521 results on '"Bhan, M K"'
Search Results
152. Enteroaggregative Escherichia coli Associated with Persistent Diarrhea in a Cohort of Rural Children in India
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Bhan, M. K., primary, Raj, P., additional, Levine, M. M., additional, Kaper, J. B., additional, Bhandari, N., additional, Srivastava, R., additional, Kumar, R., additional, and Sazawal, S., additional
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- 1989
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153. Antireticulin Antibodies
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Khoshoo, V., Bhan, M. K., Unsworth, D. J., Kumar, R., and Smith, J. A. Walker
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R-1 anti-reticulin antibodies (ARA) were present in sera of 10 of the 12 children who subsequently fulfilled the ESPGAN diagnostic criteria for celiac disease (CD), hut was not found in any children in the age-matched control groups, viz., severely malnourished (n = 20). acute gastroenteritis (n = 23), normally nourished asymptomatic (n = 38), and 42 children with protracted diarrhoea and failure to thrive due to nonceliac causes. ARA was a highly specific (100) and sensitive (83) assay for the early diagnosis of CD. A positive ARA assay with an initial subtotal villous atrophy was seen to always suggest CD, and these together would provide a useful basis for instituting gluten-free diets in suspected cases of CD rather than histological findings alone, which may be often present in children in the third world with protracted diarrhoea and associated severe malnutrition.
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- 1988
154. Child Neurodevelopment After Multidomain Interventions From Preconception Through Early Childhood: The WINGS Randomized Clinical Trial.
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Upadhyay, Ravi Prakash, Taneja, Sunita, Chowdhury, Ranadip, Dhabhai, Neeta, Sapra, Savita, Mazumder, Sarmila, Sharma, Sitanshi, Tomlinson, Mark, Dua, Tarun, Chellani, Harish, Dewan, Rupali, Mittal, Pratima, Bhan, M. K., and Bhandari, Nita
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NEURODEVELOPMENTAL treatment for infants , *EARLY intervention (Education) , *NEURAL development , *CLINICAL trials , *TODDLERS development , *SOCIAL support , *CHILD development - Abstract
Key Points: Question: How does a package of multidomain interventions addressing health, nutrition, psychosocial care and support, and environmental hygiene delivered during preconception, pregnancy, and early childhood affect child neurodevelopment at 24 months? Findings: In this second report of a randomized trial in India assessing interventions during preconception, pregnancy, and early childhood on childhood preterm births and childhood growth as primary outcomes, the secondary outcome was neurodevelopment at 24 months. Among 1712 children assessed, preconception, pregnancy, and early childhood interventions were associated with modest improvements in scores and lower incidence of moderate to severe neurodevelopmental delay in the cognitive, language, and socioemotional domains. Meaning: Multidomain interventions in the preconception period, along with those in pregnancy and early childhood, may be beneficial for child neurodevelopment. Importance: Multidomain interventions in pregnancy and early childhood have improved child neurodevelopment, but little is known about the effects of additional preconception interventions. Objective: To evaluate the effect of a multifaceted approach including health; nutrition; water, sanitation, and hygiene (WASH); and psychosocial support interventions delivered during the preconception period and/or during pregnancy and early childhood on child neurodevelopment. Design, Setting, and Participants: In this randomized trial involving low- and middle-income neighborhoods in Delhi, India, 13 500 participants were assigned to preconception interventions or routine care for the primary outcome of preterm births and childhood growth. Participants who became pregnant were randomized to pregnancy and early childhood interventions or routine care. Neurodevelopmental assessments, the trial's secondary outcome reported herein, were conducted in a subsample of children at age 24 months, including 509 with preconception, pregnancy, and early childhood interventions; 473 with preconception interventions alone; 380 with pregnancy and early childhood interventions alone; and 350 with routine care. This study was conducted from November 1, 2000, through February 25, 2022. Interventions: Health, nutrition, psychosocial care and support, and WASH interventions delivered during preconception, pregnancy, and early childhood periods. Main Outcomes and Measures: Cognitive, motor, language, and socioemotional performance at age 24 months, assessed using the Bayley Scales of Infant and Toddler Development 3 tool. Results: The mean age of participants at enrollment was 23.8 years (SD, 3.0 years). Compared with the controls at age 24 months, children in the preconception intervention groups had higher cognitive scores (mean difference [MD], 1.16; 98.3% CI, 0.18-2.13) but had similar language, motor, and socioemotional scores as controls. Those receiving pregnancy and early childhood interventions had higher cognitive (MD, 1.48; 98.3% CI, 0.49-2.46), language (MD, 2.29; 98.3% CI, 1.07-3.50), motor (MD, 1.53; 98.3% CI, 0.65-2.42), and socioemotional scores (MD, 4.15; 98.3% CI, 2.18-6.13) than did controls. The pregnancy and early childhood group also had lower incidence rate ratios (RRs) of moderate to severe delay in cognitive (incidence RR, 0.62; 98.3% CI, 0.40-0.96), language (incidence RR, 0.73; 98.3% CI, 0.57-0.93), and socioemotional (incidence RR, 0.49; 98.3% CI, 0.24-0.97) development than did those in the control group. Children in the preconception, pregnancy, and early childhood intervention group had higher cognitive (MD, 2.60; 98.3% CI, 1.08-4.12), language (MD, 3.46; 98.3% CI, 1.65-5.27), motor (MD, 2.31; 98.3% CI, 0.93-3.69), and socioemotional (MD, 5.55; 98.3% CI, 2.66-8.43) scores than did those in the control group. Conclusions and Relevance: Multidomain interventions during preconception, pregnancy and early childhood led to modest improvements in child neurodevelopment at 24 months. Such interventions for enhancing children's development warrant further evaluation. Trial Registration: Clinical Trials Registry–India CTRI/2017/06/008908 This randomized trial assesses interventions that span preconception through early childhood compared with usual care on neurodevelopment among children at age 24 months in low- and middle-income neighborhoods in India. [ABSTRACT FROM AUTHOR]
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- 2024
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155. Rotavirus infection and persistent diarrhoea in young children.
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Khoshoo, V, Bhan, M K, Jayashree, S, Kumar, R, and Glass, R I
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RETROVIRUS diseases , *IMMUNOGLOBULIN analysis , *DIARRHEA , *LONGITUDINAL method , *VIRAL antibodies , *ROTAVIRUSES , *ACUTE diseases , *DIAGNOSIS - Published
- 1990
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156. Rotavirus-Specific Antibody Response in Saliva of Infants with Rotavirus Diarrhea.
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Aiyar, Jayashree, Bhan, M. K., Bhandari, Nita, Kumar, Ramesh, Raj, Pushker, and Sazawal, Sunil
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The reliability of saliva as an indicator of rotavirus infection was assessed among 15 infants (3–12 months) with rotaviral and 15 with nonrotaviral diarrhea. Paired salivary samples collected during acute and convalescent phases were tested for rotavirus-specific IgA and IgM byan ELISA. The sensitivity ofIgA or IgM alone to predict infection was 53.3% and 46.6%, respectively; used in conjunction, the sensitivity rose to 80%. It seems that infants with rotaviral diarrhea mount mucosal antibody responses as reflected in their saliva; possibly salivary antibodies could beused to evaluate vaccine “take” in rotavirus vaccine trials. [ABSTRACT FROM PUBLISHER]
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- 1990
157. New type of cholera.
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Jain, Y., Das, B., Bhan, M., and Bhan, M K
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- 1993
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158. Mutational landscape of gingivo-buccal oral squamous cell carcinoma reveals new recurrently-mutated genes and molecular subgroups.
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Maitra, Arindam, Biswas, Nidhan K., Amin, Kishore, Kowtal, Pradnya, Kumar, Shantanu, Das, Subrata, Sarin, Rajiv, Majumder, Partha P., Bagchi, I, Bairagya, B. B., Basu, A., Bhan, M. K., Chaturvedi, P., Das, D., D'Cruz, A., Dhar, R., Dutta, D., Ganguli, D., Gera, P., and Gupta, T.
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- 2013
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159. Picture of the Month
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Gellis, Sydney S., Feingold, Murray, Srivastava, R. N., Azamy, Shafiga, Ziayee, M. H., and Bhan, M. K.
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DENOUMENT AND DISCUSSION ROTHMUND-THOMSON SYNDROME (POIKELODERMA CONGENITAL) MANIFESTATIONS This rare disorder is characterized by distinctive cutaneous abnormalities. Maculopapular, erythematous lesions with patches of hypopigmentation usually over the cheeks first appear at the age of 3 to 6 months. Subsequently, they are observed over the rest of the face, dorsum of hands and gluteal regions, forearms, and legs. Photosensitivity may be present. In advanced stages, telangiectases, brownish hyperpigmentation, and reticular, depigmented patches of skin atrophy are seen. Keratoses may develop on exposed skin after several years and squamous cell carcinoma may occur in the keratoses or neighboring skin.Bilateral cataracts are present in approximately 50% to 75% of the patients. They usually appear by age 7 years and may be anterior, subcapsular, perinuclear, or posterior stellate.Other features of the syndrome include premature senile appearance, bird-like facies, diminished scalp hair, hypogonadism, short stature, small hands and feet, and hypoplastic thumbms. Mental
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- 1978
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160. Review Of G And P Typing Results From A Global Collection Of Rotavirus Strains: Implications For Vaccine Development.
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Gentsch, J. R., Woods, P. A., Ramachandran, M., Das, B. K., Leite, J. P., Alfieri, A., Kumar, R., Bhan, M. K., and Glass, R. I.
