Wednesday, 31 August 2016

NEJM Week of 4th August 2016 (#54)

Professor Brian Andrews NEJM Recommendations for Medical Students and Tutors
Week of 4th August 2016 (#54)
University of Notre Dame Australia (Fremantle Campus)


Occasional Editorial Comment

I have included three perspective articles on open-access data sharing in the final section of this week’s blog. Students have tended to breeze over these article, but they are important for those students planning a research career in terms of the development of clinical trials and the subsequent publication of data from those trials.


Must Read or Save Articles


None


Articles Recommended for Medical Students


ORIGINAL ARTICLE

Innate Immunity and Asthma Risk in Amish and Hutterite Farm Children


The Amish and the Hutterites are farming communities with similar gene pools, but asthma and allergy are more common in Hutterites. The authors provide data that support the idea that the Amish environment stimulates the innate immune response and protects the children from asthma.


EDITORIAL

Innate Immunity in Asthma


This is a landmark article with an excellent accompanying editorial.

The study is based on the observation that the prevalence of asthma and allergic disease in children is 4 - 6 times higher in the Hutterite farming communities than in the Amish farming communities. Both communities share a common German alpine genetic origin. However, a major difference exists between the communities related to methods used in dairy farming which may result in environmental differences in which the children develop. The Amish practice single-family, non-mechanized dairy farming while the Hutterites use modern mechanization in their dairies. Dust samples from Amish farms show increased levels of lipopolysaccharides and a distinct microbial composition when compared with Hutterite dust samples.

The hypothesis generated is that the dust from Amish farms induces a low level innate immune response involving transcriptional pathways and mediators acting via NFkB and IRF7 preventing asthma and allergic responses. Microbial peptides may also act via MyD88 and toll-like receptors (TLRs) that activate regulatory T cells and enhance mucosal tolerance. This type of response contrasts with the more common adaptive immune response to allergens seen in asthmatics where allergen-specific type 2 helper T cell and IgE B cell responses are dominant, producing the acute and delayed allergic responses.

The results of this study on 30 Amish and 30 Hutterite children aged between 7–14 years indicate that:

1.     Endotoxin in Amish dust were 6.8 times higher than in Hutterite dust (Figure 1B).
2.     In studies of peripheral blood leukocytes comparing both populations, the Amish group had:
3.     Increased numbers of neutrophils but with reduced cell surface markers for the chemokine receptor CXCR4,
4.     Lower numbers of eosinophils and with reduced CD11b receptors,
5.     No difference between monocyte numbers or CD11c receptor expression. However, reduced expression of HLA-DR4 and increased expression of ILT3 suggest an anti-inflammatory response in the Amish.

In a murine model of experimental allergic asthma, mice were sensitized to ovalbumin by intraperitoneal injection of the antigen and subsequently challenged by airway installation of the ovalbumin to produce acute asthma. Amish or Hutterite dust were then installed a total of 14 times over 4-6 weeks into the nasal cavities of mice to induce a presumed protection against asthma as seen in the Amish population.

The dust-exposed BALB/c mice were then challenged with inhaled ovalbumin followed by increasing doses of nebulized acetylcholine.  Both airway’s resistance and cell composition of the bronchoalveolar lavage (BAL) fluid were studied (Figure 4A). In the mice previously exposed to Amish dust, airway’s resistance was significantly lower than in those primed with Hutterite dust.  Further the BAL eosinophil count was significantly lower following Amish dust exposure. In order to study Myd88 and Myd88-Trif knockout CD57BL6 mice, mice under similar experimental circumstances, CD57BL6 mice were also required as controls, with similar results to the BALB/c mice (Figure 4B). The deletion of the proteins Myd88 and Trif essentially disables the innate immune response.   In both knockout mice groups (Figures 4C and D), deletion of Myd88 or Myd88 + Trif resulted in abrogation of the protective effects of Amish dust.

The murine studies indicate that Amish dust exposure reduced airway’s resistance and BAL eosinophil count and that this effect required both Myd88 and Trif to be functional. This provided a mechanism for the protective effect of Amish dust by inhibiting the innate immune response.

Recommended learning:

1.     Review the pathophysiology of asthma and the clinical presentations and management of asthma in the paediatric and adult populations.
2.     Review the MED300 medicine clinical case.


REVIEW ARTICLE

Fire-Related Inhalation Injury


Fire-related inhalation injury results from a combination of direct exposures, systemic effects of inhaled toxins, accrual of endobronchial debris, and secondary infection. This brief review discusses the pathogenesis of and approach to fire-related inhalation injury.

