Your search keyword '"Vinayaka R. Prasad"' showing total 92 results

51. Methods to Study Monocyte Migration Induced by HIV-Infected Cells

Author

Joan W. Berman, Eliseo A. Eugenin, Vinayaka R. Prasad, and Vasudev R. Rao

Subjects

Chemokine, Biology, Article, Monocytes, law.invention, Cell Line, Cell Migration Assays, Leukocyte, law, Cell Movement, Hiv infected, medicine, Humans, Cells, Cultured, Monocyte, virus diseases, medicine.disease, Chemokine activity, In vitro, Cell biology, medicine.anatomical_structure, Cell culture, biology.protein, Recombinant DNA, HIV-1, tat Gene Products, Human Immunodeficiency Virus, Chemokines, Infiltration (medical)

Abstract

HIV-associated dementia (HAD) is a multi-factorial disease set in motion by the presence of HIV-infected cells in the brain. A characteristic feature of HAD is the infiltration of mononuclear phagocytes into the brain, which is aided by HIV-1 Tat protein and other chemokines secreted by both HIV-infected cells and uninfected cells in their vicinity. Both direct and indirect chemokine activity of HIV-1 Tat protein has been demonstrated employing purified recombinant Tat protein. However, a corroboration of a key role for Tat or other chemokines in monocyte migration, in the context of HIV-infection, has not yet been demonstrated. Here we describe methods, to measure the role of soluble factors, such as chemokines and Tat, released by HIV-infected cells or uninfected cells in their vicinity, in monocyte migration in vitro.

Published

2009

52. Analysis of 2-LTR circle junctions of viral DNA in infected cells

Author

Vinayaka R. Prasad and Dibyakanti Mandal

Subjects

viruses, T-Lymphocytes, Viral transformation, Biology, Virus Replication, Virology, Reverse transcriptase, Article, Cell Line, chemistry.chemical_compound, Real-time polymerase chain reaction, Viral replication, chemistry, Rolling circle replication, Viral entry, DNA, Viral, HIV-1, Humans, HIV Long Terminal Repeat, DNA, Circular, DNA

Abstract

The unintegrated viral DNA synthesized during human immunodeficiency virus type 1 infection includes linear and circular forms. Circular forms of viral DNA are surrogate markers for nuclear import of viral DNA during virus replication as well as events surrounding the completion of reverse transcription. Analysis of 2-LTR circles is convenient and the quantity of 2-LTR circle formed is directly proportional to the amount of viral DNA imported into the cell nucleus. In addition, correct synthesis of 2-LTR circles is an outcome of HIV-1 Gag-Pol function. Thus, quantitation and sequence analysis of 2-LTR circles have been very important in studying the structure and function relationship of key viral proteins. In this chapter, we describe the methods of quantitation and analysis of 2-LTR circle junctions isolated from HIV-1 infected cells.

Published

2008

53. HIV-1 clade-specific differences in the induction of neuropathogenesis

Author

Vinayaka R. Prasad, Andrew Sas, Eliseo A. Eugenin, Nagadenahalli B. Siddappa, Joan W. Berman, William R. Tyor, Vasudev R. Rao, Heather A. Bimonte-Nelson, and Udaykumar Ranga

Subjects

AIDS Dementia Complex, HIV Infections, Mice, SCID, CCL2, Biology, Virus, Article, Mice, Immune system, medicine, Animals, Humans, Clade, Cells, Cultured, General Neuroscience, Monocyte, virus diseases, medicine.disease, Virology, In vitro, Astrogliosis, Mice, Inbred C57BL, medicine.anatomical_structure, Immunology, Gene Products, tat, HIV-1, Neuropathogenesis

Abstract

Human immunodeficiency virus (HIV)-associated dementia (HAD) is common among clade B HIV-infected individuals, but less common and less severe among individuals infected with clade C HIV-1, suggesting clade-specific differences in neuropathogenicity. Although differences in neuropathogenicity have been investigatedin vitrousing viral proteins responsible for HAD, to date there are no virological studies using animal models to address this issue. Therefore, we investigated neuropathogenesis induced by HIV-1 clades using the severe combined immune deficiency (SCID) mouse HIV encephalitis model, which involves intracranial injection of macrophages infected with representative clade B (HIV-1ADA) or clade C (HIV-1Indie-C1) HIV-1 isolates into SCID mice. In cognitive tests, mice exposed to similar inputs of HIV-1 clade C made fewer memory errors than those exposed to HIV-1 clade B. Histopathological analysis of mice exposed to clade B exhibited greater astrogliosis and increased loss of neuronal network integrity.In vitroexperiments revealed differences in a key characteristic of HIV-1 that influences HAD, increased monocyte infiltration. HIV-1Indie-C1-infected macrophages recruited monocytes poorlyin vitrocompared with HIV-1ADA-infected macrophages. Monocyte recruitment was HIV-1 Tat and CCL2 dependent. This is the first demonstration, ever since HIV neuropathogenesis was first recognized, that viral genetic differences between clades can affect disease severity and that such studies help identify key players in neuropathogenesis by HIV-1.