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Candidate rotavirus vaccines have been prepared with reassortant strains specifically to protect against the 4 major rotavirus G serotypes (Gl-4). Many studies using P (VP4) genotyping methods have indicated that, worldwide, rotavirus strains of the 4 common G serotypes are each associated with 1 P genotype: Gt, G3, and G4 are associated with P[8], and G2 is associated with P[4]. In contrast, G and P genotyping of rotavirus in specimens from India revealed that a high percentage of the childhood diarrhea strains belong to genotype P[6], and the most common strain had an unusual G serotype, G9. Similarly, in all regions surveyed in Brazil, apparent reassortants of genotype P[8], G5 were found in children with gastroenteritis. These studies indicate that while rotavirus strains have limited diversity in many settings, reassortment between common and uncommon serotypes or animal strains can arise in some settings and, thus, lead to unusual diversity. [ABSTRACT FROM PUBLISHER]
- Published
- 1996
161. Chlamydia trachomatisInfection Among Pregnant Women Prevalence and Prenatal Importance
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Paul, V. K., Singh, M., Gupta, U., Buckshee, K., Bhargava, V. L., Takkar, D., Nag, V. L., Bhan, M. K., and Deorari, A. K.
- Abstract
Because the prevalence of chlamydial infection in pregnant Indian women, as well as its associations with low birth weight and prematurity, remains unclear, a preliminary study was conducted to ascertain the prevalence of infection with Chlamydia trachomatisin 94 pregnant women in midgestation attending an antenatal clinic. An additional prevalence study focused on 172 women who presented after 26 weeks’ gestation in spontaneous labor. None had multiple pregnancies or received erythromycin antenatally. Placenta previa and stillbirths were other grounds for exclusion. This group included mainly housewives less than 30 years old who had at least a high school education, were married, and did not smoke or drink.
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- 2000
162. Serum and Salivary Antibodies as Indicators of Rotavirus Infection in Neonates
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Jayashree, S., Bhan, M. K., Kumar, R., Raj, P., Glass, R., and Bhandari, N.
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- 1988
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163. ENTEROAGGREGATIVE ESCHERICHIA COLI PRODUCE A HEATLABILE TOXIN WHICH HAS HOMOLOGY WITH HAEMOLYSIN A
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Baldwin, T. J., Williams, P. H., Knutton, S., Sellers, L., Hernandez, A., Aitken, A., Bhan, M. K., and McNeish, A. S.
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- 1991
164. Mid upper arm circumference as a predictor of risk of mortality in children in a low resource setting in India.
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Taneja, Sunita, Rongsen-Chandola, Temsunaro, Mohan, Sanjana Brahmawar, Mazumder, Sarmila, Bhandari, Nita, Kaur, Jasmine, Arya, Nikita, Chowdhury, Ranadip, Martines, Jose Carlos, Bahl, Rajiv, and Bhan, M. K.
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ARM circumference , *CHILD mortality , *DEATH rate , *PUBLIC health , *CAUSES of death - Abstract
Objective: In this secondary analysis of data from an intervention trial, we assessed the performance of Mid Upper Arm Circumference (MUAC) as a predictor of mortality in children aged 6–59 months from Delhi, India, one year after their initial MUAC measurements were taken. Additionally, we assessed MUAC as an absolute value and MUAC z-scores as predictors of risk of mortality. Methods: In the trial, children were screened using MUAC prior to referral to the study clinic. These children were revisited a year later to ascertain their vital status. Baseline MUAC and MUAC z-scores were used to categorize children as severely (MUAC <115 mm, MUAC z-score <-3SD) or moderately (MUAC 115 to <125 mm, MUAC z-score <-2SD) malnourished. The proportion of malnutrition, risk of mortality, relative risk estimates, positive predictive value and area under the curve (AUC) by MUAC and MUAC z-scores were calculated. Results: In the resurvey, the first 36159 children of the 48635 in the initial survey were contacted. Of these, vital status of 34060 (94.2%) was available. The proportion of severe malnutrition by MUAC (<115 mm) was 0.5% with an associated mortality of 4.7% over a one year period and an attributable mortality of 13% while the proportion of the severe malnutrition by MUAC z-score (<-3SDwas 0.9% with an associated mortality of 2.2%. Conclusions: MUAC is a significant predictor of subsequent mortality in under-five children. In settings where height measurement is not feasible, MUAC can be used as a screening tool for identifying severely malnourished children for management. [ABSTRACT FROM AUTHOR]
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- 2018
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165. International network of cancer genome projects.
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Hudson (Chairperson), Thomas J., Anderson, Warwick, Aretz, Axel, Barker, Anna D., Bell, Cindy, Bernabé, Rosa R., Bhan, M. K., Calvo, Fabien, Eerola, Iiro, Gerhard, Daniela S., Guttmacher, Alan, Guyer, Mark, Hemsley, Fiona M., Jennings, Jennifer L., Kerr, David, Klatt, Peter, Kolar, Patrik, Kusuda, Jun, Lane, David P., and Laplace, Frank
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GENETIC mutation , *TUMORS , *GENOMES , *CANCER treatment , *ONCOGENES , *PROGNOSIS - Abstract
The International Cancer Genome Consortium (ICGC) was launched to coordinate large-scale cancer genome studies in tumours from 50 different cancer types and/or subtypes that are of clinical and societal importance across the globe. Systematic studies of more than 25,000 cancer genomes at the genomic, epigenomic and transcriptomic levels will reveal the repertoire of oncogenic mutations, uncover traces of the mutagenic influences, define clinically relevant subtypes for prognosis and therapeutic management, and enable the development of new cancer therapies. [ABSTRACT FROM AUTHOR]
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- 2010
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166. Quantitative Evaluation of Rotaviral Antigenemia in Children with Acute Rotaviral Diarrhea.
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Ray, Pratima, Fenaux, Martijn, Sharma, Sumit, Malik, Jyoti, Subodh, Swati, Bhatnagar, Shinjini, Greenberg, Harry, Glass, Roger I., Gentsch, Jon, and Bhan, M. K.
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GASTROENTERITIS in children , *ROTAVIRUSES , *GASTROINTESTINAL diseases , *SERUM , *RNA , *GASTROENTERITIS , *DIARRHEA - Abstract
Background. Rotaviral antigen and RNA have recently been identified in the serum of patients with rotaviral gastroenteritis, but the roles they play in disease remains undetermined. Methods. Rotaviral antigen and RNA were quantified by enzyme-linked immunosorbant assay and by quantitative reverse-transcription polymerase chain reaction in stool and serum specimens from children with rotaviral diarrhea (n = 102), children with nonrotaviral diarrhea (n = 40), and nondiarrheal control children (n = 30). Results. Rotaviral antigenemia was detected in 64%, 3%, and 0% of the children with rotaviral diarrhea, the children with nonrotaviral diarrhea, and the nondiarrheal control children, respectively. The level of rotaviral antigen in serum was ∼2×10²-fold lower than that in stool, and a moderate correlation was observed between the 2 levels. Rotaviral RNA was detected in 93% of the antigen-positive serum specimens. The median number of RNA copies in serum was ∼1×105-fold lower than that in stool, and no correlation was observed between the 2 levels. Serum levels of both antigen and RNA were inversely associated with baseline titers of rotaviral serum immunoglobulin G (P<.01). Antigenemia was also associated with G1 serotype. Conclusions. Rotaviral antigenemia and viremia were common in children with rotaviral diarrhea, but antigen and RNA levels in serum were substantially lower than those in stool. Antigenemia was associated with infection with G1 strains and with low baseline titers of rotaviral serum antibody. [ABSTRACT FROM AUTHOR]
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- 2006
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167. Incidence of Severe Rotavirus Diarrhea in New Delhi, India, and G and P Types of the Infecting Rotavirus Strains.
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Bahl, Rajiv, Ray, Pratima, Subodh, Swati, Shambharkar, Prashant, Saxena, Manju, Parashar, Umesh, Gentsch, Jon, Glass, Roger, and Bhan, M. K.
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DIARRHEA , *ROTAVIRUS diseases , *VIRUS diseases , *MEDICAL care , *INTESTINAL diseases - Abstract
A total of 62,475 children <5 years old from a defined population of ∼500,000 children and adults from slums in New Delhi, India, were assessed for 1 year by means of passive surveillance, to identify children who were hospitalized for diarrhea. The incidence of severe rotavirus diarrhea was estimated, and the G and P types of the infecting rotavirus strains were determined and were correlated with the clinical severity of diarrhea. Of 584 children who were hospitalized with diarrhea, 137 (23.5%) had rotavirus detected in stool specimens (incidence of rotavirus diarrhea-associated hospitalizations, 337 hospitalizations/100,000 children <5 years of age). Most cases of diarrhea (98%) occurred during the first 2 years of life, peaking at 9-11 months of age. Rotavirus-associated diarrhea occurred year-round but was predominant in winter. Among the strains that could be G-typed, G1 was the most common serotype, followed by G9 and G2; 10% of cases of diarrhea were due to mixed G-type infections. Common strains identified in the present surveillance study were P[8]G1, P[4]G2, P[8]G9, P[6]G1, P[6]G9, and P[6]G3. Children infected with G1 strains had a greater risk of developing more-severe cases of diarrhea than did children infected with other rotavirus strains (odds ratio, 2.95; 95% confidence interval, 1.3-6.67). [ABSTRACT FROM AUTHOR]
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- 2005
168. Bacteriuria and urinary tract infections in malnourished children.
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Bagga, Arvind, Tripathi, Partha, Jatana, Vishal, Hari, Pankaj, Kapil, Arti, Srivastava, R. N., and Bhan, M. K.
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MALNUTRITION in children , *URINARY tract infections in children , *DIARRHEA in children , *FEVER in children - Abstract
Cites findings of a study conducted to examine the incidence of bacteriuria and urinary tract infections (UTI) in malnourished children. Examination of the clean-catch and suprapubic urine specimens in the study; Impact of diarrhea and fever on the risk of bacterium and UTI; Association of bacterium with symptoms and elevated levels of acute-phase reactants; Significance of urinalysis in screening for UTI.
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- 2003
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169. Selection of single chain variable fragments (scFv) against the glycoprotein antigen of the rabies virus from a human synthetic scFv phage display library and their fusion with the Fc region of human IgG1.