This is a review that should be read by MED300 and MED400 during their surgical, ED or ICU rotations.

This article describes fire-related inhalation injury and also includes an excellent discussion of the pathological processes involved. Apart from the important clinical examination, the role of bronchoscopy and imaging in the early management is discussed. The Figure 2 and Table 1 provide a treatment algorithm and summary of the management, together with a detailed discussion of the clinical course and time-based management.

Recommended learning: Review the pathophysiology of burns, types of burns and management of burns and their sequelae at various sites


IMAGES IN CLINICAL MEDICINE

Borrelia recurrentis Infection


After collapsing in Munich, a 16-year-old male Somalian refugee was brought to a local hospital with severe headache and abdominal pain. His vital signs were notable for a temperature of 41°C, a heart rate of 105 bpm, and blood pressure of 95/50 mm Hg.

This is a very interesting blood smear demonstrating the causative spirochaete.

This infectious disease is seen most frequently in immigrant populations usually from Sudan or Ethiopia. Patients frequently present with recurrent episodes of fever, prominent headache, mental status changes, and nausea.  Borrelia recurrentis is a spirochaete that is present in the body cavity of the louse. The organism is spread when the louse is crushed. It can be introduced into a break in the skin or into the conjunctiva when the eyes are rubbed or from the fingers into the mouth. It is spread when humans are confined to small areas, such as during winter when the population is indoors or in tents e.g. refugee camps when the infected louse spreads from clothing, blankets etc.

All other causes of relapsing fever are spread by ticks who harbour the spirochaete in their saliva.

Recommended learning: Review the human diseases caused by spirochaetes.


IMAGES IN CLINICAL MEDICINE

Urticaria Multiforme


A 3-year-old girl presented to the ED on day 1 of a mild pruritic urticarial rash. The parents described a viral respiratory illness that had occurred a week earlier. Fever developed on day 2, along with a generalized polycyclic annular rash with wheals and ecchymotic centers.

This is a classical presentation of a rare paediatric condition.  One feature that characterises urticarial multiforme is the significant facial and acral oedema with the urticarial eruption. If you have a particular interest in dermatology and would like more information and a more in-depth discussion of the differential diagnoses, this is a good site: (http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3613272/ )


CLINICAL PROBLEM-SOLVING

Prevention as Precipitant


Two days after undergoing uncomplicated bilateral total knee arthroplasties, a 72-year-old man had a temperature of 101°F and a pruritic, erythematous rash that originated on his trunk and spread peripherally to his arms and upper thighs over the course of 24 hours.

As stated above, this is an interesting case of a patient who had a bilateral total knee arthroplasty and over 24 hours developed a fever and a rash. Discussion of the differential diagnoses focuses on cutaneous drug reactions.\


Important Articles Related to Mechanisms of Disease and Translational Research


ORIGINAL ARTICLE

Inherited DNA-Repair Gene Mutations in Men with Metastatic Prostate Cancer


Inherited mutations in DNA-repair genes were found in nearly 12% of men with metastatic prostate cancer, as compared with 2.7% in an unselected general population.

Although the role of PSA determinations is still an area of controversy, local guidelines have been established. What is clear is that with the introduction of routine PSA screening, there was a dramatic fall in the number of patients presenting to physicians with metastatic disease of the prostate (http://www.nejm.org/doi/full/10.1056/NEJMp1510443 ). However, in an individual with an elevated PSA level and microscopic evidence of prostate cancer, the natural history of the tumour in the individual patient cannot be predicted (also compare microscopic intraductal breast cancer and papillary carcinoma of the thyroid).
The answer as to how the tumour will behave in the short-term in the individual patient will reside in the identification of specific tumour markers and/or the genetic profile of the tumour.

This multicentre study of 692 men with documented metastatic prostate cancer is compared with 499 patients with localized prostate cancer (TCGA cohort) and 53,105 controls without clinical evidence of cancer (Exome Aggregation Consortium). Germline mutations in genes mediating DNA-repair processes (Table 2) were identified in 11.8% of patients with metastatic disease, in 4.6% among patients with localized prostate cancer, and in 2.7% of the control population. Of the 16 DNA repair genes identified with mutations (Figure 2), the most common were in BRCA2 (44%), ATM (13%), CHEK2 (12%) and BRCA1 (7%). The 12 remaining ranged from 1-4% of the identified mutations.