Published

2008

54. Utilization of a Deoxynucleoside Diphosphate Substrate by HIV‐1 Reverse Transcriptase

Author

Vinayaka R. Prasad and Scott J. Garforth

Subjects

Chemistry, Genetics, Human immunodeficiency virus (HIV), medicine, Substrate (chemistry), medicine.disease_cause, Molecular Biology, Biochemistry, Combinatorial chemistry, Reverse transcriptase, Biotechnology

Published

2008

55. The active site residue Valine 867 in human telomerase reverse transcriptase influences nucleotide incorporation and fidelity

Author

Vinayaka R. Prasad and William C. Drosopoulos

Subjects

Models, Molecular, Telomerase, Protein subunit, Biology, Conserved sequence, 03 medical and health sciences, Telomerase RNA component, 0302 clinical medicine, Genetics, Humans, Thymine Nucleotides, Telomerase reverse transcriptase, Amino Acid Sequence, Polymerase, Conserved Sequence, 030304 developmental biology, 0303 health sciences, Binding Sites, Nucleotides, Nucleic Acid Enzymes, Valine, Processivity, DNA, Templates, Genetic, Molecular biology, Telomere, Biochemistry, Amino Acid Substitution, 030220 oncology & carcinogenesis, Mutation, biology.protein, Sequence Alignment

Abstract

Human telomerase reverse transcriptase (hTERT), the catalytic subunit of human telomerase, contains conserved motifs common to retroviral reverse transcriptases and telomerases. Within the C motif of hTERT is the Leu866-Val867-Asp868-Asp869 tetrapeptide that includes a catalytically essential aspartate dyad. Site-directed mutagenesis of Tyr183 and Met184 residues in HIV-1 RT, residues analogous to Leu866 and Val867, revealed that they are key determinants of nucleotide binding, processivity and fidelity. In this study, we show that substitutions at Val867 lead to significant changes in overall enzyme activity and telomere repeat extension rate, but have little effect on polymerase processivity. All Val867 substitutions examined (Ala, Met, Thr) led to reduced repeat extension rates, ranging from approximately 20 to 50% of the wild-type rate. Reconstitution of V867M hTERT and telomerase RNAs (TRs) with mutated template sequences revealed the effect on extension rate was associated with a template copying defect specific to template A residues. Furthermore, the Val867 hTERT mutants also displayed increased nucleotide incorporation fidelity, implicating Val867 as a determinant of telomerase fidelity. These findings suggest that by evolving to have a valine at position 867, the wild-type hTERT protein may have partially compromised polymerase fidelity for optimal and rapid repeat synthesis.

Published

2007

56. High-affinity RNA Aptamers Against the HIV-1 Protease Inhibit Both In Vitro Protease Activity and Late Events of Viral Replication

Author

Vinayaka R. Prasad, Sonald Duclair, Archana Gautam, and Andrew D. Ellington

Subjects

medicine.medical_treatment, Aptamer, Biology, HIV-1 protease, RNA aptamer structure, Drug Discovery, medicine, Nucleotide, chemistry.chemical_classification, Protease, lcsh:RM1-950, Mutagenesis, Molecular biology, In vitro, HIV-1 inhibitor, 3. Good health, lcsh:Therapeutics. Pharmacology, RNA aptamer, Viral replication, chemistry, HIV-1 PR inhibitor, biology.protein, anti-HIV-1 gene therapy, Molecular Medicine, Original Article, Systematic evolution of ligands by exponential enrichment

Abstract

HIV-1 aspartyl protease (PR) plays a key role in virion morphogenesis, underscoring the effectiveness of protease inhibitors (PI). Despite their utility, side effects and drug-resistance remains a problem. We report the development of RNA aptamers as inhibitors of HIV-1 PR for potential use in anti-HIV gene therapy. Employing Systematic Evolution of Ligands by Exponential Enrichment (SELEX), we isolated four unique families of anti-HIV-1 PR RNA aptamers displaying moderate binding affinities (Kd = 92–140 nmol/l) and anti-PR inhibitory activity (Kis = 138–647 nmol/l). Second-generation RNA aptamers selected from partially randomized pools based on two of the aptamer sequences displayed striking enhancements in binding (Kds = 2–22 nmol/l) and inhibition (Kis = 31–49 nmol/l). The aptamers were specific in that they did not bind either the related HIV-2 protease, or the cellular aspartyl protease, Cathepsin D. Site-directed mutagenesis of a second-generation aptamer to probe the predicted secondary structure indicated that the stem-loops SL2 and SL3 and the stem P1 were essential for binding and that only the 3’-most 17 nucleotides were dispensable. Anti-PR aptamers inhibited HIV replication in vitro and the degree of inhibition was higher for second-generation aptamers with greater affinity and the inhibition was abrogated for a nonbinding aptamer variant.

Published

2015

57. Structural features of mouse telomerase RNA are responsible for the lower activity of mouse telomerase versus human telomerase

Author

Vinayaka R. Prasad, Yan Yun Wu, and Scott J. Garforth

Subjects

Cell Extracts, Telomerase, Chemistry, RNA, Context (language use), Translation (biology), Cell Biology, Templates, Genetic, Biochemistry, Molecular biology, Protein Structure, Secondary, Telomere, Telomerase RNA component, Mice, Cell Line, Tumor, Mutation, Animals, Humans, Telomerase reverse transcriptase, Nucleic acid structure, Molecular Biology, Research Article

Abstract

Human and mouse telomerases show a high degree of similarity in both the protein and RNA components. Human telomerase is more active and more processive than the mouse telomerase. There are two key differences between hTR [human TR (telomerase RNA)] and mTR (mouse TR) structures. First, the mouse telomerase contains only 2 nt upstream of its template region, whereas the human telomerase contains 45 nt. Secondly, the template region of human telomerase contains a 5-nt alignment domain, whereas that of mouse has only 2 nt. We hypothesize that these differences are responsible for the differential telomerase activities. Mutations were made in both the hTR and mTR, changing the template length and the length of the RNA upstream of the template, and telomerase was reconstituted in vitro using mouse telomerase reverse transcriptase generated by in vitro translation. We show that the sequences upstream of the template region, with a potential to form a double-stranded helix (the P1 helix) as in hTR, increase telomerase activity. The longer alignment domain increases telomerase activity only in the context of the P1 helix. Thus the TR contributes to regulating the level of activity of mammalian telomerases.