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Ray, K., Embleton, M. J., Jailkhani, B. L., Bhan, M. K., and Kumar, R.
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RABIES virus , *ANTIGENS , *BACTERIOPHAGES - Abstract
We have prepared human recombinant antibody molecules against the glycoprotein antigen of the rabies virus (GPRV) based on the single chain variable fragment (scFv) format. Anti-GPRV scFvs were selected from a human synthetic scFv phage display library with a repertoire of approximately 109 specificities. After three rounds of selection against the PV11 strain of the virus, 40% of the clones tested recognized the rabies antigen. Of the 20 positive clones that were sequenced, five distinct sequences were identified. These distinct scFvs were cloned into a mammalian expression vector carrying the human IgG1 Fc region. The specificity of the resulting scFv-Fc molecules for GPRV was established by ELISA, dot blot and western blot analyses and membrane immunofluorescence. Two of the scFv-Fc fusion proteins neutralized the PV11 strain in a standard in vivo neutralization assay where the virus was incubated with the scFv-Fc molecules before intracranial inoculation in mice. These anti-GPRV scFv-Fc molecules have the potential to be used as an alternative to the presently available HRIG, for use in post-exposure preventive treatment. [ABSTRACT FROM AUTHOR]
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- 2001
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170. Impact of a package of health, nutrition, psychosocial support, and WaSH interventions delivered during preconception, pregnancy, and early childhood periods on birth outcomes and on linear growth at 24 months of age: factorial, individually randomised controlled trial.
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Taneja S, Chowdhury R, Dhabhai N, Upadhyay RP, Mazumder S, Sharma S, Bhatia K, Chellani H, Dewan R, Mittal P, Bhan MK, Bahl R, and Bhandari N
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- Pregnancy, Infant, Newborn, Child, Child, Preschool, Female, Humans, Psychosocial Support Systems, Water, Hygiene, Growth Disorders, Sanitation, Psychiatric Rehabilitation
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Objective: To determine the effect of integrated and concurrent delivery of health, nutrition, water, sanitation and hygiene (WaSH), and psychosocial care interventions during the preconception period alone, during pregnancy and early childhood, and throughout preconception, pregnancy, and early childhood on birth outcomes and linear growth at 24 months of age compared with routine care., Design: Individually randomised factorial trial., Setting: Low and middle income neighbourhoods of Delhi, India., Participants: 13 500 women were randomised to receive preconception interventions (n=6722) or routine care (n=6778). 2652 and 2269 pregnant women were randomised again to receive pregnancy and early childhood interventions or routine care. The analysis of birth outcomes included 1290 live births for the preconception, pregnancy, and early childhood interventions (group A), 1276 for the preconception intervention (group B), 1093 for the pregnancy and early childhood interventions (group C), and 1093 for the control (group D). Children aged 24 months by 30 June 2021 were included in the 24 month outcome analysis (453 in group A, 439 in B, 293 in C, and 271 in D)., Interventions: Health, nutrition, psychosocial care and support, and WaSH interventions were delivered during preconception, pregnancy, and early childhood periods., Main Outcome Measures: The primary outcomes were low birth weight, small for gestational age, preterm, and mean birth weight. At 24 months, the outcomes were mean length-for-age z scores and proportion stunted. Three prespecified comparisons were made: preconception intervention groups (A+B) versus no preconception intervention groups (C+D); pregnancy and early childhood intervention groups (A+C) versus routine care during pregnancy and early childhood (B+D) and preconception, pregnancy, and early childhood interventions groups (A) versus control group (D)., Results: The proportion with low birth weight was lower in the preconception intervention groups (506/2235) than in the no preconception intervention groups (502/1889; incidence rate ratio 0.85, 98.3% confidence interval 0.75 to 0.97; absolute risk reduction -3.80%, 98.3% confidence interval -6.99% to -0.60%). The proportion with low birth weight was lower in the pregnancy intervention groups (502/2096) than in the no pregnancy intervention groups (506/2028) but the upper limit of the confidence interval crossed null effect (0.87, 0.76 to 1.01; -1.71%, -4.96% to 1.54%). There was a larger effect on proportion with low birth weight in the group that received interventions in the preconception and pregnancy periods (267/1141) compared with the control group (267/934; 0.76, 0.62 to 0.91; -5.59%, -10.32% to -0.85%). The proportion stunted at 24 months of age was substantially lower in the pregnancy and early childhood intervention groups (79/746) compared with the groups that did not receive these interventions (136/710; 0.51, 0.38 to 0.70; -8.32%, -12.31% to -4.32%), and in the group that received preconception, pregnancy, and early childhood interventions (47/453) compared with the control group (51/271; 0.49, 0.32 to 0.75; -7.98%, -14.24% to -1.71%). No effect on stunting at 24 months was observed in the preconception intervention groups (132/892) compared with the no preconception intervention groups (83/564)., Conclusions: An intervention package delivered during preconception, pregnancy, and early childhood substantially reduced low birth weight and stunting at 24 months. Pregnancy and early childhood interventions alone had lower but important effects on birth outcomes and 24 month outcomes. Preconception interventions alone had an important effect on birth outcomes but not on 24 month outcomes., Trial Registration: Clinical Trial Registry-India CTRI/2017/06/008908., Competing Interests: Competing interests: All authors have completed the ICMJE uniform disclosure form at www.icmje.org/disclosure-of-interest/ and declare: support from the Biotechnology Industry Research Assistance Council of the Department of Biotechnology, Government of India and Bill and Melinda Gates Foundation, USA for the submitted work; no financial relationships with any organizations that might have an interest in the submitted work in the previous three years; no other relationships or activities that could appear to have influenced the submitted work., (© Author(s) (or their employer(s)) 2019. Re-use permitted under CC BY. No commercial re-use. See rights and permissions. Published by BMJ.)
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- 2022
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171. Emergence of G12 rotavirus strains in Delhi, India, in 2000 to 2007.
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Sharma S, Ray P, Gentsch JR, Glass RI, Kalra V, and Bhan MK
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- Child, Child, Preschool, Communicable Diseases, Emerging virology, Diarrhea virology, Feces virology, Genotype, Humans, India epidemiology, Molecular Sequence Data, Phylogeny, Prevalence, Reverse Transcriptase Polymerase Chain Reaction, Rotavirus genetics, Rotavirus Infections virology, Sequence Analysis, DNA, Antigens, Viral genetics, Capsid Proteins genetics, Communicable Diseases, Emerging epidemiology, Diarrhea epidemiology, Rotavirus classification, Rotavirus isolation & purification, Rotavirus Infections epidemiology
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The prospect that rotavirus diarrhea in children may soon be prevented by vaccines has placed a new priority on understanding the diversity of rotavirus strains and the mechanism by which these strains evolve over time. We have characterized a total of 465 rotavirus strains collected in North India from 2000 to 2007 for G and P types by reverse transcription-PCR and sequencing. The novel G12 rotavirus strains recently detected in other countries were first detected in India in 2001 and have emerged as the predominant strains in Delhi, India, during 2005 to 2007. While the VP7 sequence was highly homologous among G12 strains isolated in Delhi, suggesting recent emergence from a common ancestor, the strains had a diverse constellation of other gene segments, demonstrating substantial reassortment. For the entire period, the common rotavirus G types G1 (26%), G2 (25%), and G9 (14%) comprised 65% of the strains, and common P types, P[4] (19%), P[6] (22%), and P[8] (35%), comprised 76% of the total P types. Of note, we detected a high percentage of unusual (17%) strains and fecal specimens with mixed (12% G and 15% P) rotavirus infections having a variety of genomic constellations. For the first time, we identified two novel rotavirus strains with unusual G/P combinations, G2P[11] and G3P[11], in patients with diarrhea. The study highlights the great diversity among rotaviruses isolated from Indian children, the opportunity for genetic reassortment between strains, and the emergence of a novel G12 strain in our country. Due to the demonstrated effect of antigenic diversity on rotavirus vaccines, it will be important to continue careful monitoring of these strains as rotavirus vaccine programs are implemented in India.
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- 2008
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172. Polymorphism in L-selectin, E-selectin and ICAM-1 genes in Asian Indian pediatric patients with celiac disease.
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Kaur G, Rapthap CC, Kumar S, Bhatnagar S, Bhan MK, and Mehra NK
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- Alleles, Amino Acid Substitution, Child, Gene Frequency, Humans, India, Polymorphism, Genetic, Celiac Disease genetics, E-Selectin genetics, Genetic Predisposition to Disease, Intercellular Adhesion Molecule-1 genetics, L-Selectin genetics
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Celiac disease (CD) follows an autoimmune course in which both genetic and environmental factors contribute to its development. A strong association with HLA class II molecules, predominantly HLA-DQ2, has been reported in most ethnic groups with CD. The aim of this study was to determine if genetic polymorphisms in L-selectin, E-selectin, and intercellular adhesion molecule-1 (ICAM-1) have any correlation with CD. We investigated 5 mutations, namely F206L in L-selectin, S128R and L554F in E-selectin, and G241R and K469E in ICAM-1, in 37 North Indian pediatric patients with CD. A significant increase in allele frequencies of 128R of E-selectin and the associated genotype SR was observed in patients. No significant differences were observed in the F206L polymorphism of L-selectin, or the G241R and E469K polymorphisms in the ICAM-1 gene in CD. This study illustrates that selectin gene polymorphism might contribute to the genetic background of CD and invites further investigation relevant to understanding the mechanisms underlying the immunopathogenesis of this autoimmune disease.
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- 2006
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173. Safety and immunogenicity of two live attenuated human rotavirus vaccine candidates, 116E and I321, in infants: results of a randomised controlled trial.