Patient with metastatic prostate cancer who exhibit these mutations are more likely to respond to inhibitors of PARP1 and to platinum-based chemotherapy.

The role of screening all men with metastatic prostate cancer for these genes is as yet undetermined. However, this study and others involving a variety of tumour types, indicate the future direction of genetic testing in malignancy in the hope of predicting metastatic potential of localized tumours and thus the ability to predict responses to chemotherapeutic agents (pharmacogenetics).

 Recommended learning:

1.     Review the epidemiology, genetics, pathology, clinical presentations and the principles of management of prostate cancer.
2.     Review the current guidelines for PSA screening and indications in clinical practice.


CLINICAL IMPLICATIONS OF BASIC RESEARCH

Modeling Zika Virus Infection in Pregnancy


 This article reviews the results of four recent murine studies which demonstrate that ZIKR administered to pregnant mice results in similar changes to those described in humans. The passage of ZIKR across the placenta and into the developing brain is well illustrated in Figure 1.

The investigators have found that ZIKR replicates in maternal and fetal trophoblastic cells, in foetal endothelial cells, and in macrophages within the placenta. ZIKR appears to bind to a cell-surface tyrosine kinase called AXL.

This process can either lead to damage of placental vessels, decreased fetal blood flow and increased fetal death. Moreover, the virus may spread to cortical neural progenitor cells and radial glial cells resulting in cortical atrophy and subsequent microcephaly.

These murine models will help to define ZIKR induced pathology and hopefully can be used to define ZIKR human immunopathogenesis due to similarities between murine and human trophoblast function and placental development and also parallel developments in the nervous systems.


Other Articles which should interest medical students


REVIEW ARTICLE

THE CHANGING FACE OF CLINICAL TRIALS
Pragmatic Trials


In pragmatic trials, participants are broadly representative of people who will receive a treatment or diagnostic strategy, and the outcomes affect day-to-day care. The authors review the unique features of pragmatic trials through a wide-ranging series of exemplar trials.

This is another review article in the Clinical Trial Series which addresses the area of pragmatic trials. The authors attempt to contrast explanatory trials with pragmatic trials.

Nine levels for assessing the level of pragmatism in a trial are outlined in Table 1 and each level is individually addressed throughout the article. In Table 2, examples of specific trials and their pragmatic attributes are described. At the end of the article the message I got was that most trials exhibit varying degrees of pragmatism, none are completely pragmatic, and none are capable of answering all of the potential questions about the value of any health care intervention. The authors suggest that with any trial, it should be as pragmatic as possible except when the quality of the trial is compromised or clinical questions of interest are not able to be addressed.

Perspective

Strengthening Research through Data Sharing (1)


Data sharing can strengthen academic research, the practice of medicine, and the integrity of the clinical trial system. Many policy, privacy, and practical issues need to be addressed, but the stakes are too high to step back in the face of that challenge.


Perspective

The Yale Open Data Access (YODA) Project — A Mechanism for Data Sharing (2)


As medical research moves toward the more open approach to data sharing from which physics, astronomy, and genetics currently benefit, the YODA Project offers one of several pioneering data-sharing mechanisms that are already in use.


Perspective

Toward Fairness in Data Sharing (3)


A new consortium, ACCESS CV, aims to provide avenues for data sharing while minimizing risks and unintended consequences. It has identified challenges including data complexity, publication and selection bias, increased risk of type I errors, and patient privacy.

I will attempt to summarize the above three perspectives in the following statements:

In January 2016, a proposal from the International Committee of Medical Journal Editors (ICMJE) regarding data-sharing from clinical trials was published in the Journal http://www.nejm.org/doi/full/10.1056/NEJMe1515172 . In this, the authors outlined reasons for sharing data from clinical trials whether they be publicly funded (NIH) or funded by pharmaceutical companies.  They suggested that the investigators agree to data sharing at the time of the clinical trial registration and that the investigators agree to sharing the data from deidentified patients within six months of publication as a requirement for publishing their data in a specific journal.

In Editorial 1 of this week’s Journal, the editors, who strongly favour the recommendations of the ICMJE, recruited Senator Elizabeth Warren to comment on the proposal. As a JD and a faculty member of Harvard, a member of the ICMJE, a Senator from Massachusetts, and a powerful national liberal political force, she provided an eloquent endorsement of the recommendations. In addition to an inability to publish in specific journals, she also suggested that those federally funded who elect not to share their data may find themselves ineligible for future federal funding.

