Your search keyword '"Pravat Nalini Sahoo"' showing total 16 results

1. HIV Skews a Balanced Mtb-Specific Th17 Response in Latent Tuberculosis Subjects to a Pro-inflammatory Profile Independent of Viral Load

Author

Srabanti Rakshit, Nitin Hingankar, Shuba Varshini Alampalli, Vasista Adiga, Bharath K. Sundararaj, Pravat Nalini Sahoo, Greg Finak, Anto Jesuraj Uday Kumar J, Chirag Dhar, George D’Souza, Rashmi Govind Virkar, Manisha Ghate, Madhuri R. Thakar, Ramesh S. Paranjape, Stephen C. De Rosa, Tom H.M. Ottenhoff, and Annapurna Vyakarnam

Subjects

HIV, tuberculosis, CD4+ T cells, CD8+ T cells, Th17, ART, Biology (General), QH301-705.5

Abstract

Summary: HIV infection predisposes latent tuberculosis-infected (LTBI) subjects to active TB. This study is designed to determine whether HIV infection of LTBI subjects compromises the balanced Mycobacterium tuberculosis (Mtb)-specific T helper 17 (Th17) response of recognized importance in anti-TB immunity. Comparative analysis of Mtb- and cytomegalovirus (CMV)-specific CD4+ T cell responses demonstrates a marked dampening of the Mtb-specific CD4+ T cell effectors and polyfunctional cells while preserving CMV-specific response. Additionally, HIV skews the Mtb-specific Th17 response in chronic HIV-infected LTBI progressors, but not long-term non-progressors (LTNPs), with preservation of pro-inflammatory interferon (IFN)-γ+/interleukin-17+ (IL-17+) and significant loss of anti-inflammatory IL-10+/IL-17+ effectors that is restored by anti-retroviral therapy (ART). HIV-driven impairment of Mtb-specific response cannot be attributed to preferential infection as cell-associated HIV DNA and HIV RNA reveal equivalent viral burden in CD4+ T cells from different antigen specificities. We therefore propose that beyond HIV-induced loss of Mtb-specific CD4+ T cells, the associated dysregulation of Mtb-specific T cell homeostasis can potentially enhance the onset of TB in LTBI subjects.

Published

2020

2. Evidence for Highly Variable, Region-Specific Patterns of T-Cell Epitope Mutations Accumulating in Mycobacterium tuberculosis Strains

Author

Arunachalam Ramaiah, Soumya Nayak, Srabanti Rakshit, Abigail L. Manson, Thomas Abeel, Sivakumar Shanmugam, Pravat Nalini Sahoo, Anto Jesuraj Uday Kumar John, Jagadish Chandrabose Sundaramurthi, Sujatha Narayanan, George D'Souza, Paul von Hoegen, Tom H. M. Ottenhoff, Soumya Swaminathan, Ashlee M. Earl, and Annapurna Vyakarnam

Subjects

Mycobacterium tuberculosis, genome sequence, T-cell epitopes, evolution, immune response, TB vaccine, Immunologic diseases. Allergy, RC581-607

Abstract

Vaccines that confer protection through induction of adaptive T-cell immunity rely on understanding T-cell epitope (TCE) evolution induced by immune escape. This is poorly understood in tuberculosis (TB), an ancient, chronic disease, where CD4 T-cell immunity is of recognized importance. We probed 905 functionally validated, curated human CD4 T cell epitopes in 79 Mycobacterium tuberculosis (Mtb) whole genomes from India. This screen resulted in identifying 64 mutated epitopes in these strains initially using a computational pipeline and subsequently verified by single nucleotide polymorphism (SNP) analysis. SNP based phylogeny revealed the 79 Mtb strains to cluster to East African Indian (EAI), Central Asian Strain (CAS), and Beijing (BEI) lineages. Eighty-nine percent of the mutated T-cell epitopes (mTCEs) identified in the 79 Mtb strains from India has not previously been reported. These mTCEs were encoded by genes with high nucleotide diversity scores including seven mTCEs encoded by six antigens in the top 10% of rapidly divergent Mtb genes encoded by these strains. Using a T cell functional assay readout, we demonstrate 62% of mTCEs tested to significantly alter CD4 T-cell IFNγ and/or IL2 secretion with associated changes in predicted HLA-DR binding affinity: the gain of function mutations displayed higher predicted HLA-DR binding affinity and conversely mutations resulting in loss of function displayed lower predicted HLA-DR binding affinity. Most mutated antigens belonged to the cell wall/cell processes, and, intermediary metabolism and respiration families though all known Mtb proteins encoded mutations. Analysis of the mTCEs in an SNP database of 5,310 global Mtb strains identified 82% mTCEs to be significantly more prevalent in Mtb strains isolated from India, including 36 mTCEs identified exclusively in strains from India. These epitopes had a significantly higher predicted binding affinity to HLA-DR alleles that were highly prevalent in India compared to HLA-DR alleles rare in India, highlighting HLA-DR maybe an important driver of these mutations. This first evidence of region-specific TCE mutations potentially employed by Mtb to escape host immunity has important implications for TB vaccine design.