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Bhandari N, Sharma P, Glass RI, Ray P, Greenberg H, Taneja S, Saksena M, Rao CD, Gentsch JR, Parashar U, Maldonado Y, Ward RL, and Bhan MK
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- Double-Blind Method, Female, Humans, Infant, Male, Rotavirus genetics, Rotavirus Infections genetics, Rotavirus Infections immunology, Rotavirus Infections prevention & control, Rotavirus Vaccines genetics, Rotavirus immunology, Rotavirus Vaccines adverse effects, Rotavirus Vaccines immunology
- Abstract
We evaluated safety and immunogenicity of two orally administered human rotavirus vaccine candidates 116E and I321. Ninety healthy infants aged 8 weeks received a single dose of 116E (10(5)FFu (florescence focus units)), I321 (10(5)FFu) or placebo. There were no significant differences in the number of adverse events. Fever was reported by 6/30, 1/30 and 5/30 in the 116E, I321 and placebo groups; the corresponding figures for diarrhoea were 5/30, 8/29 and 3/30. Serum IgA seroconversion rates were 73%, 39% and 20% in the 116E, I321 and placebo groups, respectively. Vaccine virus was shed on days 3, 7 or 28 in 11/30 infants of the 116E and none in the other two groups. The 116E strain is attenuated, clinically safe and highly immunogenic with a single dose.
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- 2006
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174. Variability pattern and correlation studies in Silybum marianum Gaertn.
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Ram G, Bhan MK, Gupta KK, Thaker B, Jamwal U, and Pal S
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- Genotype, Humans, Genetic Variation, Silybum marianum genetics, Phytotherapy, Quantitative Trait, Heritable
- Abstract
Phenotypic and genotypic coefficient of variability, heritability in broad sense and genetic advance were determined investigating the characters of 15 accessions of Silybum marianum. Seed yield/plant and number of capsules/plant had highest estimates of genotypic variation, heritability and genetic advance which suggest that direct selection for these traits is suitable for the improvement of this crop. Number of capsules/plant had a significant positive correlation with the number of branches/plant and leaf length (r=0.3398, 0.7547), whereas seed yield/plant had a positive significant correlation with leaf length, stem diameter, capsule diameter and silymarin content (r=0.6830, 0.3140, 0.3484, 0.2925).
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- 2005
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175. Racecadotril-is there enough evidence to recommend it for treatment of acute diarrhea?
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Bhan MK and Bhatnagar S
- Subjects
- Antidiarrheals pharmacology, Humans, Thiorphan pharmacology, Thiorphan therapeutic use, Treatment Outcome, Antidiarrheals therapeutic use, Diarrhea drug therapy, Thiorphan analogs & derivatives
- Published
- 2004
176. Zinc supplementation for four months does not affect plasma copper concentration in infants.
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Sazawal S, Malik P, Jalla S, Krebs N, Bhan MK, and Black RE
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- Female, Hemoglobins analysis, Humans, Infant, Male, Time Factors, Zinc blood, Copper blood, Dietary Supplements, Zinc administration & dosage
- Abstract
Aim: The aim of the present study, which was undertaken as a sub-study within a randomized controlled trial of zinc supplementation, was to evaluate the effect of prolonged zinc supplementation on copper status as assessed by hematological markers., Methods: Plasma copper and zinc were estimated at baseline and after 120 d of supplementation in a randomly selected infant subset (115) of the children. Of these, 61 children were in a zinc group (Z) getting 10 mg of elemental zinc, and 54 were in a control group (C) getting supplement without zinc., Results: Baseline plasma zinc was comparable in the two groups; post-supplementation zinc was significantly higher (Z 93.0 +/- 3.6 vs C 60.6 +/- 8.0) in the zinc supplementation group. There was no significant difference in the mean/median copper levels between the zinc and control groups. The percentage of children with plasma copper <100 microg/dl was also not significantly different between groups (baseline Z 14.8%, C 11.1%; post-supplementation Z 18.0%, C 11.1%). There were no differences between the zinc and control groups after 120 d of supplementation in hemoglobin (Hgb), mean corpuscular volume (MCV), mean corpuscular hemoglobin concentration (MCHC), or number of lymphocytes or granulocytes., Conclusion: Zinc supplementation of 10 mg/d for 4 mo in this study did not affect copper status, as assessed by plasma copper concentration and hematological parameters, diagnostics of copper deficiency.
- Published
- 2004
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177. Consensus Statement of IAP National Task Force: status report on management of acute diarrhea.
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Bhatnagar S, Bhandari N, Mouli UC, and Bhan MK
- Subjects
- Antiemetics therapeutic use, Child, Diarrhea, Infantile drug therapy, Fluid Therapy, Humans, Infant, Osmolar Concentration, Probiotics therapeutic use, Randomized Controlled Trials as Topic, Zinc administration & dosage, Zinc therapeutic use, Diarrhea drug therapy
- Published
- 2004
178. Diffuse intra-abdominal fibromatosis-report of a new entity with review of literature.
- Author
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Singal AK, Agarwala S, Mannan SA, Gupta AK, Bhan MK, and Mitra DK
- Subjects
- Child, Decision Trees, Diagnosis, Differential, Fatal Outcome, Fibromatosis, Abdominal diagnostic imaging, Fibromatosis, Abdominal pathology, Fibromatosis, Abdominal surgery, Humans, Male, Tomography, X-Ray Computed, Fibromatosis, Abdominal diagnosis
- Abstract
Fibromatosis, arare non-neoplastic spindle cell proliferation of unknown aetiology, can occur anywhere in the body. Though extra-abdominal sites are commonly involved, intra-abdominal fibromatosis has also been described. Described herein is an unusual case of diffuse intra-abdominal fibromatosis in a 9-year-old boy, who could not be salvaged despite extensive medical management.
- Published
- 2004
179. Molecular characterization of serotype G2 and G3 human rotavirus strains that have an apparently identical electropherotype of the short RNA pattern.
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Nakagomi T, Gentsch JR, Das BK, Kumar R, Bhan MK, Glass RI, and Nakagomi O
- Subjects
- Base Sequence, Electrophoresis, Polyacrylamide Gel, Genotype, Humans, Molecular Sequence Data, Serotyping, Antigens, Viral, Capsid Proteins genetics, RNA, Viral analysis, Rotavirus classification, Rotavirus genetics
- Abstract
The literature is conflicting whether or not rotavirus strains with different G serotype have an identical electropherotype. This is a contentious but an important issue because large parts of molecular epidemiological studies of rotaviruses have been based on the conception that a single strain of rotavirus can be defined by a single electropherotype. Here, we examined in detail by reverse-transcription PCR genotyping, electropherotyping, sequencing, and genogrouping using RNA--RNA hybridization three human rotavirus strains isolated in India that had apparently identical electropherotypes although one strain was typed as P[4], G3 while the other two typed as P[4], G2. These three strains showed an identical electropherotype on 7.5% and 12.5% polyacrylamide gels, but co-electrophoresis on a 10% gel demonstrated that segment 8 of the P[4], G3 strain migrated more slowly than the cognate segment of the P[4], G2 strains. Genogrouping assay and nucleotide sequencing provided evidence for the hypothesis that the P[4], G3 stain was an intergenogroup reassortant in which a P[4], G2 strain of the DS-1 genogroup had acquired the VP7 gene from an yet-unidentified concurrently circulating G3 strain. While electropherotyping remains a valuable asset for molecular epidemiology of rotaviruses, this study underscores the importance of co-electrophoresis under different electrophoretic conditions when pinpointing subtle differences.
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- 2002
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180. Pediatric celiac disease in India is associated with multiple DR3-DQ2 haplotypes.
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Kaur G, Sarkar N, Bhatnagar S, Kumar S, Rapthap CC, Bhan MK, and Mehra NK
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- Adolescent, Alleles, Child, Child, Preschool, Female, Gene Frequency, Haplotypes, Humans, India, Infant, Male, Celiac Disease genetics, Celiac Disease immunology, HLA-DQ Antigens genetics, HLA-DR3 Antigen genetics
- Abstract
The role of human leukocyte antigen (HLA) DQ2 heterodimer (DQA1*0501-DQB1*0201) in presenting gluten peptides to effector T cells in celiac disease (CD) has been well documented. Because HLA-DQ2 is carried on DR3 haplotypes due to linkage disequilibrium, such haplotypes are encountered more frequently in patients with autoimmune disease. This study analyzed 35 North Indian children below 15 years of age and diagnosed to have CD as per the ESPGAN criteria, which included histopathologic alterations in duodenal biopsies, clinical response to gluten withdrawal, and presence of antiendomysial antibodies. The HLA class I and class II alleles were determined by polymerase chain reaction-sequence-specific primers, sequence-specific oligonucleotide probe, and reverse line strip molecular techniques. A statistically significant positive association of the disease with HLA-DRB1*03 (94.2% versus 22.1% in controls, chi(2) = 73.4, p = 7.54E-11), and a negative association with DRB1*15 (chi(2) = 7.4, p = 6.5E-03) and DRB1*13 alleles was observed. The HLA-DQB1*0201 was observed in all the 35 patients (100%), whereas the DQ2 heterodimer alpha(0)beta(0) occurred in 97.1% of CD patients (31.4% in double dose, 65.7% in single dose) and revealed significant deviation from healthy controls (chi(2) = 102.08, p = 7.56E-11). Further analysis revealed involvement of multiple DR3+ve haplotypes with CD in Indians, of which A26-B8-DR3 was the most common DR3 haplotype among patients (34.28%, chi(2) = 40.57, p = 2.65E-10) followed by Ax-B21-DR3 (11.4%) (chi(2) = 13.8, p = 2E-04) and the classical Caucasian haplotype A1-B8-DR3 (5.7%). The former two haplotypes are characteristic of Asian Indians and are involved in the development of CD. We conclude that the high risk DR3 haplotypes that play a crucial role in the development of CD are unique in Asian Indians. Detailed analysis of these haplotypes in Indian patients with autoimmune diseases may help understand the influence of other intervening genes within the major histocompatibility complex.
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- 2002
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181. Effect of vitamin A administered at Expanded Program on Immunization contacts on antibody response to oral polio vaccine.