In Editorial 2, the Yale Open Data Access (YODA) Project is described. The discussion focuses on the need to ensure participants’ privacy, the role of an independent funded arbiter who would provide for accountability, transparency, and arranging for the sharing of the data. Who would fund this individual, the journal in which the results are published or the provider of the study funds? The final area involves appropriate academic recognition of the original investigators if the data they generated are then mined and analysed by another party. I consider this is a major area of concern.

In Editorial 3, opposite points of view are expressed with regard to fairness in data sharing.  The authors summarize their recommendations as follows:

1.     that the ICMJE come together with trialists and other stakeholders to discuss the potential benefits, risks, burdens, and opportunity costs of its proposal and explore alternatives that will achieve the same goals efficiently
2.     that the timeline for providing deidentified individual patient data should allow a minimum of 2 years after the first publication of the results and an additional 6 months for every year required to complete the study, up to a maximum of 5 years (the authors provide a justification for this suggestion)
3.     that an independent statistician should have the opportunity to conduct confirmatory analyses before publication of an article, thereby advancing the ICMJE’s stated goal of increasing “confidence and trust in the conclusions drawn from clinical trials,” and
4.     that persons who were not involved in an investigator-initiated trial but want access to the data should financially compensate the original investigators for their efforts and investments in the trial and the costs of making the data available


Clearly there is a long way to go to resolve these issues.  I would hope that there is significant compromise on the timeline and appropriate academic recognition by the investigators’ institution.

Tuesday, 23 August 2016

NEJM Week of 28th July 2016 (#53)

Professor Brian Andrews NEJM Recommendations for Medical Students and Tutors
Week of 28th July 2016 (#53)
University of Notre Dame Australia (Fremantle Campus)


Occasional Editorial Comment


If you open the bog at the bottom of the review, you will find the format is much easier to read.


Must Read or Save Articles



REVIEW ARTICLE

Treatment of Opioid-Use Disorders


Opioid-use disorders are common, but most physicians are not trained to recognize and treat them. This review outlines a general approach to identifying and treating these disorders.

This is a must save article. I recommend you store this hyperlink for future use.

This Review Article offers an excellent table (Table 1) which reviews the diagnostic criteria for an opioid-use disorder based on DSM-5. The remainder of the article focuses on the specific treatments of these disorders and the subsequent approaches to rehabilitation and maintenance. The treatment schedules are very detailed, but the general information needed can be obtained from reviewing the tables and reading the overview of the problem which is provided in the first five paragraphs of the article.


Articles Recommended for Medical Students



CASE RECORDS OF THE MASSACHUSETTS GENERAL HOSPITAL

Case 23-2016 — A 46-Year-Old Man with Somnolence after Orthopedic Surgery


A 46-year-old man had worsening somnolence 1 day after replacement surgery with a femoral endoprosthetic implant. Fever, tachycardia, hypertension, and tachypnea developed, and examination revealed somnolence, gaze deviation, rigidity, and hyperreflexia. A diagnosis was made.

This patient developed deterioration in mental function 14 hours after significant orthopaedic surgery.  The discussion focuses on the effects of medication and the cerebral fat embolism syndrome. A diagnostic MRI of the head is illustrated.


Perspective

Incorporating Indications into Medication Ordering — Time to Enter the Age of Reason


Beyond the five “rights” for safe medication ordering and use — the right patient, right drug, right dose, right time, and right route — a sixth element must be correct: the indication. Indications based prescribing can improve medication use in multiple ways.

Medical students in Australia are routinely taught the 6Rs of prescribing, with the 6th R representing the right indication. In hospital charts there is a place to document the prescribing indication thought this appears to be infrequently filled out. There is no place for drug indication on routine prescriptions but it is a requirement for an Authority Script.


IMAGES IN CLINICAL MEDICINE

Dysphagia Lusoria


A 46-year-old otherwise healthy man presented with a 1-year history of occasional dysphagia to solid foods that was not accompanied by weight loss. A barium-swallow examination revealed posterior oblique indentation of the proximal esophagus.

This is an extremely unusual cause of dysphagia.  However it is another cause for external compression of the oesophagus for those who like lists of rare disorders.

Recommended learning:

Review the causes and management of dysphagia.  Particularly review the case of dysphagia in the MED300 weekly clinical cases.



IMAGES IN CLINICAL MEDICINE

Herpes Zoster Mandibularis


A 70-year-old man presented with a 2-day history of facial edema, rash along the left lower jaw, and plaque that covered two thirds of the left half of his tongue. He had had pain, otalgia, and glossodynia 3 days before the outbreak of the rash.