Published

2019

3. Circulating HLA-DR+CD4+ effector memory T cells resistant to CCR5 and PD-L1 mediated suppression compromise regulatory T cell function in tuberculosis.

Author

Asma Ahmed, Vasista Adiga, Soumya Nayak, J Anto Jesuraj Uday Kumar, Chirag Dhar, Pravat Nalini Sahoo, Bharath K Sundararaj, George D Souza, and Annapurna Vyakarnam

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Chronic T cell activation is a hallmark of pulmonary tuberculosis (PTB). The mechanisms underpinning this important phenomenon are however, poorly elucidated, though known to rely on control of T effector cells (Teff) by regulatory T cells (Treg). Our studies show that circulating natural Treg cells in adults with PTB preserve their suppressive potential but Teff cells from such subjects are resistant to Treg-mediated suppression. We found this to be due to expansion of an activated Teff subset identified by Human Leukocyte Antigen (HLA)-DR expression. Sensitivity to suppression was restored to control levels by depletion of this subset. Comparative transcriptome analysis of Teff cells that contain HLA-DR+ cells versus the fraction depleted of this population identified putative resistance mechanisms linked to IFNG, IL17A, IL22, PD-L1 and β-chemokines CCL3L3, CCL4 expression. Antibody blocking experiments confirmed HLA-DR+ Teff cells, but not the fraction depleted of HLA-DR+ effectors, to be resistant to Treg suppression mediated via CCR5 and PD-L1 associated pathways. In the presence of HLA-DR+ Teff cells, activation of NFκB downstream of CCR5 and PD-L1 was perturbed. In addition, HLA-DR+ Teff cells expressed significantly higher levels of Th1/Th17 cytokines that may regulate Treg function through a reciprocal counter-balancing relationship. Taken together, our study provides novel insight on how activated HLA-DR+CD4+ T cells may contribute to disease associated inflammation by compromising Treg-mediated suppression in PTB.

Published

2018

4. BCG revaccination boosts adaptive polyfunctional Th1/Th17 and innate effectors in IGRA(+) and IGRA(-) Indian adults

Author

John Kenneth, Vasista Adiga, M. Juliana McElrath, Wesley Bonam, Christina Johnson, Stephen C. De Rosa, George D'Souza, Greg Finak, Asma Ahmed, Annapurna Vyakarnam, Raphael Gottardo, Srabanti Rakshit, Tom H. M. Ottenhoff, Kees L. M. C. Franken, Kenneth Stuart, Pravat Nalini Sahoo, and Bharath K. Sundararaj

Subjects

Adult, 0301 basic medicine, Tuberculosis, Adolescent, Endemic Diseases, T cell, Immunization, Secondary, India, complex mixtures, Mycobacterium tuberculosis, Young Adult, 03 medical and health sciences, Immunogenicity, Vaccine, 0302 clinical medicine, Immunity, medicine, Humans, Prospective Studies, Th1 th17, Centre for Infectious Disease Research, Antigens, Bacterial, biology, business.industry, Immunogenicity, General Medicine, Th1 Cells, biology.organism_classification, Acquired immune system, medicine.disease, Healthy Volunteers, Immunity, Innate, Treatment Outcome, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, BCG Vaccine, Th17 Cells, Female, Clinical Medicine, business, Interferon-gamma Release Tests, CD8