Published

2006

58. Structural determinants of slippage-mediated mutations by human immunodeficiency virus type 1 reverse transcriptase

Author

Kenneth Curr, Eddy Arnold, Vasudev R. Rao, Snehlata Tripathi, Stefan G. Sarafianos, Monica E. Hamburgh, Thomas A. Darden, Vinayaka R. Prasad, Bradley D. Preston, and Melissa Monaghan

Subjects

Models, Molecular, Genes, Viral, Protein Conformation, Mutant, Molecular Sequence Data, Human immunodeficiency virus (HIV), Oligonucleotides, Glutamic Acid, Biology, medicine.disease_cause, Virus Replication, Biochemistry, Frameshift mutation, law.invention, law, Drug Resistance, Viral, medicine, Nucleotide, Frameshift Mutation, Molecular Biology, DNA Primers, chemistry.chemical_classification, Base Sequence, Models, Genetic, Lysine, RNA-Directed DNA Polymerase, Cell Biology, DNA, Templates, Genetic, Molecular biology, Reverse transcriptase, HIV Reverse Transcriptase, Recombinant Proteins, chemistry, Lac Operon, DNA, Viral, Mutation, Recombinant DNA, HIV-1, Slippage, Salt bridge, Gene Deletion

Abstract

Single-base deletions at nucleotide runs or -1 frameshifting by human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT) result from template slippage during polymerization. In crystal structures of HIV-1 RT complexed with DNA-DNA template-primer, the palm subdomain in the template cleft contacts the template backbone near the proposed site of slippage via the Glu(89) side chain. We investigated the role of Glu(89) in frameshifting by perturbing this interaction. Substitutions with Asp, Gly, Ala, Val, Ser, Thr, Asn, or Lys were created in recombinant HIV RT, and frameshift frequencies of the resulting mutant RTs were measured. All substitutions led to reduced -1 frameshifting by HIV-1 RT (2-40-fold). Interestingly, the suppression of -1 frameshifting frequently coincided with an enhancement of +1 frameshifting (3-47-fold) suggesting that Glu(89) can influence the slippage of both strands. Glu(89) substitutions also led to reduced rates of dNTP misincorporation that paralleled reductions in -1 frameshifting, suggesting a common structural mechanism for both classes of RT error. Our results reveal a major influence of Glu(89) on slippage-mediated errors and dNTP incorporation fidelity. The crystal structure of HIV-1 RT reveals a salt bridge between Glu(89) and Lys(154), which may facilitate -1 frameshifting; this concept is supported by the observed reduction in -1 frameshifting for K154A and K154R mutants.

Published

2006

59. Influence of naturally occurring insertions in the fingers subdomain of human immunodeficiency virus type 1 reverse transcriptase on polymerase fidelity and mutation frequencies in vitro

Author

Vinayaka R. Prasad, Kenneth Curr, Brendan Larder, Snehlata Tripathi, and Johan Lennerstrand

Subjects

HIV-1/drug effects/*enzymology/*genetics, Medicin och hälsovetenskap, Anti-HIV Agents, Mutant, Medical and Health Sciences, law.invention, 03 medical and health sciences, Catalytic Domain/genetics, law, Catalytic Domain, Virology, Drug Resistance, Viral, Anti-HIV Agents/pharmacology, medicine, Humans, Nucleotide, Polymerase, DNA Primers, 030304 developmental biology, chemistry.chemical_classification, Genetics, 0303 health sciences, biology, Nucleoside analogue, 030302 biochemistry & molecular biology, Nucleosides, Drug Resistance, Viral/genetics, Nucleotidyltransferase, Molecular biology, HIV Reverse Transcriptase, Reverse transcriptase, 3. Good health, DNA Primers/chemistry/genetics/metabolism, chemistry, Amino Acid Substitution, Duplex (building), Mutation, HIV-1, biology.protein, Recombinant DNA, HIV Reverse Transcriptase/chemistry/*genetics/*metabolism, medicine.drug, Nucleosides/metabolism

Abstract

The fingers subdomain of human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT) is a hotspot for nucleoside analogue resistance mutations. Some multi-nucleoside analogue-resistant variants contain a T69S substitution along with dipeptide insertions between residues 69 and 70. This set of mutations usually co-exists with classic zidovudine-resistance mutations (e.g. M41L and T215Y) or an A62V mutation and confers resistance to multiple nucleoside analogue inhibitors. As insertions lie in the vicinity of the dNTP-binding pocket, their influence on RT fidelity was investigated. Commonly occurring insertion mutations were selected, i.e. T69S-AG, T69S-SG and T69S-SS alone, in combination with 3′-azido-2′,3′-deoxythymidine-resistance mutations M41L, L210W, R211K, L214F, T215Y (LAGAZand LSGAZ) or with an alternate set where A62V substitution replaces M41L (VAGAZ, VSGAZand VSSAZ). Using alacZαgapped duplex substrate, the forward mutation frequencies of recombinant wild-type and mutant RTs bearing each of the above sets of mutations were measured. All of the mutants displayed significant decreases in mutation frequencies. Whereas the dipeptide insertions alone showed the least decrease (4·0- to 7·5-fold), the VAG series showed an intermediate reduction (5·0- to 11·4-fold) and the LAG set showed the largest reduction in mutation frequencies (15·3- and 16·3-fold for LAGAZand LSGAZ, respectively). Single dNTP exclusion assays for mutants LSGAZand LAGAZconfirmed their large reduction in misincorporation efficiencies. The increasedin vitrofidelity was not due to excision of the incorrect nucleotide via ATP-dependent removal. There was also no direct correlation between increased fidelity and template–primer affinity, suggesting a change in the active site that is conducive to better discrimination during dNTP insertion.