This is an excellent clinical photograph of a patient with Herpes zoster involving the mandibular branch of the trigeminal nerve. Note the typical facial involvement together with involvement of the anterior 2/3 of the tongue via the lingual nerve. Vesicles may also have been present on the tympanic membrane which is innervated by the auriculo-temporal branch of the mandibular nerve.

Recommended learning:

Review the anatomy of the trigeminal nerve (V), in particular the motor and sensory innervations and the clinical examination of the trigeminal nerve.


EDITORIAL

Von Willebrand Factor — A Rapid Sensor of Paravalvular Regurgitation during TAVR?



ORIGINAL ARTICLE

Von Willebrand Factor Multimers during Transcatheter Aortic-Valve Replacement


In patients undergoing transcatheter aortic-valve replacement, defects in high-molecular-weight von Willebrand factor multimers and the closure time with adenosine diphosphate (a measure of hemostasis) were closely correlated with postprocedural aortic regurgitation.


Before reading the Editorial and the study, I strongly recommend watching the accompanying video which describes the normal biological function of von Willebrand factor (vWF), as well as the procedure transcatheter aortic-valve replacement (TAVR).  I also suggest you review the YouTube presentation.

The premise for this study is that vWF under normal shear stress circulates as partially unfolded, elongated multimers with exposed binding sites for platelets and collagen. With active binding, the zinc-dependent metalloprotease ADAMTS13 cleaves vWF into appropriate sizes to optimize the clotting process. (In most cases of acquired TTP, an autoantibody is directed against ADAMTS13).

Under situations of increased shear stress and the generation of excessive turbulence, such as valvular heart disease (in this study patients with severe aortic stenosis), hypertrophic obstructive cardiomyopathy (HOCM), circulatory-assist devices, and extracorporeal membrane oxygenators, high-molecular weight vWF multimers are cleaved resulting in acquired vWF deficiency and the potential for bleeding.

The hypothesis generated for this study involves TAVR for treating severe aortic stenosis. If the valve is placed successfully, only minimal to mild paravalvular aortic regurgitation (AR) should result.  Moderate to severe paravalvular AR is described in 12% of patients with the first generation of the valve and in 4% with the second generation.

With severe aortic stenosis (Figure 2 in study), the high MW vWF multimers represent approximately 61% of vWF present in pooled normal human plasma and with subsequent correction of the AR, the percentage increases to 100% within five minutes. A similar parallel improvement in clotting test (CT-ADP (closure-time with ADP) is seen with correction of the paravalvular AR.

The mortality rate at one year in those undergoing TAVR is twice as high in those patients with residual moderate to serve resultant paravalvular AR (Figure 4).                                                                                                                                                                                                                                                                                                                                                                                                                                                                                          
Important Articles Related to Mechanisms of Disease and Translational Research


None


Other Articles which should interest medical students



ORIGINAL ARTICLE

Liraglutide and Cardiovascular Outcomes in Type 2 Diabetes


Patients with type 2 diabetes and high cardiovascular risk were assigned to receive either the glucagon-like peptide 1 analogue liraglutide or placebo. The rate of first occurrence of cardiovascular death, nonfatal MI, or nonfatal stroke was lower with liraglutide.
                 

ORIGINAL ARTICLE

Empagliflozin and Progression of Kidney Disease in Type 2 Diabetes


Among patients with type 2 diabetes at high cardiovascular risk, the rates of progression of kidney disease and clinically relevant renal events were lower among patients receiving empagliflozin, a sodium–glucose cotransporter 2 inhibitor, than among those receiving placebo.


EDITORIAL

Cardiac and Renovascular Complications in Type 2 Diabetes — Is There Hope?


These two articles describe placebo-controlled, double blind trials involving patients with type 2 diabetes mellitus who were at high risk for cardiovascular events. In general, the first study used liraglutide, a glucagon-like peptide 1 agonist, to determine the effects of the drug on limiting macrovascular complications of diabetes.  The second article focussed on the prevention of microvascular complications of diabetes in the kidney using empagliflozin, a sodium-glucose cotransporter 2 (SGLT2) inhibitor. Both drugs improved diabetic control over placebo.