Abstract

BACKGROUND: Bacille Calmette-Guérin (BCG) vaccine is protective against Tuberculosis (TB) in children, but its efficacy wanes with age. Consequently, determining if BCG revaccination augments anti-TB immunity in young adults in TB endemic regions is vital. METHODS: Two hundred healthy adults, BCG vaccinated at birth, were tested for their IFN-γ release assay (IGRA) status. Of these, 28 IGRA(+) and 30 IGRA(–) were BCG revaccinated, and 24 IGRA(+) and 23 IGRA(–) subjects served as unvaccinated controls. T and innate cell responses to mycobacterial antigens were analyzed by 14-color flow cytometry over 34 weeks. RESULTS: IFN-γ and/or IL-2 Ag85A- and BCG-specific CD4(+) and CD8(+) T cell responses were boosted by revacciantion at 4 and 34 weeks, respectively, and were > 2-fold higher in IGRA(+) compared with IGRA(–) vaccinees. Polyfunctional Ag85A, BCG, and mycobacterium tuberculosis (Mtb) latency Ag–specific (LTAg-specific) CD4(+) T cells expressing up to 8 cytokines were also significantly enhanced in both IGRA(+) and IGRA(–) vaccinees relative to unvaccinated controls, most markedly in IGRA(+) vaccinees. A focused analysis of Th17 responses revealed expansion of Ag85A-, BCG-, and LTAg-specific total IL-17A(+),IL-17F(+),IL-22(+), and IL-10(+) CD4(+) T cell effectors in both IGRA(+) and IGRA(–) subjects. Also, innate IFN-γ(+) NK/γδ/NKT cell responses were higher in both IGRA(+) and IGRA(–) vaccinees compared with controls. This is the first evidence to our knowledge that BCG revaccination significantly boosts antimycobacterial Th1/Th17 responses in IGRA(+) and IGRA(–) subjects. CONCLUSION: These data show that BCG revaccination is immunogenic in IGRA(–) and IGRA(+) subjects, implying that Mtb preinfection in IGRA(+) subjects does not impact immunogenicity. This has implications for public health and vaccine development strategies. FUNDING: This work was funded principally by DBT-NIH (BT/MB/Indo-US/HIPC/2013).

Published

2019

5. Circulating HLA-DR+CD4+ effector memory T cells resistant to CCR5 and PD-L1 mediated suppression compromise regulatory T cell function in tuberculosis

Author

J. Anto Jesuraj Uday Kumar, George D. Souza, Annapurna Vyakarnam, Pravat Nalini Sahoo, Soumya Nayak, Bharath K. Sundararaj, Asma Ahmed, Chirag Dhar, Vasista Adiga, and Lewinsohn, David M.

Subjects

0301 basic medicine, Bacterial Diseases, CD4-Positive T-Lymphocytes, Male, Physiology, Lymphocyte Activation, T-Lymphocytes, Regulatory, B7-H1 Antigen, Immune tolerance, Interleukin 22, Sequencing techniques, Immune Physiology, Cellular types, lcsh:QH301-705.5, Staining, education.field_of_study, Innate Immune System, biology, Chemistry, Immune cells, Cell Staining, RNA sequencing, Regulatory T cells, Middle Aged, 3. Good health, Up-Regulation, Actinobacteria, medicine.anatomical_structure, Infectious Diseases, Host-Pathogen Interactions, White blood cells, Cytokines, Female, medicine.symptom, Research Article, lcsh:Immunologic diseases. Allergy, Adult, Cell biology, Blood cells, Receptors, CCR5, Regulatory T cell, T cell, Population, Immunology, T cells, Inflammation, Human leukocyte antigen, Research and Analysis Methods, Microbiology, 03 medical and health sciences, Latent Tuberculosis, Virology, PD-L1, Genetics, medicine, Immune Tolerance, Tuberculosis, Humans, education, Molecular Biology Techniques, Molecular Biology, Tuberculosis, Pulmonary, Medicine and health sciences, Biology and life sciences, Bacteria, Organisms, HLA-DR Antigens, Mycobacterium tuberculosis, Molecular Development, Tropical Diseases, 030104 developmental biology, lcsh:Biology (General), Animal cells, Specimen Preparation and Treatment, Immune System, Cancer research, biology.protein, Parasitology, lcsh:RC581-607, Immunologic Memory, Developmental Biology, Cloning