- Author
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Bahl R, Bhandari N, Kant S, Mølbak K, Østergaard E, and Bhan MK
- Subjects
- Adult, Dietary Supplements, Double-Blind Method, Female, Humans, India, Infant, Male, Poliovirus Vaccine, Oral blood, Postpartum Period physiology, Poverty Areas, Urban Population, Vitamin A Deficiency prevention & control, Antibody Formation drug effects, Poliovirus Vaccine, Oral immunology, Vitamin A administration & dosage, Vitamin A pharmacology
- Abstract
Objective: Vitamin A supplementation to mothers in the postpartum period and to their infants at routine immunization contacts is being considered to reduce vitamin A deficiency in infancy. This study was conducted to determine the impact of maternal and infant vitamin A supplementation on antibody response to oral polio vaccine (OPV)., Design: Randomized, double blind, placebo-controlled trial., Interventions: Mothers in the intervention group received 60 mg retinol equivalent (RE) vitamin A 3-4 weeks after delivery and their infants 7.5 mg RE with each OPV dose at 6, 10 and 14 weeks of age. The control group mothers and their infants received a placebo at each of these contacts., Main Outcomes: Geometric mean (GM) titer of neutralizing antibodies and proportion of children with protective titer to the three polioviruses at 26 weeks of age., Results: Vitamin A supplementation increased the proportion of infants with protective antibody titer against poliovirus type 1 (relative risk (RR) 1.15, 95% confidence interval (CI) 1.03-1.28) and the GM antibody titer (ratio of GM 1.55, 95% CI 1.03-2.31) following immunization. The proportion of infants with protective antibody titer against poliovirus type 2 (RR 0.99, 95% CI 0.94-1.05) or type 3 (RR 1.05, 95% CI 0.96-1.15) was not significantly different in vitamin A and placebo groups. The GM antibody titer for poliovirus type 2 (ratio of GM 0.99, 95% CI 0.64-1.54) or poliovirus type 3 (ratio of GM 1.10, 95% CI 0.69-1.75) also did not differ across groups., Conclusions: Vitamin A given to the mothers in the postpartum period and their infants with OPV did not interfere with the antibody response to any of the three polioviruses and enhanced the response to poliovirus type 1.
- Published
- 2002
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182. Great diversity of group A rotavirus strains and high prevalence of mixed rotavirus infections in India.
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Jain V, Das BK, Bhan MK, Glass RI, and Gentsch JR
- Subjects
- Child, Child, Preschool, Electrophoresis, Polyacrylamide Gel methods, Genotype, Humans, India epidemiology, Prevalence, Reverse Transcriptase Polymerase Chain Reaction, Rotavirus Infections virology, Serotyping, Genetic Variation, Rotavirus classification, Rotavirus genetics, Rotavirus Infections epidemiology
- Abstract
We previously observed a marked diversity of rotavirus strains and a high prevalence of the uncommon serotype G9 in a small survey of rotavirus strains collected from six centers in India. In the present study, we characterized a larger collection of strains from children hospitalized with severe diarrhea in seven Indian cities between 1996 and 1998. A total of 287 strains were G and P genotyped by reverse transcription-PCR, and some were further characterized by electropherotyping and subgrouping. Of the four strains common globally, three were found in only 43% of samples (P[8], G1, 15%; P[4], G2, 22%; P[8], G4, 6%), whereas G9 strains made up 17% of the total. Three different G9 strains were present: a P[8], G9 strain, which displayed the long electropherotype and subgroup II VP6 specificity, and two P[6], G9 strains, one with the long electropherotype and subgroup II specificity and the other with the short electropherotype and subgroup I specificity. Marked diversity was observed among strains collected from different cities and collected over time. Of the 253 strains that were fully typed, 54 (21%) had a mixed G or P genotype. Serotype G2 strains were detected more often in infections caused by single strains than in mixed infections (P < 0.05), whereas serotype G1 strains were found more often in mixed infections than in infections caused by single strains (P < 0.05). The diversity of rotavirus strains and the high prevalence of mixed infections confirm trends reported earlier and help to better characterize the strains of rotavirus circulating in India. Vaccines under development should clearly target G9 strains, and G9 should be included as one of the common global serotypes.
- Published
- 2001
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183. Pneumococcal pulmonary infection, septicaemia and survival in young zinc-depleted mice.
- Author
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Strand TA, Briles DE, Gjessing HK, Maage A, Bhan MK, and Sommerfelt H
- Subjects
- Animals, Bacteremia metabolism, Body Weight, Disease Susceptibility, Female, Femur chemistry, Mice, Mice, Inbred BALB C, Micronutrients administration & dosage, Micronutrients analysis, Pneumonia, Pneumococcal metabolism, Pneumonia, Pneumococcal mortality, Proportional Hazards Models, Zinc administration & dosage, Zinc analysis, Bacteremia etiology, Micronutrients deficiency, Pneumonia, Pneumococcal etiology, Zinc deficiency
- Abstract
The aim of the present study was to explore whether mice fed a diet low in Zn (2.0 mg Zn/kg diet) for a relatively short period of time were more prone to severe Streptococcus pneumoniae infection than mice fed a normal diet (25 mg elemental Zn/kg). The Zn-deficient mice were compared with mice in two Zn-adequate control groups; one pair-fed and another with free access to the diet. After 2 weeks feeding, the mice were infected intranasally under anaesthesia with a suspension containing about 10(7) pneumococci. Clinical status was observed every day and blood samples were examined for S. pneumoniae every second day for a week. All infected mice examined carried the infecting strain intranasally. The survival time and time before positive blood culture were significantly shorter in the Zn-depleted group than in the pair-fed Zn-adequate group (hazard ratios 15.6 and 3.2, and respectively). At the end of the observation period, ten of the twelve mice in the Zn-deficient group were dead while one of twelve and two of twelve were dead in the two Zn-adequate control groups. This study shows that even acutely-induced Zn deficiency dramatically increases the risk of serious pneumococcal infection in mice.
- Published
- 2001
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184. Food supplementation with encouragement to feed it to infants from 4 to 12 months of age has a small impact on weight gain.
- Author
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Bhandari N, Bahl R, Nayyar B, Khokhar P, Rohde JE, and Bhan MK
- Subjects
- Body Height, Breast Feeding, Dysentery epidemiology, Edible Grain, Energy Intake, Female, Fever epidemiology, Food Supply, Humans, India, Infant, Infant Nutrition Disorders mortality, Infant Nutritional Physiological Phenomena, Male, Morbidity, Socioeconomic Factors, Weaning, Dietary Supplements, Growth physiology, Infant Food, Infant Nutrition Disorders prevention & control, Nutritional Sciences education, Weight Gain
- Abstract
It is unclear whether a substantial decline in malnutrition among infants in developing countries can be achieved by increasing food availability and nutrition counseling without concurrent morbidity-reducing interventions. The study was designed to determine whether provision of generous amounts of a micronutrient-fortified food supplement supported by counseling or nutritional counseling alone would significantly improve physical growth between 4 and 12 mo of age. In a controlled trial, 418 infants 4 mo of age were individually randomized to one of the four groups and followed until 12 mo of age. The first group received a milk-based cereal and nutritional counseling; the second group monthly nutritional counseling alone. To control for the effect of twice-weekly home visits for morbidity ascertainment, similar visits were made in one of the control groups (visitation group); the fourth group received no intervention. The median energy intake from nonbreast milk sources was higher in the food supplementation group than in the visitation group by 1212 kJ at 26 wk (P < 0.001), 1739 kJ at 38 wk (P < 0.001) and 2257 kJ at 52 wk (P < 0.001). The food supplementation infants gained 250 g (95% confidence interval: 20--480 g) more weight than did the visitation group. The difference in the mean increment in length during the study was 0.4 cm (95% confidence interval: -0.1--0.9 cm). The nutritional counseling group had higher energy intakes ranging from 280 to 752 kJ at different ages (P < 0.05 at all ages) but no significant benefit on weight and length increments. Methods to enhance the impact of these interventions need to be identified.
- Published
- 2001
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185. Community-based controlled trial of dietary management of children with persistent diarrhea: sustained beneficial effect on ponderal and linear growth.
- Author
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Valentiner-Branth P, Steinsland H, Santos G, Perch M, Begtrup K, Bhan MK, Dias F, Aaby P, Sommerfelt H, and Mølbak K
- Subjects
- Administration, Oral, Body Height, Body Weight, Child, Preschool, Diarrhea physiopathology, Feces microbiology, Feces parasitology, Female, Guinea-Bissau, Humans, Infant, Male, Reference Values, Time Factors, Urban Population, Diarrhea diet therapy, Growth physiology, Micronutrients administration & dosage, Vitamins administration & dosage
- Abstract
Background: Uncontrolled hospital-based studies in developing countries have reported promising results of dietary rehabilitation of children with persistent diarrhea., Objective: The objective was to determine the immediate and long-term effects of a dietary supplement and micronutrients given to children with persistent diarrhea during the episode and for 1 wk during convalescence., Design: The study was open, controlled, and community-based and was conducted in a periurban area in Guinea-BISSAU: Children <3 y of age with persistent diarrhea were identified during weekly household visits. The children randomly assigned to the treatment and control groups were examined by a physician and all medical conditions were treated. The children in the treatment group were offered home-based dietary treatment consisting of locally available foods and micronutrient supplements., Results: There were 141 episodes of persistent diarrhea during the study: 70 in the treatment group (in 58 children) and 71 in the control group (in 62 children). During the intervention period (median: 17 d), weight gain in the treatment group exceeded that of the control group by 61.5 g/wk (95% CI: 49.2, 73.8), whereas there was no significant difference in linear growth on the basis of knee-heel length. At a median follow-up period of 6.6 mo after the intervention was stopped, weight gain in the treatment group exceeded that of the control group by 12.5 g/wk (95% CI: 7.7, 17.3); knee-heel length was 7.5 mm/y (4.8, 10.2) greater and total length was 0.65 cm/y (0.11, 1.19) greater in the treatment group., Conclusion: Therapeutic feeding and micronutrient supplementation had an immediate and sustained beneficial effect on growth in children with persistent diarrhea.