 In the first study, liraglutide was added to standard diabetic therapy (4688 patients received liraglutide and 4672 placebo) and patients were followed for a median time of 176 weeks after randomization. Moreover in this group, there was a significant reduction in death from cardiovascular causes (p=0.007) and death due to any cause (p=0.02) (Figure 1). There were no differences in nonfatal myocardial infarction and strokes or hospitalization for heart failure. When the primary composite outcome was subsequently reanalysed as an expanded composite outcome (Table 1), where coronary revascularisation and hospitalization for either unstable angina or heart failure were added to death from cardiovascular causes, or nonfatal MI or stroke, the p value fell from 0.01 to 0.005.
In the other study using empagliflozin, a total of 7018 patients were randomized to receive empagliflozin (4685 patients) or placebo (2333 patients) and further broken down into those with baseline creatinine clearances less than (25.5%) or greater (74.5%) than 60 ml/minute, with a minimum of 30 ml/minute. Two doses of empagliflozin studied. Overall, empagliflozin was superior to placebo in slowing the progression of kidney disease (Figure 1) and in significantly improving seven renal outcome measures (Figure 2). Empagliflozin resulted in a fall in eGFR with both doses over the first four weeks of the 192 week study and then rose, such that by 80 weeks, eGFR was higher than placebo over the remainder of the study.

Both of these studies were reviewed in the accompanying Editorial.  All patients studied had extensive cardiovascular disease, although in the liraglutide study eligible patients less than 60 years of age had to have a coexisting cardiovascular condition and if 60 or older, one cardiovascular risk factor would suffice (? effect of age).  Both studies were large, expensive, and multicentre and employed patient populations which were similar, though not identical. As summarized in the Editorial, it appears that both therapies add to the management of type 2 diabetic patients with a high risk for cardiovascular events with more studies and drugs to come. The problem I have with all of these studies is how to reconcile the differences in study design, the varying inclusion and exclusion criteria and the number of similar drugs coming on the market. I wonder where SGLT1 inhibitors, that reduce glucose absorption from the intestine, will fit into the treatment of type 2 diabetes mellitus.

Recommend learning:

Review the mechanisms of action and the underlying physiology of the groups of non-insulin therapies used to treat diabetes mellitus:

1.     Sulfonlyureas
3.     Thiazolidinediones
4.     DPP-4 inhibitors
5.     Glucagon-like peptide-1 analogues
6.     Sodium-glucose cotransporter 2 inhibitors (SGLT2 inhibitors) (http://www.nejm.org/doi/full/10.1056/NEJMcibr1506573)
7.     Acarbose

By the end of MED200, you should have a working knowledge of the medication groups used to treat diabetes mellitus, not just metformin and the sulfonylureas.



Monday, 15 August 2016

NEJM Week of 21st July 2016 (#52)

Professor Brian Andrews NEJM Recommendations for Medical Students and Tutors
Week of 21st July 2016 (#52)
University of Notre Dame Australia (Fremantle Campus)


Occasional Editorial Comment


This is the one year anniversary of my blog. In the survey I recently sent out, 25% of medical students responded.  All indicated that this was a valuable learning resource and agreed that I should continue with the blog. I wish to thank all readers for your support.



Must Read or Save Articles



REVIEW ARTICLE

Medical Considerations before International Travel


The scope of illnesses that may befall international travelers is broad. A guide to preparing for the preventable causes of illness is provided. Physicians may find it useful in counseling their patients who travel internationally.

This is an in-depth review of many of the medical consideration you may have regarding international travel. I recommend reviewing the Supplemental Appendix where you will find numerous web addresses including Travel Health Online (http://www.tripprep.com/ ).  After you register, type in the place you want to visit and nearly all the information you require will be presented. Unfortunately it is not up to date as I typed in Puerto Rico and no mention was made of ZIKA virus infection. More current information is provided in the text of the article with hyperlinks.

I recommend that you store this article and review as needed.

Recommended learning: MED300 and MED400 should review the medical cases on travel and infectious diseases (Fever and Polyarthritis, Fever in a Traveller and Traveller’s Diarrhoea).



Articles Recommended for Medical Students



IMAGES IN CLINICAL MEDICINE

Thyroid Ophthalmopathy, Dermopathy, and Acropachy


A 56-year-old man was referred to a dermatologist for assessment of the progression of his thyroid dermopathy. Three years earlier, he had received a diagnosis of Graves’ disease with thyroid-associated ophthalmopathy and dermopathy.

The clinical photographs demonstrate the autoimmune manifestations of Graves’ disease – ophthalmopathy, pretibial myxoedema, and thyroid acropachy which are all associated with high levels of TSH-receptor stimulating antibody. Acropachy is rare with periostitis also involving the lower radius and ulna. The periostitis is described as “wool on a sheep’s back” (also seen in the hands in psoriatic arthritis) in contrast to the linear periostitis seen at the lower radius and ulna in hypertrophic pulmonary osteoarthropathy (HPO).

