Pulmonary hypertension in sickle cell hemoglobinopathy: a clinicopathologic study of 20 cases

Pulmonary hypertension is one of the major causes of morbidity and mortality of patients with sickle cell hemoglobinopathy (SCH). Although a clinically recognized complication of sickle cell disease (SCD), there are few published pathologic studies of pulmonary findings in these patients. The aim of this study was to define the pulmonary pathologic changes and to investigate correlation between the pathologic changes, the antemortem diagnosis of pulmonary hypertension, and the severity of SCH. Cases of SCH were identified from the autopsy database using Snomed codes. Clinical and echocardiograph data were collected for correlation with the pathologic data. A total of 20 adult patients (12 males and 8 females) were identified. Hemoglobin electrophoresis results were available for 16 patients, with hemoglobin S fraction percentages ranging from 23% to 97.8%. Eleven patients had SCD, 5 patients had sickle cell trait (SCT), and the remaining 4 patients without hemoglobin electrophoresis were included in the SCT group. The mean age of the SCT group was higher than that of the SCD group (P = 0.03). Histologically, all 20 patients demonstrated changes in pulmonary vasculature considered diagnostic of pulmonary hypertension grade I to grade IV, associated with plexiform lesions in 60% of patients. Medial hypertrophy and intimal hyperplasia/fibrosis, considered potentially reversible lesions, were seen in all patients. A weak association was found between SCD and plexiform lesions. Fibroelastic degeneration of small arteries, arterioles, and venules was identified in almost all (95%) cases. Clinically, tricuspid regurgitation was detected by echocardiogram in 10 of 20 (50%) patients; 6 of these 10 had significant regurgitation to allow estimation of systolic pressure. Sudden death occurred in 8 patients, with males having a significantly higher incidence. Cardiomegaly was present in 95% of patients, however, autosplenectomy and hepatic cirrhosis/hemochromatosis were observed almost exclusively in patients with SCD. Cirrhosis was found to have a strong positive association with SCD. This study demonstrates pulmonary hypertensive changes in all 20 autopsied patients who had SCH but died from various causes. We conclude that a high prevalence of pulmonary hypertension is associated with SCH with consequent high mortality. Therefore, patients with SCH would benefit from a regular periodic assessment for pulmonary hypertension regardless of age, sex, and severity of hemoglobinopathy.     

Epidemiological characteristics of sixty five cases of Kala-azar attending to a laboratory in Mymensingh

To find out the epidemiological characteristics of the patients with Kala-azar attending to a pathology laboratory at Mymensingh we studied retrospectively in a total of 65 patients. These patients were suspected to be Kala-azar as they were suffering from usually chronic fever, anaemia and splenomegaly. They were referred for serological detection of anti-k39 Leishmanial antibody by Immunochromatographic test (ICT) method. ICT positive cases were included for study. Majority cases were suffering from fever of more than 3 months (40%). Out of 65 patients 43 (66.15%) were males and 22 (33.85%) were females with a M:F ratio 2:1. Patients of 10 or less then 10 years of age were 17 (26.15%), in 11-20 years 23 (35.38%), in 21-30 years 13 (20.00%), in 31-40 years 5 (7.69%), in 41-50 years (6.15%) and in more than 50 years 3 (4.62%). Distribution of patients in different districts were: Mymensingh 54 (83.08%), Tangail 5 (7.69%), Jamalpur (4.62%), Netrokona 1 (1.54%) and Kishorgonj 1 (1.54%). In Mymensingh district patients were distributed as following Upazilla:Trishal 22 (40.74%), Fulbaria 11 (20.37%), Mymensingh Sadar 7 (12.96%), Gaforgaon 7 (12.96%),Bhaluka 5 (9.96%), Fulpur 1 (1.85%) and Nandail 1 (1.85%). Patients were found to scattered among different Unions of the affected Upazillas. The details addresses of the Kala-azar patients are recorded in authors computer databases. This may help in the further study regarding pathogenesis, reservoir and vectors of Leishmania in endemic areas. It may also helps in the community based study of Kala-azar. Present study supports that Kala-azar is still prevailing in the south-western region of greater Mymensingh in Bangladesh of which males and the adolescents are more affected.     

Bioabsorption qualities of chitosan-absorbable vascular templates(1)

PURPOSE:The scope of endovascular surgical techniques has expanded to include the treatment of diseases considered at one time to be amenable only to surgical treatment. The development of the biodegradable template follows as an extension of current permanent stent technology. The goal of our project is to develop and test chitosan as an absorbable template for the vascular system.Ultrapure chitosan, heparin sodium salt and lysozyme, and contrast agents MD-76R and Oxilan-350 were used to give radioopaque quality. Prototype chitosan vascular templates were obtained by a dip coating method in which alternate layers of chitosan were coagulated with nonsolvents or heparin. The amount of loaded and released heparin was determined using Azure II colorimetric assay. In vitro enzymatic degradation of templates was evaluated using lysozyme solutions in phosphate buffered saline. Mechanical properties were analyzed using the Dynamic Mechanical Analyzer, DMA-7 (Perkin Elmer, Foster City, Calif.). The microstructure of freeze-dried templates was investigated by field emission scanning electron microscopy (FE SEM) using an LEO 982 electron microscope (Zeiss, Thornwood, NY).In vivo deployment of the templates was undertaken in 10 full-sized pigs (Sus scrofa). After open expose and control of the iliac artery, a closed balloon catheter technique was used to advance and place the balloon catheter and template. The balloon was then expanded, deploying a Palmaz stent with a chitosan template anchored distally. Patency and deployment of the stent-template complex was confirmed by an arteriogram. The animals were sacrificed at 1, 2, 3, 4, and 5 weeks poststent placement, and arterial sections were taken for microscopic analysis. The amount of chitosan remaining was estimated to determine an in vivo rate of absorption.On hematoxilyn and eosin staining of the section arterial samples, a marked inflammatory response was noted and progressed with duration of in vivo contact. A giant cell foreign body reaction coupled with intense intimal hyperplasia and organized thrombus was also noted and progressed with duration of time in vivo. Also noted was the degradation of the template material with only small remnants of material noted within the giant cell by week 4. Clinically, none of the pigs developed limb ischemia or evidence of thromboembolic events.In this in vivo study, the chitosan template proved to be biodegradable but elicited an intense thrombotic and foreign body reaction despite heparin bonding. Further investigation is ongoing as to decreasing the thrombogenic and antigenic qualities of the template materials by either alteration of the base material or addition of bioactive side chains.     