Published

2006

60. HIV-1 reverse transcriptase mutations that confer decreased in vitro susceptibility to anti-RT DNA aptamer RT1t49 confer cross resistance to other anti-RT aptamers but not to standard RT inhibitors

Author

Vinayaka R. Prasad, Pheroze Joshi, and Timothy S. Fisher

Subjects

lcsh:Immunologic diseases. Allergy, 0303 health sciences, Research, Aptamer, 030302 biochemistry & molecular biology, Mutant, RNA, Processivity, Biology, Virology, Molecular biology, Reverse transcriptase, In vitro, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, chemistry, biology.protein, Molecular Medicine, Pharmacology (medical), lcsh:RC581-607, RNase H, DNA, 030304 developmental biology

Abstract

RNA and DNA aptamers specific for HIV-1 reverse transcriptase (RT) can inhibit reverse transcription in vitro. RNA aptamers have been shown to potently block HIV-1 replication in culture. We previously reported mutants of HIV-1 RT with substitutions N255D or N265D that display resistance to the DNA aptamer RT1t49. Variant viruses bearing these mutations singly or in combination were compromised for replication. In order to address the wider applicability of such aptamers, HIV-1 RT variants containing the N255D, N265D or both (Dbl) were tested for the extent of their cross-resistance to other DNA/RNA aptamers as well as to other RT inhibitors. Both N265D and Dbl RTs were resistant to most aptamers tested. N255D mutant displayed mild resistance to two of the DNA aptamers, little change in sensitivity to three and hypersensitivity to one. Although all mutants displayed wild type-like ribonuclease H activity, their activity was compromised under conditions that prevent re-binding. This suggests that the processivity defect caused by these mutations can also affect RNase H function thus contributing further to the replication defect in mutant viruses. These results indicate that mutants conferring resistance to anti-RT aptamers significantly affect many HIV-1 RT enzymatic activities, which could contribute to preventing the development of resistance in vivo. If such mutations were to arise in vivo, our results suggest that variant viruses should remain susceptible to many existing anti-RT inhibitors. This result was tempered by the observation that NRTI-resistance mutations such as K65R can confer resistance to some anti-RT aptamers.

Published

2005

61. Aptamers directed to HIV-1 reverse transcriptase display greater efficacy over small hairpin RNAs targeted to viral RNA in blocking HIV-1 replication

Author

Pheroze Joshi, Vinayaka R. Prasad, and Thomas W. North

Subjects

Small interfering RNA, Time Factors, Transcription, Genetic, Aptamer, Biology, Virus Replication, Virus, Green fluorescent protein, Viral vector, Cell Line, RNA, Small Nuclear, Drug Discovery, Genetics, Promoter Regions, Genetic, Gene, Molecular Biology, Base Pairing, Pharmacology, RNA, Virology, Reverse transcriptase, HIV Reverse Transcriptase, Kinetics, HIV-1, Molecular Medicine, RNA, Viral

Abstract

RNA molecules can be powerful inhibitors of HIV-1 replication. To determine the relative efficacy of siRNAs and RNA aptamers, a direct comparison of three anti-HIV reverse transcriptase aptamers and three shRNAs targeted to HIV-1(R3b) was made. U6 promoter-driven anti-HIV genes were delivered into CEMx174 cells via a retroviral vector, and transduced cells were sorted out via green fluorescent protein function and challenged with HIV. The results show that, at low virus input, shRNAs can block HIV as efficiently as aptamers. When expressed in target cells, both classes of inhibitors blocked early events of reverse transcription, suggesting they are both able to access intracellular reverse transcription complexes. However, at higher multiplicities of infection (m.o.i. of 50), while the aptamers could efficiently inhibit HIV replication, shRNAs did not. RNase protection assays indicated similar steady-state levels or nucleocytoplasmic distribution showing that the differential efficacy was not a reflection of intracellular concentration. The higher potency of anti-RT aptamers could be due to their ability to inhibit two successive rounds of reverse transcription owing to their unique ability to be encapsidated into virion particles. Furthermore, anti-RT aptamers expressed in T cells afforded protection against high-dose infection by chimeric RT-SHIV viruses.

Published

2004

62. Interaction between human immunodeficiency virus type 1 reverse transcriptase and integrase proteins

Author

Vinayaka R. Prasad, Pheroze Joshi, Ganjam V. Kalpana, and Eric A. Hehl

Subjects

Binding Sites, Immunology, Replication, Processivity, HIV Integrase, Biology, Nucleotidyltransferase, Microbiology, Molecular biology, Reverse transcriptase, Catalysis, HIV Reverse Transcriptase, Conserved sequence, Integrase, Viral replication, Virology, Insect Science, biology.protein, Binding site, Dimerization, Conserved Sequence, Micrococcal nuclease

Abstract

Reverse transcriptase (RT) and integrase (IN) are two key catalytic enzymes encoded by all retroviruses. It has been shown that a specific interaction occurs between the human immunodeficiency virus type 1 (HIV-1) RT and IN proteins (X. Wu, H. Liu, H. Xiao, J. A. Conway, E. Hehl, G. V. Kalpana, V. R. Prasad, and J. C. Kappes, J. Virol. 73:2126-2135, 1999). We have now further examined this interaction to map the binding domains and to determine the effects of interaction on enzyme function. Using recombinant purified proteins, we have found that both a HIV-1 RT heterodimer (p66/p51) and its individual subunits, p51 and p66, are able to bind to HIV-1 IN. An oligomerization-defective mutant of IN, V260E, retained the ability to bind to RT, showing that IN oligomerization may not be required for interaction. Furthermore, we report that the C-terminal domain of IN, but not the N-terminal zinc-binding domain or the catalytic core domain, was able to bind to heterodimeric RT. Deletion analysis to map the IN-binding domain on RT revealed two separate IN-interacting domains: the fingers-palm domain and the carboxy-terminal half of the connection subdomain. The carboxy-terminal domain of IN alone retained its interaction with both the fingers-palm and the connection-RNase H fragments of RT, but not with the half connection-RNase H fragment. This interaction was not bridged by nucleic acids, as shown by micrococcal nuclease treatment of the proteins prior to the binding reaction. The influences of IN and RT on each other's activities were investigated by performing RT processivity and IN-mediated 3′ processing and joining reactions in the presence of both proteins. Our results suggest that, while IN had no influence on RT processivity, RT stimulated the IN-mediated strand transfer reaction in a dose-dependent manner up to 155-fold. Thus, a functional interaction between these two viral enzymes may occur during viral replication.