- Published
- 2001
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186. Micronutrient deficiency in children.
- Author
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Bhan MK, Sommerfelt H, and Strand T
- Subjects
- Breeding, Child, Child, Preschool, Female, Humans, Infant, Plants, Edible, Pregnancy, Pregnancy Complications prevention & control, Developing Countries, Food, Fortified, Health Policy, Micronutrients deficiency
- Abstract
Malnutrition increases morbidity and mortality and affects physical growth and development, some of these effects resulting from specific micronutrient deficiencies. While public health efforts must be targeted to improve dietary intakes in children through breast feeding and appropriate complementary feeding, there is a need for additional measures to increase the intake of certain micronutrients. Food-based approaches are regarded as the long-term strategy for improving nutrition, but for certain micronutrients, supplementation, be it to the general population or to high risk groups or as an adjunct to treatment must also be considered. Our understanding of the prevalence and consequences of iron, vitamin A and iodine deficiency in children and pregnant women has advanced considerably while there is still a need to generate more knowledge pertaining to many other micronutrients, including zinc, selenium and many of the B-vitamins. For iron and vitamin A, the challenge is to improve the delivery to target populations. For disease prevention and growth promotion, the need to deliver safe but effective amounts of micronutrients such as zinc to children and women of fertile age can be determined only after data on deficiency prevalence becomes available and the studies on mortality reduction following supplementation are completed. Individual or multiple micronutrients must be used as an adjunct to treatment of common infectious diseases and malnutrition only if the gains are substantial and the safety window sufficiently wide. The available data for zinc are promising with regard to the prevention of diarrhea and pneumonia. It should be emphasized that there must be no displacement of important treatment such as ORS in acute diarrhea by adjunct therapy such as zinc. Credible policy making requires description of not only the clinical effects but also the underlying biological mechanisms. As findings of experimental studies are not always feasible to extrapolate to humans, the biology of deficiency as well as excess of micronutrients in humans must continue to be investigated with vigour.
- Published
- 2001
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187. Micronutrients as adjunct therapy of acute illness in children: impact on the episode outcome and policy implications of current findings.
- Author
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Mahalanabis D and Bhan MK
- Subjects
- Acute Disease, Chemotherapy, Adjuvant, Child, Preschool, Folic Acid administration & dosage, Humans, Infant, Kwashiorkor drug therapy, Measles mortality, Pneumonia drug therapy, Vitamin A administration & dosage, Zinc administration & dosage, Developing Countries, Diarrhea drug therapy, Health Policy, Measles drug therapy, Micronutrients therapeutic use
- Abstract
Role of micronutrients namely vitamin A, zinc and folate, as adjunct therapy of illness episodes in children in developing countries have been discussed in the light of health policy. Apart from a selective review, attempts have been made to statistically combine results of several studies to address policy issues. In children, vitamin A supplementation during illness has (a) a profound effect in reducing mortality in measles, (b) possibly a significant effect in reducing persistent diarrhea episodes in children with acute diarrhea, and (c) no benefit in pneumonia. Use of large dose vitamin A is recommended during measles episodes but not in non-measles pneumonia. Its use in acute diarrhea is debatable but recommended in persistent diarrhea and in severe malnutrition as a component of a micronutrient mixture. Large dose vitamin A supplementation should be used with caution in young infants as there are unresolved concerns about its safety particularly, bulging fontanelle observed in infants when co-administered at immunization. In children, zinc supplementation during illness, (a) had a marked effect in reducing prolonged episodes and a modest effect on episode duration in acute diarrhea, (b) resulted in reduced rate of treatment failure and death in persistent diarrhea, (c) had no effect in measles and non-measles pneumonia, and (d) probably had a detrimental effect of increasing death rate when a large dose was used in severely malnourished children. The desirability of routine zinc supplementation therapy of undernourished children with acute diarrhea should be assessed further. Concerning policy, zinc supplementation as a component of a micronutrient mixture is recommended in the rehabilitation of severely malnourished children and in persistent diarrhea. However, recommendation for its routine use in all cases of acute diarrhea in children needs additional studies on effectiveness, cost, operations and safety. In two randomized controlled trials folate has been evaluated in acute and persistent diarrhea and found to have no beneficial effect. Folate is not recommended as adjunct therapy of diarrhea. Role of folate in preventing severe disease and/or death deserves further evaluation.
- Published
- 2001
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188. Molecular characterization of serotype G9 rotavirus strains from a global collection.
- Author
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Ramachandran M, Kirkwood CD, Unicomb L, Cunliffe NA, Ward RL, Bhan MK, Clark HF, Glass RI, and Gentsch JR
- Subjects
- Base Sequence, Genes, Viral, Genetic Variation, Genotype, Geography, Humans, Molecular Sequence Data, Rotavirus isolation & purification, Serotyping, Viral Structural Proteins genetics, Antigens, Viral, Capsid genetics, Capsid Proteins, Phylogeny, Rotavirus classification, Rotavirus genetics
- Abstract
Between 1992 and 1998, serotype G9 human rotavirus (RV) strains have been detected in 10 countries, including Thailand, India, Brazil, Bangladesh, Malawi, Italy, France, the United States, the United Kingdom, and Australia, suggesting the possible emergence of the fifth common serotype worldwide. Unlike the previously characterized reference G9 strains (i.e., WI61 and F45), the recent G9 isolates had a variety of gene combinations, raising questions concerning their origin and evolution. To identify the progenitor strain and examine the on-going evolution of the recent G9 strains, we characterized by genetic and antigenic analyses 16 isolates obtained from children with diarrhea in India, Bangladesh, the United States, and Malawi. Specifically, we sequenced their VP7 and NSP4 genes and compared the nucleotide (nt) and deduced amino acid sequences with the reference G9 strains. To identify reassortment, we examined the products of five gene segments; VP4, VP7, and NSP4 genotypes (genes 4, 9, and 10); subgroups (gene 6); electropherotypes (gene 11); and the genogroup profiles of all of the recent G9 isolates. Sequence analysis of the VP7 gene indicated that the recent U.S. P[6],G9 strains were closely related to the Malawian G9 strains (>99% nt identity) but distinct from G9 strains of India ( approximately 97% nt identity), Bangladesh ( approximately 98% nt identity), and the reference strains ( approximately 97% nt identity). Phylogenetic analysis identified a single cluster for the U.S. P[6],G9 strains that may have common progenitors with Malawian P[6],G9 strains whereas separate lineages were defined for the Indian, Bangladeshi, and reference G9 strains. Northern hybridization results indicated that all 11 gene segments of the Malawian P[6],G9 strains hybridized with a probe derived from a U.S. strain of the same genotype and may have the same progenitor, different from the Indian G9 strains, whereas the Bangladesh strains may have evolved from the U.S. G9 progenitors. Overall, our findings suggest that much greater diversity among the newly identified G9 strains has been generated by reassortment between gene segments than through the accumulation of mutations in a single gene., (Copyright 2000 Academic Press.)
- Published
- 2000
- Full Text
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189. Community-based randomized controlled trial of reduced osmolarity oral rehydration solution in acute childhood diarrhea.
- Author
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Valentiner-Branth P, Steinsland H, Gjessing HK, Santos G, Bhan MK, Dias F, Aaby P, Sommerfelt H, and Mølbak K
- Subjects
- Acute Disease, Administration, Oral, Child, Preschool, Diarrhea, Infantile microbiology, Double-Blind Method, Feces microbiology, Guinea-Bissau, Home Care Services, Humans, Infant, Infant, Newborn, Osmolar Concentration, Treatment Outcome, Diarrhea, Infantile therapy, Fluid Therapy methods, Rehydration Solutions therapeutic use
- Abstract
Objective: The standard oral rehydration solution (ORS) recommended by WHO and UNICEF does not reduce the volume or frequency of stools or the length of the episode. Hospital-based studies from developing and developed countries and intestinal perfusion studies suggest a beneficial effect on water and sodium absorption with reduced osmolarity ORS as compared with standard ORS. We conducted a community-based study comparing the efficacy of reduced osmolarity ORS (224 mmol/l) with standard ORS (311 mmol/l) in acute childhood diarrhea in a West African community., Methods: Infants and toddlers age 0 to 30 months having 738 episodes of diarrhea identified by weekly household visits were randomly assigned to treatment with either standard ORS (n = 376) or reduced osmolarity ORS (n = 362). The children were followed by daily home visits to assess ORS intake and clinical characteristics. Duration of diarrhea was compared by proportional hazards regression analysis, the hazard ratio being interpreted as the relative recovery rate between the children receiving the two types of ORS. Because earlier reports have suggested that weaning status might be an important modifier for the performance of reduced osmolarity ORS, the effect was assessed overall and as an interaction between type of ORS and weaning status and age. Maternal satisfaction was assessed in a paired analysis among mothers whose children participated at least twice in the study., Results: In the overall analysis reduced osmolarity ORS was as efficacious as standard ORS as assessed by duration of diarrheal episode and total number of stool evacuations on Days 1 and 2. Non-breast-fed toddlers (i.e. children ages 12 to 30 months) treated with reduced osmolarity ORS had significantly shorter diarrheal episodes [1.14 days vs. 1.78 days with standard ORS; hazard ratio, 1.50; 95% confidence interval (CI), 1.07 to 2.09] and lower total number of stool evacuations on Days 1 and 2 (3.9 stool evacuations vs. 5.0 stool evacuations with standard ORS; ratio of geometric means, 0.77; 95% CI 0.60 to 1.01). No significant difference was found for breast-fed toddlers or for infants. There was no statistically significant difference in the ORS intake between the two treatment groups. The odds ratio for the mother preferring reduced osmolarity ORS to standard ORS was 1.92 (95% CI 0.97 to 3.85)., Conclusions: Reduced osmolarity ORS was as efficacious as standard ORS. Non-breast-fed children treated with reduced osmolarity ORS had significantly shorter diarrheal episodes and a tendency toward lower stool frequency. These findings may be of importance, especially in developing countries where early weaning is common.