Recommended learning: Review causes of thyrotoxicosis and Graves’ disease, particularly from the weekly MED300 medical cases.



IMAGES IN CLINICAL MEDICINE

Nodular Lymphoid Hyperplasia


An 18-year-old woman presented with recurrent episodes of diarrhea associated with epigastric discomfort and bloating. Examination of the stool revealed trophozoites of the species Giardia lamblia. Gastroduodenoscopy revealed multiple nodules in the duodenum.

Nodular lymphoid hyperplasia can occur throughout the GI tract but is most frequent within the small intestine. It may, as in this case, or may not be associated with an immunodeficiency state (most often IgA deficiency or common variable immunodeficiency). For those needing more information, I recommend the following NIH review (http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4231492/ ).

Recommended learning: Review immunodeficiency which was covered in MED100, particularly IgA deficiency.


CASE RECORDS OF THE MASSACHUSETTS GENERAL HOSPITAL

Case 22-2016 — A 65-Year-Old Man with Syncope, Dyspnea, and Leg Edema


A 65-year-old man presented with syncope. One month earlier, cough, dyspnea, and leg edema had developed. Imaging studies of the chest revealed lymphadenopathy, and an echocardiogram showed hypertrophic obstructive cardiomyopathy. A diagnostic procedure was performed.

 This patient presents with syncope and symptoms and signs of pulmonary hypertension. There is an interesting discussion of the primary disease.


Important Articles Related to Mechanisms of Disease and Translational Research



ORIGINAL ARTICLE

BRIEF REPORT

Proopiomelanocortin Deficiency Treated with a Melanocortin-4 Receptor Agonist


Absence of proopiomelanocortin results in early-onset obesity, hyperphagia, hypopigmentation, and hypocortisolism. Two affected patients received setmelanotide, a new melanocortin-4 receptor agonist, which led to sustainable reduction of hunger and substantial weight loss.


EDITORIAL

Hormone-Replacement Therapy for Melanocyte-Stimulating Hormone Deficiency


 This Brief Report is my choice of article of the week but was not reviewed by any of the medical students.

It describes two patients with neonatal hypoadrenalism and extreme obesity associated with hyperphagy.  It relates these biological effects to a mutation in the gene encoding proopiomelanocortin (POMC) and describes the therapeutic benefit of a drug which activates MSH receptors within the hypothalamus leading to reduced food intake and weight loss. One patient has a heterozygous mutation in POMC, while the other has a homozygous mutation, both resulting in a similar phenotype.

POMC is produced in the pituitary, is a long precursor polypeptide, and is catalysed to MSH, ACTH, b-endorphin and b-lipotropin.

I learned the following about melanocortin receptors:
 
1.     MSH binds to four of the five melanocortin receptors (1,3,4,5), while ACTH binds to the melanocortin-2 receptor (MC2R) in the zona fasciculata of the adrenal gland.
2.     Lack of activation of the MC1R results in depigmentation and red hair.
3.     Lack of activation of the MC4R and the MC3R lead to hyperphagy and extreme obesity.
4.     Lack of activation of the MC5R activation lead to decreased sebum production and lesser effects on RBC differentiation, thermoregulation, fatty acid oxidation in skeletal muscle and lipolysis in fat cells, and the inflammatory response.

Thus the phenotype of functional deficiency of POMC is hypoadrenalism in the newborn, depigmentation and red hairs, hyperphagy and extreme obesity.

The authors describe the anti-obesity effect of a drug, setmelanotide, which binds to and activates the MC4- and MC3-receptors, resulting in decreased food intake and weight loss.

The Editorial summarises the results of the article, discussing the possible role of setmelanotide, leptin therapy, and the role of MCR4R agonists in treating obesity. This is an example of patient to bench and back to the patient.

Recommended learning:

1.     Review the epidemiology, causes and effects of obesity.
2.     Review the management of obesity, including the place for bariatric surgery.
3.     Consider the physiological roles of leptin and ghrelin.
                                                                                                                                                                                                                                                                                                                          
CLINICAL IMPLICATIONS OF BASIC RESEARCH

Defining Metastatic Cell Latency


A study modeling lung-cancer and breast-cancer metastasis in the mouse showed how tumor cells, once seeded to a site distant from that of the primary tumor, may maintain a state of dormancy until they are “reawakened.”