Abstract

Chronic T cell activation is a hallmark of pulmonary tuberculosis (PTB). The mechanisms underpinning this important phenomenon are however, poorly elucidated, though known to rely on control of T effector cells (Teff) by regulatory T cells (Treg). Our studies show that circulating natural Treg cells in adults with PTB preserve their suppressive potential but Teff cells from such subjects are resistant to Treg-mediated suppression. We found this to be due to expansion of an activated Teff subset identified by Human Leukocyte Antigen (HLA)-DR expression. Sensitivity to suppression was restored to control levels by depletion of this subset. Comparative transcriptome analysis of Teff cells that contain HLA-DR+ cells versus the fraction depleted of this population identified putative resistance mechanisms linked to IFNG, IL17A, IL22, PD-L1 and β-chemokines CCL3L3, CCL4 expression. Antibody blocking experiments confirmed HLA-DR+ Teff cells, but not the fraction depleted of HLA-DR+ effectors, to be resistant to Treg suppression mediated via CCR5 and PD-L1 associated pathways. In the presence of HLA-DR+ Teff cells, activation of NFκB downstream of CCR5 and PD-L1 was perturbed. In addition, HLA-DR+ Teff cells expressed significantly higher levels of Th1/Th17 cytokines that may regulate Treg function through a reciprocal counter-balancing relationship. Taken together, our study provides novel insight on how activated HLA-DR+CD4+ T cells may contribute to disease associated inflammation by compromising Treg-mediated suppression in PTB., Author summary An important marker of progression to PTB following Mycobacterium tuberculosis (Mtb) infection in humans is elevated frequencies of HLA-DR+CD4+ T cells, reflecting chronic T cell activation. However, the mechanisms by which activated HLA-DR+CD4+ T cells contribute to disease process is not known. We show that CD25- HLA-DR+CD4+ memory Teff from PTB patients are resistant to suppression mediated by Treg cells. An unbiased transcriptome analysis identified several key pathways that contribute to this resistance. Specifically, presence of HLA-DR+CD4+ T cells renders the effector population resistant to CCR5 and PD-L1 mediated suppression by Treg cells. In addition, the HLA-DR+CD4+ memory Teff cells express elevated levels of Th1/Th17 cytokines known to counter-regulate and dampen Treg suppression. These findings provide fresh insight to disease process in TB and identify HLA-DR+ Teff resistant to Treg suppression as a potential functional marker of disease.

Published

2018

6. Circulating Mycobacterium tuberculosis DosR latency antigen-specific, polyfunctional, regulatory IL10(+) Th17 CD4 T-cells differentiate latent from active tuberculosis

Author

Greg Finak, Chirag Dhar, Pravat Nalini Sahoo, Annapurna Vyakarnam, Srabanti Rakshit, J Anto Jesuraj Uk, Prabhat K. Sharma, George D. Souza, Krista E. van Meijgaarden, Soumya Nayak, Vasista Adiga, Tom H. M. Ottenhoff, and Stephen C. De Rosa

Subjects

0301 basic medicine, Tuberculosis, T cell, lcsh:Medicine, chemical and pharmacologic phenomena, Biochemistry, Mycobacterium tuberculosis, Interleukin 22, 03 medical and health sciences, 0302 clinical medicine, Tuberculosis diagnosis, Antigen, Immunity, medicine, lcsh:Science, Multidisciplinary, biology, lcsh:R, biology.organism_classification, medicine.disease, bacterial infections and mycoses, Virology, 3. Good health, Interleukin 10, 030104 developmental biology, medicine.anatomical_structure, Immunology, lcsh:Q, 030215 immunology

Abstract

The functional heterogeneity of T cell responses to diverse antigens expressed at different stages of Mycobacterium tuberculosis (Mtb) infection, in particular early secreted versus dormancy related latency antigens expressed later, that distinguish subjects with latent (LTBI), pulmonary (PTB) or extrapulmonary (EPTB) tuberculosis remains unclear. Here we show blood central memory CD4 T-cell responses specific to Mtb dormancy related (DosR) latency, but not classical immunodominant secretory antigens, to clearly differentiate LTBI from EPTB and PTB. The polyfunctionality score integrating up to 31 DosR-specific CD4 T-cell functional profiles was significantly higher in LTBI than EPTB or PTB subjects. Further analysis of 256 DosR-specific T-cell functional profiles identified regulatory IL10 + Th17 cells (IL10+IL17A+IL17F+IL22+) to be significantly enriched in LTBI; in contrast to pro-inflammatory Th17 cells (IFNγ+IL17A+/IL10−) in the blood and lung of EPTB and PTB subjects respectively. A blood polyfunctional, Mtb DosR latency antigen specific, regulatory, central memory response is therefore a novel functional component of T-cell immunity in latent TB and potential correlate of protection.