- Published
- 1999
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190. Typhoid fever in children aged less than 5 years.
- Author
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Sinha A, Sazawal S, Kumar R, Sood S, Reddaiah VP, Singh B, Rao M, Naficy A, Clemens JD, and Bhan MK
- Subjects
- Adolescent, Adult, Age Factors, Child, Child, Preschool, Cross-Sectional Studies, Female, Follow-Up Studies, Humans, Immunization Programs, Incidence, India epidemiology, Infant, Male, Population Surveillance, Poverty statistics & numerical data, Prospective Studies, Typhoid Fever prevention & control, Typhoid-Paratyphoid Vaccines administration & dosage, Developing Countries, Typhoid Fever epidemiology, Urban Population statistics & numerical data
- Abstract
Background: Calculation of the incidence of typhoid fever during preschool years is important to define the optimum age of immunisation and the choice of vaccines for public-health programmes in developing countries. Hospital-based studies have suggested that children younger than 5 years do not need vaccination against typhoid fever, but this view needs to be re-examined in community-based longitudinal studies. We undertook a prospective follow-up study of residents of a low-income urban area of Delhi, India, with active surveillance for case detection., Methods: A baseline census was undertaken in 1995. Between Nov 1, 1995, and Oct 31, 1996, we visited 8172 residents of 1820 households in Kalkaji, Delhi, twice weekly to detect febrile cases. Blood samples were obtained from febrile patients, and those who tested positive for Salmonella typhi were treated with ciprofloxacin., Findings: 63 culture-positive typhoid fever cases were detected. Of these, 28 (44%) were in children aged under 5 years. The incidence rate of typhoid per 1000 person-years was 27.3 at age under 5 years, 11.7 at 5-19 years, and 1.1 between 19 and 40 years. The difference in the incidence of typhoid fever between those under 5 years and those aged 5-19 years (15.6 per 1000 person-years [95% CI 4.7-26.5]), and those aged 19-40 years (26.2 [16.0-36.3]) was significant (p<0.001 for both). The difference between the incidence of typhoid at 5-19 years and the incidence at 19-40 years was also significant (10.6 [6.3-14.8], p<0.001). Morbidity in those under 5 and in older people was similar in terms of duration of fever, signs and symptoms, and need for hospital admission., Interpretation: Our findings challenge the common view that typhoid fever is a disorder of school-age children and of adults. Typhoid is a common and significant cause of morbidity between 1 and 5 years of age. The optimum age of typhoid immunisation and the choice of vaccines needs to be reassessed.
- Published
- 1999
- Full Text
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191. Chlamydia trachomatis infection among pregnant women: prevalence and prenatal importance.
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Paul VK, Singh M, Gupta U, Buckshee K, Bhargava VL, Takkar D, Nag VL, Bhan MK, and Deorari AK
- Subjects
- Adult, Chlamydia Infections diagnosis, Female, Humans, India epidemiology, Infant, Newborn, Pregnancy, Pregnancy Complications, Infectious diagnosis, Pregnancy Outcome, Prevalence, Chlamydia Infections epidemiology, Chlamydia trachomatis, Pregnancy Complications, Infectious epidemiology
- Abstract
Background: Chlamydia trachomatis infection in pregnant women is suspected to result in low birth-weight and premature infants. We conducted studies to ascertain the prevalence of this infection among pregnant women in our setting and whether its presence is a risk factor for low birth-weight or prematurity., Methods: In the first study, 94 pregnant women between 26 and 30 weeks of gestation were screened for infection with Chlamydia trachomatis. The second investigated a cohort of 172 pregnant women presenting in spontaneous labour. The infection status was related to perinatal outcome in terms of birth-weight and gestation. In both the studies, Chlamydia trachomatis infection was diagnosed using the Chlamydiazyme test performed on endocervical swabs., Results: The prevalence of Chlamydia trachomatis infection in mid-pregnancy and at labour was 17% (16/94) and 18.6% (32/172), respectively. Women with infection were relatively older than those without it [mean (SD) age: 26.6 (4.5) years v. 24.8 (3.6) years, p = 0.01]. The mean (SD) birth-weight [2869 (611) g v. 2814 (496) g], gestation [38.5 (2.6) weeks v. 38.3 (2.0) weeks], and incidence of low birth-weight [18.7% v. 20.7%] as well as prematurity [9.4% v. 10.7%] were similar among neonates born to women with or without infection. Neonates born to infected mothers experienced purulent conjunctivitis more frequently than those born to non-infected mothers [12.5% v. 2.8%, p = 0.04]., Conclusion: Chlamydia trachomatis is a relatively common infection in pregnant women. However, it was not associated with either low birth-weight or prematurity.
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- 1999
192. Histologic chorioamnionitis & its association with prematurity in a hospital-based study.
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Paul VK, Dawar R, Gupta SD, Singh M, Buckshee K, Gupta U, Bhan MK, Bhargava VL, Takkar D, and Deorari AK
- Subjects
- Female, Hospitals, Teaching, Humans, Infant, Newborn, Pregnancy, Prospective Studies, Risk Factors, Chorioamnionitis microbiology, Infant, Premature, Diseases microbiology
- Abstract
This prospective study was undertaken to study the occurrence of histologic chorioamnionitis and determine its association with prematurity; and to assess whether colonization of the genital tract of pregnant women by genital mycoplasmas or Chlamydia trachomatis is a risk factor for histologic chorioamnionitis. A total of 268 women with singleton pregnancies of over 26 weeks gestation were subjected to high vaginal cultures of genital mycoplasmas and endocervical specimens for chlamydia antigen. Placental histopathology was performed on multiple sections. Histologic chorioamnionitis was documented in 22.4 per cent (60/208) placentae. Genital tract colonization with Ureaplasma urealyticum or C. trachomatis was not a risk factor for histologic chorioamnionitis. Neonates born in association with histologic chorioamnionitis had a mean birth weight 111 g lower than those born without this lesion (2626.9 +/- 702 g vs 2737.8 +/- 500 g, NS). The relative risk (95% confidence interval) of prematurity in the presence of histologic chorioamnionitis was 1.49 (0.87-2.53). Analysis of linear trend in proportions for prevalence of histologic chorioamnionitis with decreasing gestation showed a significant association (P = 0.047, 1-tail). These results taken together suggest that histologic chorioamnionitis may be a risk factor of prematurity, but of only a modest magnitude.
- Published
- 1998
193. Careseeking for illness in young infants in an urban slum in India.
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de Zoysa I, Bhandari N, Akhtari N, and Bhan MK
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- Adolescent, Female, Humans, India, Infant, Infant, Newborn, Medicine, Traditional, Middle Aged, Mothers psychology, Practice Patterns, Physicians', Quality of Health Care, Child Health Services statistics & numerical data, Culture, Poverty
- Abstract
Illness in infants in the first two months of life can take a precipitous life-threatening course, and requires timely and appropriate medical assessment and management. We conducted a focused ethnographic study of illness in young infants and associated careseeking practices in an urban slum in New Delhi, India, in order to identify the constraints in securing effective care for severe illness in this age group. The findings suggest that maternal recognition of illness is not a limiting factor in the use of health care services for sick young infants in this setting. Mothers respond to a number of important signs of illness, including changes in the young infant's sleeping or feeding behavior, and they are usually prompt in seeking care outside the home. They are not able, however, to discriminate among the many sources of health care available in this setting, and give preference to local unqualified private practitioners. Most practitioners, including qualified medical practitioners, display critical failures in the assessment and management of sick young infants. The continuity and effectiveness of care is further compromised by the caretakers' expectations of rapid cure, which result in discontinued treatment courses and frequent changes in practitioners, and by their reluctance to seek hospital care. The implications of these findings for the design of programs to reduce young infant mortality are discussed. In particular, the feasibility and acceptability of hospital referrals according to current program guidelines are called into question.
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- 1998
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194. Association of genital mycoplasma colonization with low birth weight.
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Paul VK, Gupta U, Singh M, Nag VL, Takkar D, and Bhan MK
- Subjects
- Adult, Birth Weight, Cohort Studies, Female, Gestational Age, Humans, India epidemiology, Infant, Newborn, Infant, Premature, Infant, Small for Gestational Age, Mycoplasma Infections complications, Pregnancy, Prevalence, Ureaplasma Infections complications, Vagina microbiology, Infant, Low Birth Weight, Mycoplasma Infections epidemiology, Mycoplasma hominis isolation & purification, Obstetric Labor, Premature epidemiology, Pregnancy Complications, Infectious epidemiology, Ureaplasma Infections epidemiology, Ureaplasma urealyticum isolation & purification
- Abstract
Objective: This study was conducted to document the prevalence of maternal genital tract colonization by Ureaplasma urealyticum and Mycoplasma hominis, and to assess its association with low birth weight (LBW) and prematurity., Methods: The high vaginal swabs of pregnant women in spontaneous labor after 26 weeks of gestation were cultured for U. urealyticum and M. hominis. Clinical details and perinatal outcomes including birth weight and gestation were documented., Results: Of a total of 303 women enrolled, 148 (48.8%) had positive vaginal cultures for U. urealyticum, while only five (1.6%) grew M. hominis. The mean birth weight and the incidences of LBW and preterm neonates among ureaplasma positive and ureaplasma negative mothers were statistically comparable., Conclusions: U. urealyticum emerged as a common inhabitant of the lower genital tract of women in labor, being present in nearly half of them. Its presence was not a risk factor of LBW or prematurity. Maternal colonization with M. hominis was uncommon.