Published

2004

63. Tat Protein of Human Immunodeficiency Virus Type 1 Subtype C Strains Is a Defective Chemokine

Author

Raj Shankarappa, Nagadenahalli B. Siddappa, Vinayaka R. Prasad, Susarla K. Shankar, Ramalingam Nagendran, Udaykumar Ranga, Marthandan Mahalingam, Lakshmi Ramakrishna, Narayana Jayasuryan, Anita Mahadevan, and Parthasarathy Satishchandra

Subjects

Gene Expression Regulation, Viral, Transcriptional Activation, Chemokine, AIDS Dementia Complex, Immunology, Mutant, Mutation, Missense, Microbiology, Virus, Monocytes, Conserved sequence, Cell Line, Transactivation, Virology, medicine, Humans, Conserved Sequence, Phylogeny, biology, Monocyte, Chemotaxis, Wild type, biology.organism_classification, Protein Structure, Tertiary, medicine.anatomical_structure, Insect Science, Lentivirus, Gene Products, tat, biology.protein, HIV-1, Pathogenesis and Immunity, tat Gene Products, Human Immunodeficiency Virus, Chemokines

Abstract

Human immunodeficiency virus type 1 (HIV-1)-associated dementia (HAD) is correlated with increased monocyte migration to the brain, and the incidence of HAD among otherwise asymptomatic subjects appears to be lower in India than in the United States and Europe (1 to 2% versus 15 to 30%). Because of the genetic differences between HIV-1 strains circulating in these regions, we sought to identify viral determinants associated with this difference. We targeted Tat protein for these studies in view of its association with monocyte chemotactic function. Analyses of Tat sequences representing nine subtypes revealed that at least six amino acid residues are differentially conserved in subtype C Tat (C-Tat). Of these, cysteine (at position 31) was highly (>99%) conserved in non-subtype C viruses and more than 90% of subtype C viruses encoded a serine. We hypothesized a compromised chemotactic function of C-Tat due to the disruption of CC motif and tested it with the wild type C-Tat (CS) and its two isogenic variants (CC and SC) derived by site-directed mutagenesis. We found that the CS natural variant was defective for monocyte chemotactic activity without a loss in the transactivation property. While the CC mutant is functionally competent for both the functions, in contrast, the SC mutant was defective in both. Therefore, the loss of the C-Tat chemotactic property may underlie the reduced incidence of HAD; although not presenting conclusive evidence, this study provides the first evidence for a potential epidemiologic phenomenon associated with biological differences in the subtype C viruses.

Published

2004

64. Anti-HIV inhibitors based on nucleic acids: emergence of aptamers as potent antivirals

Author

Vinayaka R. Prasad, T S Fisher, and Pheroze Joshi

Subjects

Microbiology (medical), Pharmacology, Base Sequence, Anti-HIV Agents, Aptamer, Genetic enhancement, Molecular Sequence Data, RNA, HIV Infections, Biology, Virus Replication, Small molecule, Virology, DNA, Antisense, Viral replication, RNA interference, Nucleic Acids, Nucleic acid, HIV-1, Molecular Medicine, Humans, Systematic evolution of ligands by exponential enrichment

Abstract

The development of resistance and the inability of currently approved antiretroviral drugs to completely eradicate HIV-1 have led to increased focus on therapies other than small molecules. Although nucleic acid-based intervention requires complex tasks involving intracellular delivery and/or stable expression in target cells, recent advances in gene therapy methods combined with continued progress in stem cell approaches have made nucleic acid-based compounds excellent candidates for effectively inhibiting intracellular targets. Consequently, multiple nucleic acid-based therapies are being developed. These include antisense nucleic acids, peptide nucleic acids and RNA decoys, which can interfere with HIV-1 replication. More recently, RNA interference, which exploits a novel cellular pathway, has been shown to effectively reduce viral titers in cell culture and promises to be a potential candidate for suppressing HIV replication in vivo. A promising candidate in the midst of these emerging approaches is the aptamer approach, which involves the use of a class of small nucleic acid molecules isolated from combinatorial libraries by an in vitro evolution protocol termed SELEX. Aptamers exhibit exquisite specificity, high affinity and the virtual lack of immunogenicity, features that make them exceptionally well-suited to combat HIV without affecting the host. The powerful nature of these specific antagonists of protein function could lead to the development of an effective anti-HIV therapy. Several highly specific, nucleic acid aptamers targeting select HIV proteins have been described. Investigations with anti-HIV RNA aptamers have shown an effective block to viral replication. This review summarizes the existing nucleic-acid based approaches to block HIV replication and attempts to chart the current progress in the development of aptamers against HIV, their use in inhibiting the virus replication, prospects for their use in the clinic and potential drawbacks.