Published

2017

7. Circulating Mycobacterium tuberculosis DosR latency antigen-specific, polyfunctional, regulatory IL10

Author

Srabanti, Rakshit, Vasista, Adiga, Soumya, Nayak, Pravat Nalini, Sahoo, Prabhat Kumar, Sharma, Krista E, van Meijgaarden, Anto Jesuraj, Uk J, Chirag, Dhar, George D, Souza, Greg, Finak, Stephen C, De Rosa, Tom H M, Ottenhoff, and Annapurna, Vyakarnam

Subjects

Adult, Male, Adolescent, chemical and pharmacologic phenomena, Mycobacterium tuberculosis, Middle Aged, bacterial infections and mycoses, Article, Interleukin-10, DNA-Binding Proteins, Young Adult, Bacterial Proteins, T-Lymphocyte Subsets, CD4 Antigens, Humans, Th17 Cells, Tuberculosis, Female, Protein Kinases, Aged

Abstract

The functional heterogeneity of T cell responses to diverse antigens expressed at different stages of Mycobacterium tuberculosis (Mtb) infection, in particular early secreted versus dormancy related latency antigens expressed later, that distinguish subjects with latent (LTBI), pulmonary (PTB) or extrapulmonary (EPTB) tuberculosis remains unclear. Here we show blood central memory CD4 T-cell responses specific to Mtb dormancy related (DosR) latency, but not classical immunodominant secretory antigens, to clearly differentiate LTBI from EPTB and PTB. The polyfunctionality score integrating up to 31 DosR-specific CD4 T-cell functional profiles was significantly higher in LTBI than EPTB or PTB subjects. Further analysis of 256 DosR-specific T-cell functional profiles identified regulatory IL10 + Th17 cells (IL10+IL17A+IL17F+IL22+) to be significantly enriched in LTBI; in contrast to pro-inflammatory Th17 cells (IFNγ+IL17A+/IL10−) in the blood and lung of EPTB and PTB subjects respectively. A blood polyfunctional, Mtb DosR latency antigen specific, regulatory, central memory response is therefore a novel functional component of T-cell immunity in latent TB and potential correlate of protection.

Published

2017

8. Characterization of HIV Type 1 Subtype C protease Gene: Selection of L63P Mutation in Protease Inhibitor-Naive Indian Patients

Author

Anita Shet, Ravi Kumar, Ayesha De Costa, Ujjwal Neogi, and Pravat Nalini Sahoo

Subjects

Adult, Male, Adolescent, Maximum likelihood, medicine.medical_treatment, Molecular Sequence Data, Immunology, Human immunodeficiency virus (HIV), India, HIV Infections, Drug resistance, Biology, medicine.disease_cause, Young Adult, HIV Protease, Virology, Drug Resistance, Viral, medicine, Humans, Protease inhibitor (pharmacology), Amino Acid Sequence, Selection, Genetic, Child, Genotyping, Phylogeny, Genetics, Mutation, Protease, Sequence Analysis, DNA, Middle Aged, Genes, pol, Infectious Diseases, HIV-1, Female, Protease Gene

Abstract

Significant subtype-specific differences were observed in the protease (PR) region of the HIV-1 pol gene. Most of the previous studies were restricted to subtype B, although subtype C accounts for more than 50% of HIV infections worldwide. In this study we characterized PR sequences from primary clinical isolates from protease inhibitor (PI)-naive patients in South India (n=39) as well as database-derived HIV-1 subtype C sequences from India (n=542) and globally (n=2970). All the study sequences were identified as subtype C, which is predominant in India. Drug resistance genotyping analysis identified 2.6% (1/39) prevalence of major PI resistance (I54T) and 7.7% (3/39) of minor PI resistance (L10I, T74S, and A71T). Selection of T12S, I15V, L19I, M36I, R41K, H69K, L89M, and I93L was observed both in global and Indian subtype C while the L63P mutation was selected in Indian PR sequences. Three different codon-based maximum likelihood methods agreed on four sites (12, 19, 36, and 82) under positive selection in Indian sequences.