Cystic Optic Chiasm Lesion: Atypical Magnetic Resonance Imaging Findings

Intrinsic cystic lesions in the optic chiasm are an uncommon cause of bitemporal hemianopia compared with compressive lesions extrinsic to the chiasm. A 40-year-old man presented with difficulty driving. Clinical assessment revealed a bitemporal hemianopia. Magnetic resonance imaging showed an unusual cystic appearance of the chiasm. The appearance was felt to be most likely secondary to previous infective or inflammatory disease, but biopsy was not undertaken given the very significant risk of further visual loss.     

The metabolic abnormalities associated with non-alcoholic fatty liver disease

Non-alcoholic fatty liver disease (NAFLD) is a common disorder in the Western hemisphere. It encompasses two histological lesions: fatty liver and steatohepatitis. A large body of literature indicates that insulin resistance is a key pathophysiological abnormality in patients with NAFLD. Insulin resistance results from a complex interplay between the major targets of insulin action, i.e. muscle, adipose tissue and liver, versus the ability of the pancreatic islet beta cells to compensate for insulin resistance by increasing insulin production. The metabolic and clinical profile associated with insulin resistance is thus defined by the factors that produce and maintain insulin resistance and the effects of decreased insulin sensitivity on various insulin-dependent pathways. The major metabolic defects associated with insulin resistance are increased peripheral lipolysis, increased hepatic glucose output due to increased gluconeogenesis and increased lipid oxidation. This is associated with an oxidative stress in the liver that may be compounded by additional pathophysiological abnormalities. While much work remains to be done, the current understanding of the pathogenesis of NAFLD provides direction for both future investigation and development of therapeutic trials.     

In-vitro analysis of APA microcapsules for oral delivery of live bacterial cells

Oral administration of microcapsules containing live bacterial cells has potential as an alternative therapy for several diseases. This article evaluates the suitability of the alginate-poly-L-lysine-alginate (APA) microcapsules for oral delivery of live bacterial cells, in-vitro, using a dynamic simulated human gastro-intestinal (GI) model. Results showed that the APA microcapsules were morphologically stable in the simulated stomach conditions, but did not retain their structural integrity after a 3-day exposure in simulated human GI media. The microbial populations of the tested bacterial cells and the activities of the tested enzymes in the simulated human GI suspension were not substantially altered by the presence of the APA microcapsules, suggesting that there were no significant adverse effects of oral administration of the APA microcapsules on the flora of the human gastrointestinal tract. When the APA microcapsules containing Lactobacillus plantarum 80 (LP80) were challenged in the simulated gastric medium (pH = 2.0), 80.0% of the encapsulated cells remained viable after a 5-min incubation; however, the viability decreased considerably (8.3%) after 15 min and dropped to 2.6% after 30 min and lower than 0.2% after 60 min, indicating the limitations of the currently obtainable APA membrane for oral delivery of live bacteria. Further in-vivo studies are required before conclusions can be made concerning the inadequacy of APA microcapsules for oral delivery of live bacterial cells.     

Effect of Cissampelos pareira root extract on isoproterenol-induced cardiac dysfunction

The aim of this study was to assess the cardioprotective effect of Cissampelos pareira root extract on isoproterenol-induced cardiac dysfunction in rats. Male albino Wistar rats were randomly divided into eight groups and received either normal saline (0.5?ml/kg, intraperitoneally), isoproterenol (5?mg/kg, intraperitoneally), C. pareira (100 and 200?mg/kg, by gavage, respectively) alone, amlodipine (9?mg/kg, by gavage) alone, C. pareira (100 and 200?mg/kg, respectively)?+?isoproterenol and amlodipine (9?mg/kg)?+?isoproterenol, once a day for 30?days, respectively. Isoproterenol-induced cardiac dysfunction was characterized by a significant (P?<?0.001) increase in the heart weigh/body weight ratio, serum calcineurin, nitric oxide, lactate dehydrogenase, and thiobarbituric acid reactive substance levels, as well as a significant decrease in serum-reduced glutathione, cardiac glutathione peroxidase, glutathione reductase, and glutathione-S-transferase levels, which were significantly (P?<?0.05 and P?<?0.01) improved by C. pareira treatment. No significant alteration was observed in the group treated with C. pareira alone compared with the control. C. pareira treatment also restored histopathological changes observed in isoproterenol-induced rats. Amlodipine is used as standard drug in this study. Thus, these results suggest that the attenuation of isoproterenol-induced cardiac dysfunction by treatment with ethanolic root extract of C. pareira may be due to amelioration of calcineurin activity and free radical formation, and by augmentation of antioxidant enzymes activities.