Published

2004

65. Potent Inhibition of Human Immunodeficiency Virus Type 1 Replication by Template Analog Reverse Transcriptase Inhibitors Derived by SELEX (Systematic Evolution of Ligands by Exponential Enrichment)

Author

Vinayaka R. Prasad and Pheroze Joshi

Subjects

Anti-HIV Agents, Aptamer, Immunology, Ligands, Virus Replication, Microbiology, Cell Line, Jurkat Cells, Virology, Vaccines and Antiviral Agents, Humans, Viral Reverse Transcription, Binding Sites, biology, Ribozyme, Virion, RNA, Templates, Genetic, Molecular biology, Reverse transcriptase, HIV Reverse Transcriptase, Viral replication, Insect Science, biology.protein, HIV-1, Nucleic Acid Conformation, Reverse Transcriptase Inhibitors, Primer (molecular biology), Systematic evolution of ligands by exponential enrichment, HeLa Cells

Abstract

RNA aptamers derived by SELEX (systematic evolution of ligands by exponential enrichment) and specific for human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT) bind at the template-primer cleft with high affinity and inhibit its activity. In order to determine the potential of such template analog RT inhibitors (TRTIs) to inhibit HIV-1 replication, 10 aptamers were expressed with flanking, self-cleaving ribozymes to generate aptamer RNA transcripts with minimal flanking sequences. From these, six aptamers (70.8,13, 70.15, 80.55,65, 70.28, 70.28t34, and 1.1) were selected based on binding constants (K d ) and the degree of inhibition of RT in vitro (50% inhibitory concentration [IC 50 ]). These six aptamers were each stably expressed in 293T cells followed by transfection of a molecular clone of HIV R3B . Analysis of the virion particles revealed that the aptamers were encapsidated into the virions released and that the packaging of the viral genomic RNA or the cognate primer, tRNA3Lys, was apparently unaffected. Infectivity of virions produced from 293T cell lines expressing the aptamers, as measured by infecting LuSIV reporter cells, was reduced by 90 to 99.5% compared to virions released from cells not expressing any aptamers. PCR analysis of newly made viral DNA upon infection with virions containing any of the three aptamers with the strongest binding affinities (70.8,13, 70.15, and 80.55,65) showed that all three were able to form the minus-strand strong-stop DNA. However, virions with the aptamers 70.8 and 70.15 were defective for first-strand transfer, suggesting an early block in viral reverse transcription. Jurkat T cells expressing each of the three aptamers, when infected with HIV R3B , completely blocked the spread of HIV in culture. We found that the replication of nucleoside analog RT inhibitor-, nonnucleoside analog RT inhibitor-, and protease inhibitor-resistant viruses was strongly suppressed by the three aptamers. In addition, some of the HIV subtypes were severely inhibited (subtypes A, B, D, E, and F), while others were either moderately inhibited (subtypes C and O) or were naturally resistant to inhibition (chimeric A/D subtype). As virion-encapsidated TRTIs can predispose virions for inhibition immediately upon entry, they should prove to be efficacious agents in gene therapy approaches for AIDS.

Published

2002

66. Mutations That Confer Resistance to Template-Analog Inhibitors of Human Immunodeficiency Virus (HIV) Type 1 Reverse Transcriptase Lead to Severe Defects in HIV Replication

Author

Vinayaka R. Prasad, Pheroze Joshi, and Timothy S. Fisher

Subjects

Anti-HIV Agents, Immunology, Mutant, HIV Infections, Drug resistance, Biology, medicine.disease_cause, Ligands, Virus Replication, Microbiology, chemistry.chemical_compound, Virology, Vaccines and Antiviral Agents, Drug Resistance, Viral, medicine, Humans, Mutation, Processivity, Templates, Genetic, Resistance mutation, Molecular biology, Reverse transcriptase, HIV Reverse Transcriptase, Viral replication, chemistry, Insect Science, DNA, Viral, HIV-1, Reverse Transcriptase Inhibitors, DNA

Abstract

We isolated two template analog reverse transcriptase (RT) inhibitor-resistant mutants of human immunodeficiency virus (HIV) type 1 RT by using the DNA aptamer, RT1t49. The mutations associated, N255D or N265D, displayed low-level resistance to RT1t49, while high-level resistance could be observed when both mutations were present (Dbl). Molecular clones of HIV that contained the mutations produced replication-defective virions. All three RT mutants displayed severe processivity defects. Thus, while biochemical resistance to the DNA aptamer RT1t49 can be generated in vitro via multiple mutations, the overlap between the aptamer- and template-primer-binding pockets favors mutations that also affect the RT-template-primer interaction. Therefore, viruses with such mutations are replication defective. Potent inhibition and a built-in mechanism to render aptamer-resistant viruses replication defective make this an attractive class of inhibitors.

Published

2002

67. The effect of increased processivity on overall fidelity of human immunodeficiency virus type 1 reverse transcriptase

Author

Vinayaka R. Prasad, Yvonne Kew, and Lisa F. Rezende

Subjects

Mutation rate, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Mutant, DNA Mutational Analysis, Molecular Sequence Data, Context (language use), Biology, Frameshift mutation, Point Mutation, Pharmacology (medical), Mutation frequency, Frameshift Mutation, Molecular Biology, Polymerase, Base Sequence, Biochemistry (medical), Cell Biology, General Medicine, Processivity, Templates, Genetic, Virology, Molecular biology, Reverse transcriptase, HIV Reverse Transcriptase, Recombinant Proteins, Protein Structure, Tertiary, Kinetics, Mutagenesis, DNA, Viral, biology.protein, HIV-1

Abstract

We previously reported that two insertions of 15 amino acids in the beta3-beta4 hairpin loop of fingers subdomain of HIV-1(NL4-3) RT confer an increased polymerase processivity. The processivity of human immunodeficiency virus (HIV) reverse transcriptase (RT) is thought to influence the fidelity of HIV-1 RT, which tends to create errors at template sites with high termination probability. Employing the two insertion variants of HIV-1 RT (FE20 and FE103), we examined the relationship between processivity, overall fidelity and error specificity. Although the overall mutation rate was unaffected by increased processivity, one of the mutants, FE103, generated significantly fewer frameshift errors. The other mutant, FE20, generated errors at hotspots not previously observed for HIV-1 RT. Our results indicate that an increase in the polymerase processivity of HIV-1 RT does not necessarily result in a decreased mutation rate and confirm that changes in processivity alter the sequence context in which the errors are made. Furthermore, our results also reveal that the mutation frequency obtained via in vitro gap-filling reactions with wild-type HIV-1(NL4-3) RT is only 2-fold higher than that obtained via a single cycle infection assay using the same, wild-type HIV-1(NL4-3) RT sequence as part of the helper pol function [Mansky and Temin: J Virol 69:5087-5094;1995].