Published

2011

9. Dried blood spot HIV-1 RNA quantification: a useful tool for viral load monitoring among HIV-infected individuals in India

Author

Ujjwal, Neogi, Soham, Gupta, Rashmi, Rodridges, Pravat Nalini, Sahoo, Shwetha D, Rao, Bharat B, Rewari, Suresh, Shastri, Ayesha De, Costa, and Anita, Shet

Subjects

Adult, HIV-1, Commentary, Humans, India, RNA, Viral, HIV Infections, Dried Blood Spot Testing, Middle Aged, Viral Load, Real-Time Polymerase Chain Reaction

Abstract

Monitoring of HIV-infected individuals on antiretroviral treatment (ART) ideally requires periodic viral load measurements to ascertain adequate response to treatment. While plasma viral load monitoring is widely available in high-income settings, it is rarely used in resource-limited regions because of high cost and need for sophisticated sample transport. Dried blood spot (DBS) as source specimens for viral load measurement has shown promise as an alternative to plasma specimens and is likely to be a useful tool for Indian settings. The present study was undertaken to investigate the performance of DBS in HIV-1 RNA quantification against the standard plasma viral load assay.Between April-June 2011, 130 samples were collected from HIV-1-infected (n=125) and non-infected (n=5) individuals in two district clinics in southern India. HIV-1 RNA quantification was performed from DBS and plasma using Abbott m2000rt system after manual RNA extraction. Statistical analysis included correlation, regression and Bland-Altman analysis.The sensitivity of DBS viral load was 97 per cent with viral loads3.0 log 10 copies/ml. Measurable viral load (3.0 log 10 copies/ml) results obtained for the 74 paired plasma-DBS samples showed positive correlation between both the assays (r=0.96). For clinically acceptable viral load threshold values of5,000 copies/ml, Bland-Altman plots showed acceptable limits of agreement (-0.21 to +0.8 log 10 copies/ml). The mean difference was 0.29 log 10 copies/ml. The cost of DBS was $2.67 lower compared to conventional plasma viral load measurement in the setting.The significant positive correlation with standard plasma-based assay and lower cost of DBS viral load monitoring suggest that DBS sampling can be a feasible and economical means of viral load monitoring in HIV-infected individual in India and in other resource-limited settings globally.

Published

2013

10. Human APOBEC3G-mediated hypermutation is associated with antiretroviral therapy failure in HIV-1 subtype C-infected individuals

Author

Irene Bontell, Ujjwal Neogi, Anders Sönnerborg, Anita Shet, Akhil C. Banerjea, Pravat Nalini Sahoo, and Maria L. Ekstrand

Subjects

Adult, Male, Genotype, antiretroviral therapy, Molecular Sequence Data, Population, India, Somatic hypermutation, HIV Infections, APOBEC-3G Deaminase, Drug resistance, Biology, Virus, Cytidine Deaminase, Drug Resistance, Viral, Humans, education, Genotyping, education.field_of_study, drug resistance, hypermutation, Public Health, Environmental and Occupational Health, Sequence Analysis, DNA, Provirus, Virology, HIV Reverse Transcriptase, Reverse transcriptase, Treatment Outcome, Infectious Diseases, Anti-Retroviral Agents, APOBEC3G/F, DNA, Viral, Mutation, HIV-1, RNA, Viral, Female, Research Article

Abstract

Introduction: Human APOBEC3G/F (hA3G/F) restricts retroviral replication through G-to-A hypermutations, which can generate drug-resistant progenies in vitro . The clinical relevance is still inconclusive. To bridge this gap, we aim to study the role of these hypermutations in evolution of drug resistance; we characterised hA3G/F-mediated hypermutations in the RT region of the pol gene of patients with or without antiretroviral therapy (ART). Methods: In 88 HIV-1-positive individuals, drug resistance genotyping was carried out in plasma virus and provirus by population sequencing. Hypermutations were determined by three different approaches using Hypermut 2.0 software, cluster analysis and APOBEC3G-mediated defectives indices. Clinical and demographic characteristics of these individuals were studied in relation to these hypermutations. Results: hA3G/F-mediated hypermutated sequences in proviral DNA, but not in plasma virus, were identified in 11.4% (10/88) subjects. Proviral hypermutations were observed more frequently in patients with ART failure than in ART-naive individuals ( p = 0.03). In therapy failure patients, proviral hypermutation were associated with greater intra-compartmental genetic diversity ( p

Published

2013

11. Effectiveness of first-line antiretroviral therapy and acquired drug resistance among HIV-1-infected children in India