  Pathological analyses suggest that tumor cells can seed to and be maintained in many different organs. How do they escape immune attack and survive? How is their dormant state maintained, and what stimulates their escape from dormancy?

These questions, which are posed by the author, are the subject of a research article by Malladi et al. which partially addresses some of these issues.  The study involved mice injected via the tail vein with human cell lines derived from metastatic lung and breast cancer patients. These cells are defined as latency-competent cells which have the potential to seed distant sites and remain dormant for months before exhibiting their metastatic potential.

From the review and from previously described works, with the limitations of the murine models studied, I learned the following which are well illustrated in Figure 1:

1.     Once metastatic tumour cells cross the endothelial barrier and enter the tissue, two types of circulating monocytes are activated: one type is a patrolling, non-classical monocyte which recruits NK cells to destroy the majority of the tumour cells expressing an NK-activating receptor, while the other, a classical monocyte provides proliferation and survival signals to surviving tumour cells causing them to proliferate and express NK-cell-inhibitory receptors.
2.     The low number of latency-competent tumour cells which survive have properties of stem cells with expression of cell specific transcription factors. These cells maintain their dormancy by down-regulation of Wnt signalling due to increased expression of Dkk1. They also evade NK-mediated destruction by continued expression of NK-cell-inhibitory receptors.
3.     At a time in the future, the dormant cell comes to life as a metastatic lethal lesion following activation of the Wnt pathway, presumably via the intercession of a monocyte or macrophage.

 The author of the Editorial addresses possible ways in the future that these results may be translated into identifying these metastatic cell clusters and destroy them before they proliferate.

Recommended learning: Review the pathology and immunological mechanisms involved with metastatic disease.



Other Articles which should interest medical students



ORIGINAL ARTICLE

Extending Aromatase-Inhibitor Adjuvant Therapy to 10 Years


An additional 5 years of adjuvant aromatase-inhibitor therapy in women with early hormone-receptor–positive breast cancer resulted in longer disease-free survival and a lower incidence of contralateral breast cancer than placebo, but not in longer overall survival.


EDITORIAL

Changing Adjuvant Breast-Cancer Therapy with a Signal for Prevention


This is a double-blind, placebo controlled trial involving 1918 post-menopausal women with previously treated hormone receptor positive breast cancer which compares an aromatase inhibitor (letrozole) with placebo over an extended 5 year period.

This study commenced at a median time from initial diagnosis of 10.6 years (which is the time over which most metastatic lesions would have become apparent). 79% of women had been treated initially with tamoxifen (70% from between 4.5 - 6 years) followed by an aromatase inhibitor for a additional median duration of 5 years. These patients were then entered in the study.

The results of the study indicated:

1.     A significant reduction in the annual incidence rate of contralateral breast cancer (letrozole= 0.21% versus placebo 0.49%, P=0.007) (see Figure 2)
2.     No significant difference in overall survival rate between the letrazole and placebo treated groups, as expected.
3.     A disease free survival greater for the letrozole treated group which was defined as either disease recurrence or new disease in the contralateral breast.  This result was predicted.
4.     A higher incidence of bone pain, fractures and new-onset osteoporosis in the letrozole group, which would be expected, as no early treatment with bisphosphonates was initiated.
5.     The influence of letrozole on hot flashes, arthralgia, myalgia and quality of life was not as pronounced as that seen in earlier studies.
6.     That there were no signals to date for increased cardiovascular risks

There was a discussion in the Editorial regarding the use of aromatase inhibitors in primary prevention of breast cancer, comparing this with cardiologists and their use of drugs in primary prevention of cardiovascular disease.



ORIGINAL ARTICLE

HIV Infection Linked to Injection Use of Oxymorphone in Indiana, 2014–2015


A rapid spread of HIV type 1 was identified in a community in Indiana and was found to be related to injection use of oxymorphone.

The article describes 11 new diagnoses of HIV infection in a small community in Indiana associated with IV injection of oxymorphone.

 The messages I got from this article were:

1.     Within one month of initiating a needle exchange program, there was a dramatic fall in the number of new HIV cases reported (what’s new?), and
2.     Who else but Donald Trump would choose a vice-presidential running mate (Mike Pence) who is the current unpopular governor of the ultraconservative Republican state of Indiana and who, because of his evangelical “principles,” opposed needle exchange until public pressure forced him to agree to change his “principles.”  Even in a right wing state like Indiana, it is obvious that the citizens have a higher regard for the health of others than their highly unpopular governor.