of the population controls, heterozygous deletions of 22q11.2 were identified.

9.     The authors have identified a gene crkl that is responsible for the congenital renal abnormalities of the DiGeorge syndrome and a small number of patients with sporadic congenital renal and urinary tract abnormalities.