Author

Ayesha De Costa, Pravat Nalini Sahoo, Ujjwal Neogi, and Anita Shet

Subjects

Microbiology (medical), Male, Treatment response, Pediatrics, medicine.medical_specialty, Adolescent, First line, Human immunodeficiency virus (HIV), India, HIV Infections, Drug resistance, medicine.disease_cause, Drug Resistance, Viral, medicine, Antiretroviral treatment, Humans, Child, business.industry, Treatment options, Viral Load, Antiretroviral therapy, VIROLOGIC FAILURE, Infectious Diseases, Cross-Sectional Studies, Treatment Outcome, Anti-Retroviral Agents, Child, Preschool, Pediatrics, Perinatology and Child Health, Mutation, HIV-1, Female, business

Abstract

Analysis of treatment response among HIV-infected children in India on first-line antiretroviral treatment for >2 years revealed that 85% were virologically suppressed. Of those with virologic failure, only 17% manifested immunologic failure, whereas majority had resistance-associated mutations. The presence of resistance highlights the need for virologic monitoring of children receiving antiretroviral treatment to optimize treatment success and preserve future treatment options.

Published

2012

12. Comparative analysis of the host mediated antigen-specific responses In Indian cohorts with different TB infected states

Author

Bharath K. Sundararaj, T. H. M. Ottenhoff, Pravat Nalini Sahoo, Annapurna Vyakarnam, George D'Souza, Srabanti Rakshit, K. E. Van Meijgaarden, and A. Jesuraj

Subjects

Microbiology (medical), Infectious Diseases, business.industry, Host (biology), Antigen specific, Immunology, Medicine, General Medicine, business, Virology

Published

2016

13. Higher prevalence of predicted X4-tropic strains in perinatally infected older children with HIV-1 subtype C in India

Author

Anita Shet, Ujjwal Neogi, Karthika Arumugam, Pravat Nalini Sahoo, Ayesha De Costa, and Anders Sönnerborg

Subjects

Male, Receptors, CXCR4, Adolescent, Receptors, CCR5, viruses, Population, Human immunodeficiency virus (HIV), India, HIV Infections, Biology, medicine.disease_cause, CXCR4, Genotype, medicine, Prevalence, Humans, Pharmacology (medical), education, Child, Tropism, education.field_of_study, Base Sequence, Disease progression, virus diseases, Gene Products, env, Virology, Viral Tropism, Infectious Diseases, Child, Preschool, Immunology, Coreceptor tropism, Tissue tropism, HIV-1, Female

Abstract

BACKGROUND Coreceptor switch from CCR5 to CXCR4 is considered to be less common in HIV-1 subtype C even in advanced stages of infection. In this study, we have examined viral genotypic coreceptor tropism and its clinical, virological, and host genetic determinants among perinatally infected children in India. METHODS Genotypic coreceptor tropism analysis was conducted on env V3 sequences using Geno2pheno with a threshold of 10% false-positive rate. A total of 473 sequences were obtained from 72 isolates amplified from children aged 2-17 years. Factors associated with viral tropism in subtype C infections were studied using logistic regression. RESULTS Among the samples, 98.6% (71 of 72) were HIV-1 subtype C. Coreceptor tropism analysis determined 81.7% (58 of 71) as R5 tropic, 9.9% (7 of 71) as X4 tropic, and 8.5% (6 of 71) as R5/X4 tropic or dual-tropic HIV-1 strains. Children with X4 or R5/X4 strains were more likely to be older than those with R5-tropic strains (P < 0.05), have lower CD4 counts (P < 0.05), and have viral populations with greater intrapopulation viral divergence (P < 0.01). Older age was a significant independent predictor for X4 or R5/X4 tropism in these children (P < 0.05). None were identified as being heterozygous or homozygous for the CCR5[INCREMENT]32 deletion. CONCLUSIONS The high prevalence of X4 and R5/X4 tropic strains among older perinatally infected children with HIV-1 subtype C in India indicate that this phenomenon is not uncommon as previously thought and suggest that coreceptor transition can occur with longer duration of infection and greater disease progression in this population of perinatally infected children living with HIV-1 subtype C.