Published

2001

68. Differential influence of nucleoside analog-resistance mutations K65R and L74V on the overall mutation rate and error specificity of human immunodeficiency virus type 1 reverse transcriptase

Author

Hiroaki Mitsuya, Michael A. Parniak, Monica E. Hamburgh, John G. Arnez, Falguni S. Shah, Vinayaka R. Prasad, and Kenneth Curr

Subjects

Models, Molecular, Mutation rate, Anti-HIV Agents, viruses, Mutant, Molecular Sequence Data, Biology, Biochemistry, medicine, Ternary complex, Molecular Biology, Nucleoside analogue, Base Sequence, Nucleic acid sequence, Drug Resistance, Microbial, Cell Biology, biochemical phenomena, metabolism, and nutrition, Virology, Molecular biology, Reverse transcriptase, In vitro, HIV Reverse Transcriptase, DNA, Viral, Mutation, Reverse Transcriptase Inhibitors, Nucleoside, medicine.drug

Abstract

Human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT) variants with the K65R or L74V substitution display resistance to several nucleoside analogs. An in vitro dNTP exclusion assay revealed an increased fidelity for K65R RT compared with wild-type RT, but little change for L74V RT. When the forward mutation rates were measured via a gap-filling assay, the K65R variant displayed an 8-fold decrease in the overall mutation rate (1.0 x 10(-3) versus 8.6 x 10(-3) for wild-type HIV-1 RT), whereas the rate for the L74V variant was closer to that for wild-type RT (5.0 x 10(-3)). The increase in overall fidelity observed for K65R RT is the largest reported for any drug-resistant HIV-1 RT variant. Nucleotide sequence analysis of lacZalpha mutants generated by variant RTs indicated that K65R RT displays uniform reduction in most types of errors, whereas L74V RT does not. Modeling the substitutions into the x-ray structure of the ternary complex revealed that the major influence of Leu(74) in stabilizing the templating base is unaffected by Val substitution, whereas the K65R substitution appears to increase the stringency of dNTP binding. It is speculated that the increased fidelity of K65R RT is due to an altered interaction with the dNTP substrate.

Published

2000

69. The ankyrin repeat-containing adaptor protein Tvl-1 is a novel substrate and regulator of Raf-1

Author

Roger Brent, Antonios M. Makris, Christine McMahon, Erica A. Golemis, Susan E. Bear, Vinayaka R. Prasad, Jun Hsiang Lin, Philip N. Tsichlis, and Christos Patriotis

Subjects

cDNA library, Molecular Sequence Data, Signal transducing adaptor protein, Cell Biology, Transfection, Biology, Biochemistry, Molecular biology, Cell biology, Ankyrin Repeat, Substrate Specificity, DNA-Binding Proteins, Proto-Oncogene Proteins c-raf, Cytoplasm, ANK1, Animals, Ankyrin repeat, Amino Acid Sequence, Nuclear protein, Carrier Proteins, Molecular Biology, Cells, Cultured, Proto-oncogene tyrosine-protein kinase Src, Adaptor Proteins, Signal Transducing, Transcription Factors

Abstract

Tvl-1 is a 269-amino acid ankyrin repeat protein expressed primarily in thymus, lung, and testes that was identified by screening a murine T-cell two-hybrid cDNA library for proteins that associate with the serine-threonine kinase Raf-1. The interaction of Tvl-1 with Raf-1 was confirmed by co-immunoprecipitation of the two proteins from COS-1 cells transiently transfected with Tvl-1 and Raf-1 expression constructs as well as by co-immunoprecipitation of the endogenous proteins from CV-1 and NB2 cells. Tvl-1 interacts with Raf-1 via its carboxyl-terminal ankyrin repeat domain. The same domain also mediates Tvl-1 homodimerization. Tvl-1 was detected by immunofluorescence in both the cytoplasm and the nucleus suggesting that in addition to Raf-1 it may also interact with nuclear proteins. Activated Raf-1 phosphorylates Tvl-1 both in vitro and in vivo. In baculovirus-infected Sf9 insect cells, Tvl-1 potentiates the activation of Raf-1 by Src and Ras while in COS-1 cells it potentiates the activation of Raf-1 by EGF. These data suggest that Tvl-1 is both a target as well as a regulator of Raf-1. The human homologue of Tvl-1 maps to chromosome 19p12, upstream of MEF2B with the two genes in a head to head arrangement.