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- 1998
- Full Text
- View/download PDF
195. Lack of maternal antibodies to P serotypes may predispose neonates to infections with unusual rotavirus strains.
- Author
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Ramachandran M, Vij A, Kumar R, Das BK, Gentsch JR, Bhan MK, and Glass RI
- Subjects
- Antibodies, Viral blood, Case-Control Studies, Female, Fetal Blood immunology, Humans, Immunity, Maternally-Acquired, Immunoglobulin A blood, Immunoglobulin A metabolism, Infant, Newborn, Neutralization Tests, Polymerase Chain Reaction, Pregnancy, RNA, Viral isolation & purification, Rotavirus genetics, Rotavirus Infections prevention & control, Saliva immunology, Serotyping, Viral Vaccines pharmacology, Antibodies, Viral metabolism, Rotavirus classification, Rotavirus immunology, Rotavirus Infections etiology, Rotavirus Infections immunology
- Abstract
Rotavirus (RV) strains infecting newborns often have unique neutralization antigens (P serotypes) on their outer capsids that are distinct from those found on RV strains that cause diarrhea in older children. We examined the hypothesis that unusual RV strains preferentially infect newborns because the newborns lack maternal neutralizing antibodies to these strains. To test this hypothesis, sera and saliva samples collected from neonates infected with 116E-like (P[11]G9) strains in the maternity ward of the All India Institute of Medical Sciences (AIIMS) hospital in New Delhi were tested for neutralizing antibodies against common RV strains and those infecting newborns and these titers were compared with those of newborns who did not become infected (controls). The infected neonates had significantly lower levels of cord blood neutralizing antibodies to 116E than the controls, suggesting that immunity to neonatal RV infection is acquired transplacentally through maternal antibodies. Further, this study confirmed the immunogenicity of the AIIMS neonatal strain 116E, a vaccine candidate, in its ability to evoke a potent RV-specific immunoglobulin A and neutralizing antibody response in serum and saliva among the infected babies. Our findings have important implications for the development of an effective RV vaccine. In India, where G9 strains are common in the community, the use of 116E as a vaccine, together with the rhesus tetravalent vaccine, may provide a broader protection against all the circulating RV serotypes, including serotype G9, which is not represented in the current rhesus RV tetravalent vaccine (G1-G4).
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- 1998
- Full Text
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196. Zinc supplementation reduces the incidence of acute lower respiratory infections in infants and preschool children: a double-blind, controlled trial.
- Author
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Sazawal S, Black RE, Jalla S, Mazumdar S, Sinha A, and Bhan MK
- Subjects
- Child, Preschool, Double-Blind Method, Female, Humans, Immunocompetence drug effects, India, Infant, Male, Protein-Energy Malnutrition complications, Protein-Energy Malnutrition immunology, Regression Analysis, Respiratory Tract Infections immunology, Risk Factors, Treatment Outcome, Urban Population, Zinc blood, Zinc deficiency, Gluconates administration & dosage, Respiratory Tract Infections prevention & control
- Abstract
Background: Increased acute lower respiratory infection incidence, severity, and mortality are associated with malnutrition, and reduced immunological competence may be a mechanism for this association. Because zinc deficiency results in impaired immunocompetence and zinc supplementation improves immune status, we hypothesized that zinc deficiency is associated with increased incidence and severity of acute lower respiratory infection., Methods: We evaluated the effect of daily supplementation with 10 mg of elemental zinc on the incidence and prevalence of acute lower respiratory infection in a double-blind, randomized, controlled trial in 609 children (zinc, n = 298; control, n = 311) 6 to 35 months of age. Supplementation and morbidity surveillance were done for 6 months., Results: After 120 days of supplementation, the percentage of children with plasma zinc concentrations <60 microg/dL decreased from 35.6% to 11.6% in the zinc group, whereas in the control group it increased from 36.8% to 43.6%. Zinc-supplemented children had 0.19 acute lower respiratory infection episodes/child/year compared with 0.35 episodes/child/year in the control children. After correction for correlation of data using generalized estimating equation regression methods, there was a reduction of 45% (95% confidence interval, 10% to 67%) in the incidence of acute lower respiratory infections in zinc-supplemented children., Conclusions: A dietary zinc supplement resulted in a significant reduction in respiratory morbidity in preschool children. These findings suggest that interventions to improve zinc intake will improve the health and survival of children in developing countries.
- Published
- 1998
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197. Efficacy of milk versus yogurt offered as part of a mixed diet in acute noncholera diarrhea among malnourished children.
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Bhatnagar S, Singh KD, Sazawal S, Saxena SK, and Bhan MK
- Subjects
- Acute Disease, Animals, Child, Preschool, Diarrhea, Infantile diet therapy, Humans, Infant, Infant Nutrition Disorders diet therapy, Male, Rehydration Solutions administration & dosage, Treatment Outcome, Weight Gain, Child Nutrition Disorders diet therapy, Diarrhea diet therapy, Milk, Yogurt
- Abstract
We compared the clinical outcome of acute diarrhea in 96 malnourished boys (aged 4 to 47 months) receiving full-strength milk compared with yogurt offered as part of a mixed diet. All had weight for height less than or equal to 80% of the National Centre for Health Statistics median. They were randomly assigned to receive milk formula (MF; 67 cal/100 ml) or yogurt formula (YF; prepared from the same milk formula) at the rate of 120 ml/kg body weight in seven divided feedings. Stool-reducing substances (> 1%) were detected more frequently in the MF group, and the differences were significant for day 3 of the study (p = 0.04). However, the geometric mean (95% confidence interval) of the total stool weights (gm/kg) during 0 to 72 hours (MF 128.8 [103, 161.4]; YF 110.9 [87, 142.2]) was comparable (p = 0.37) as was the median (range) duration of diarrhea (hours) (MF 45 [4, 183]; YF 52 [7, 173] p = 0.94). The treatment failure rates in the MF (8.2%) and YF (6.3%) groups were also similar (p = 0.67). The children consuming milk had higher median percent weight gain at the end of 72 hours of the study (p = 0.04) and at recovery (p = 0.02). Routine substitution of yogurt as small frequent feedings as an addition for semisolid food to malnourished children with acute diarrhea does not achieve any significant clinical benefit versus milk.
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- 1998
- Full Text
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198. Country profile: India.
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Nath I, Reddy KS, Dinshaw KA, Bhisey AN, Krishnaswami K, Bhan MK, Ganguly NK, Kaur S, Panda SK, Jameel S, Srinivasan K, Thankappan KR, and Valiathan MS
- Subjects
- Education, Medical, Humans, India epidemiology, Research, Health Services, Morbidity
- Published
- 1998
- Full Text
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199. Cholestatic jaundice due to congenital Toxoplasma gondii infection.
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Singh S, Lodha R, Passi GR, and Bhan MK
- Subjects
- Cholestasis, Intrahepatic drug therapy, Diagnosis, Differential, Drug Therapy, Combination, Humans, Infant, Male, Pyrimethamine therapeutic use, Sulfadiazine therapeutic use, Toxoplasmosis, Congenital drug therapy, Cholestasis, Intrahepatic diagnosis, Toxoplasmosis, Congenital diagnosis
- Abstract
A case of congenital toxoplasmosis manifesting as hepatosplenomegaly and cholestatic jaundice in a 4 month old child is reported. To the best of our knowledge this is the first report of cholestatic jaundice due to congenital toxoplasmosis from India. The child was successfully treated with sulphadiazine and pyremethamine combination.
- Published
- 1998
- Full Text
- View/download PDF
200. Sequence analysis of NSP4 gene of human rotavirus allows classification into two main genetic groups.
- Author
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Cunliffe NA, Woods PA, Leite JP, Das BK, Ramachandran M, Bhan MK, Hart CA, Glass RI, and Gentsch JR
- Subjects
- Amino Acid Sequence, Animals, Base Sequence, DNA Primers genetics, Diarrhea virology, Genetic Variation, Humans, Infant, Newborn, Molecular Sequence Data, Phylogeny, Polymerase Chain Reaction, Rotavirus isolation & purification, Rotavirus Infections virology, Sequence Homology, Amino Acid, Toxins, Biological, Genes, Viral, Glycoproteins genetics, Rotavirus classification, Rotavirus genetics, Viral Nonstructural Proteins genetics
- Abstract
The rotavirus nonstructural glycoprotein NSP4 may represent the first identified viral enterotoxin. We have sequenced reverse transcription-polymerase chain reaction (RT-PCR)-generated fragments of 16 NSP4 genes of human rotavirus (HRV) strains from six different countries, representing seven different G and P type combinations. Based on the amount of sequence divergence between these and 11 previously sequenced NSP4 genes of human and animal rotaviruses, three distinct genetic groups could be recognized. Most strains within a group were closely related to each other at the nucleotide (nt) and amino acid (aa) levels (usually <10% divergence) but more distantly related (maximum 30.0% nt divergence and 24.7% aa divergence) to members of the other groups. Intergroup variation occurred in two highly variable regions of NSP4 (aa 16-34 and aa 131-148). The NSP4 "toxic peptide" (aa 114-135) exhibited aa variation at its carboxy terminus both within and between genetic groups. The largest group (genetic group II) contained HRV strains of subgroup II specificity (including genotypes P[8]G1, P[8]G3, P[6]G3, and P[8]G5 and serotype P8[11]G9), and the smaller group (genetic group I) contained HRV strains of subgroup I specificity (genotype P[4]G2). The NSP4 sequence of the rhesus rotavirus vaccine strain was distinct from all other strains and formed the third group (genetic group III). The NSP4 genes of animal rotaviruses UK, NCDV, and SA11 (genetic group I) and YM (genetic group II) and two possible human-animal rotavirus reassortant strains, Brazilian P[8]G5 and Indian P[11]G9 (genetic group II), could also be classified into one of these groups, suggesting a close evolutionary relationship between human and animal NSP4 genes. These results will facilitate studies of the host immune response to NSP4, which may be relevant to future HRV vaccine design.
- Published
- 1997
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