Published

2011

14. Emergence of HIV-1 drug resistance in antiretroviral therapy experienced perinatally infected children in South India

Author

Ujjwal Neogi, Anita Shet, Ayesha De Costa, and Pravat Nalini Sahoo

Subjects

medicine.medical_specialty, Pathology, business.industry, virus diseases, Drug resistance, biochemical phenomena, metabolism, and nutrition, Resistance mutation, Virological failure, Antiretroviral therapy, Virology, Medical microbiology, Infectious Diseases, Parasitology, Tropical medicine, Poster Presentation, Medicine, business, Viral load

Abstract

Results Among those who had been on ART for a median period of 24 months 51 children (83.6%) achieved virological suppression. There were 10 children with virological failure, and only two amongst these manifested immunological failure. Nine children (90%) had reverse transcriptase-related DRMs, and none had protease inhibitor-related DRMs. The most frequent NRTI mutation was M184V (n=9) followed by two thymidine analogous associated mutations (TAMs) M41L and T215Y (n=2). The most frequent nNRTI mutations were K103N (n=6) and Y181C (n=3).

Published

2012

15. Characterization of HIV Type 1 Subtype C proteaseGene: Selection of L63P Mutation in Protease Inhibitor-Naive Indian Patients.

Author

Ujjwal Neogi, Pravat Nalini Sahoo, Ravi Kumar, Ayesha De Costa, and Anita Shet

Abstract

AbstractSignificant subtype-specific differences were observed in the protease (PR) region of the HIV-1 polgene. Most of the previous studies were restricted to subtype B, although subtype C accounts for more than 50% of HIV infections worldwide. In this study we characterized PR sequences from primary clinical isolates from protease inhibitor (PI)-naive patients in South India (n=39) as well as database-derived HIV-1 subtype C sequences from India (n=542) and globally (n=2970). All the study sequences were identified as subtype C, which is predominant in India. Drug resistance genotyping analysis identified 2.6% (1/39) prevalence of major PI resistance (I54T) and 7.7% (3/39) of minor PI resistance (L10I, T74S, and A71T). Selection of T12S, I15V, L19I, M36I, R41K, H69K, L89M, and I93L was observed both in global and Indian subtype C while the L63P mutation was selected in Indian PR sequences. Three different codon-based maximum likelihood methods agreed on four sites (12, 19, 36, and 82) under positive selection in Indian sequences. [ABSTRACT FROM AUTHOR]

Published

2011

16. High viremia and low level of transmitted drug resistance in anti-retroviral therapy-naïve perinatally-infected children and adolescents with HIV-1 subtype C infection

Author

Anita Shet, Ujjwal Neogi, Ayesha De Costa, and Pravat Nalini Sahoo

Subjects

Male, medicine.medical_specialty, HIV-1 perinatal transmission, Adolescent, Genotype, Population, India, HIV Infections, Viremia, Drug resistance, Biology, Asymptomatic, lcsh:Infectious and parasitic diseases, Medical microbiology, Drug Resistance, Viral, medicine, Humans, lcsh:RC109-216, Child, education, Genotyping, Asymptomatic Diseases, education.field_of_study, Viral Load, Subtype C, medicine.disease, Virology, Cross-Sectional Studies, Infectious Diseases, Child, Preschool, Viral dynamics, HIV-1, Female, medicine.symptom, Viral load, Research Article

Abstract

Background High plasma viremia in HIV-1 infection is associated with rapid CD4 cell decline and faster disease progression. Children with HIV infection have high viral loads, particularly in early childhood. In this study we sought to understand the relationship between duration of HIV-1 infection and viral dynamics among perinatally-infected children and adolescents in India along with transmitted drug resistance in this population. Methods During 2007–2011, cross-sectional samples were collected from ART-naïve children (n = 105) with perinatally-acquired HIV infection, aged 2–16 years from Bangalore, India. CD4 counts, viral load and in-house genotyping were performed and transmitted drug resistance mutations were identified using the World Health Organization recommendations for Surveillance of Drug Resistance Mutations (SDRM_2009) list. Results Among 105 children studied, 73.3% (77/105) were asymptomatic, but had a median viral load of 5.24 log copies/mL (IQR 4.62-5.66). In the adolescent age group, 54% (21/39) had high levels of viremia (median 5.14 log copies/mL) but were asymptomatic. HIV-1 subtyping identified 98% strains (103/105) as subtype C; one A1 and one unique recombinant form (URF). Transmitted NRTI resistance was 1.9% (2/105); NNRTI resistance was 4.8% (5/105) and overall prevalence of transmitted drug resistance was 5.7% (6/105). Conclusions The high burden of plasma viremia found among untreated asymptomatic adolescents needs to be addressed both from an individual angle to halt disease progression, and from a public health perspective to arrest horizontal transmission. The low level of transmitted drug resistance among perinatally-infected children is reassuring; however with improving ART access globally, regular genotyping surveillance is indicated.