Published

1999

70. Long-Term Amerlioration of Bilirubin Glucuronidation Defect in Gunn Rats by Transplanting Genetically Modified Immortalized Autologous Hepatocytes

Author

Jayanta Roy-Chowdhury, P Manchikalapudi, P van Duijvendijk, Namita Roy-Chowdhury, Vinayaka R. Prasad, Piter J. Bosma, Kouji Tada, B H Kim, I J Fox, and Other departments

Subjects

0301 basic medicine, SV40 large T antigen, Cell Transplantation, Bilirubin, medicine.medical_treatment, Rats, Gunn, Biomedical Engineering, Glucuronidation, Clone (cell biology), lcsh:Medicine, Simian virus 40, Biology, Liver transplantation, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Antigen, medicine, Animals, Humans, Glucuronosyltransferase, Antigens, Viral, Tumor, Cells, Cultured, Transplantation, lcsh:R, Gene Transfer Techniques, Genetic Therapy, Cell Biology, Cell Transformation, Viral, Virology, Molecular biology, Liver Transplantation, Rats, 030104 developmental biology, Liver, chemistry, Immortalised cell line, 030217 neurology & neurosurgery

Abstract

Ex vivo gene therapy, in which hepatocytes are harvested from mutants, retrovirally transduced with a normal gene and transplanted back into the donor, has been used for correction of inherited metabolic defects of liver. Major drawbacks of this method include limited availability of autologous hepatocytes, inefficient retroviral transduction of primary hepatocytes, and the limited number of hepatocytes that can be transplanted safely. To obviate these problems, we transduced primary hepatocytes derived from inbred bilirubin–UDP–glucuronosyl–transferase (BUGT)-deficient Gunn rats by infection with a recombinant retrovirus expressing temperature-sensitive mutant SV40 large T antigen (tsT). The immortalized cells were then transduced with a second recombinant retrovirus expressing human B-UGT, and a clone expressing high levels of the enzyme was expanded by culturing at permissive temperature (33°C). At 37°C, tsT antigen was degraded and the cells expressed UGT activity toward bilirubin at a level approximately twice that present in normal rat liver homogenates. For seeding the cells into the liver bed, 1 × 107 cells were injected into the spleens of syngeneic Gunn rats five times at 10-day intervals. Excretion of bilirubin glucuronides in bile was demonstrated by HPLC analysis and serum bilirubin levels were reduced by 27 to 52% in 40 days after the first transplantation and remained so throughout the duration of the study (120 days). None of the transplanted Gunn rats or SCID mice transplanted with the immortalized cells developed tumors. © 1998 Elsevier Science Inc.

Published

1998

71. Virtues of being faithful: can we limit the genetic variation in human immunodeficiency virus?

Author

Vinayaka R. Prasad, Mark A. Wainberg, Lisa F. Rezende, and William C. Drosopoulos

Subjects

Genetics, Innate immune system, Genetic Variation, Drug Resistance, Microbial, Biology, medicine.disease, biology.organism_classification, Virology, Reverse transcriptase, Virus, HIV Reverse Transcriptase, Immune system, Acquired immunodeficiency syndrome (AIDS), Viral replication, Drug Discovery, Lentivirus, medicine, HIV-1, Molecular Medicine, Humans, Viral disease, Genetics (clinical)

Abstract

Human immunodeficiency virus (HIV) infections are characterized by a high degree of viral variation. The genetic variation is thought to be a combined effect of a high error rate of reverse transcriptase (RT), viral genomic recombination, the selection forces of the human immune system, the requirement for growth in multiple cell types during pathogenesis, and persistent immune activation associated with HIV disease. This hypermutability gives the virus an ability to escape mechanisms of innate immune surveillance and therapeutic interventions. Indeed, HIV variants that are resistant to drugs that antagonize both the HIV protease and RT enzymes are well described. Furthermore, there are seemingly no procedures to restrict this disarming property of HIV to mutate rapidly. Recently we have shown that some of the drug-resistant RTs display an increased in vitro polymerase fidelity. The question is whether this finding will stimulate new approaches that will not only help the immune system to deal with the virus more efficiently but also to reduce or delay resistance to various classes of anti-HIV drugs. The pros and cons of this concept and the influence of viral replication rates and viral fitness on HIV variability are discussed.

Published

1998

72. Effects of mutations in Pr160gag-pol upon tRNA(Lys3) and Pr160gag-plo incorporation into HIV-1

Author

Vinayaka R. Prasad, Israel Lowy, Yue Huang, Lawrence Kleiman, Michael A. Parniak, Johnson Mak, Qun Cao, Ahmad Khorchid, and Mark A. Wainberg

Subjects

viruses, Mutant, Molecular Sequence Data, Gene Products, gag, Gene Products, pol, RNA, Transfer, Amino Acyl, gag Gene Products, Human Immunodeficiency Virus, Structural Biology, Animals, Humans, Protein Precursors, RNase H, Molecular Biology, chemistry.chemical_classification, Binding Sites, biology, Base Sequence, Hybridization probe, Virus Assembly, Molecular biology, Reverse transcriptase, HIV Reverse Transcriptase, Amino acid, Integrase, chemistry, Mutagenesis, pol Gene Products, Human Immunodeficiency Virus, Transfer RNA, COS Cells, biology.protein, HIV-1, Primer (molecular biology), Protein Processing, Post-Translational

Abstract

During HIV-1 viral assembly, both Pr160 gag-pol and primer tRNA Lys3 are packaged into the virus. tRNA Lys packaging (both tRNA Lys3 and tRNA Lys1,2 ) is dependent upon the presence of RT sequences within Pr160 gag-pol . In this work, we have monitored the effect of Pr160 gag-pol mutations upon incorporation of tRNA Lys3 and Pr160 gag-pol into HIV-1 produced from COS-7 cells transfected with mutant HIV-1 proviral DNAs. Mutations include carboxy deletions of Pr160 gag-pol and small amino acid insertions and replacements within the various functional domains of the reverse transcriptase (RT). tRNA Lys3 incorporation was monitored both by 2D PAGE of viral RNA, and by hybridization with tRNA Lys3 -specific DNA probes. Our data indicates: (1) deletion of integrase sequence has a moderate effect upon select tRNA Lys3 packaging, while carboxy terminal deletions extending further into the RNase H and connection domains more strongly reduce viral tRNA Lys3 content; (2) tRNA Lys3 incorporation is strongly reduced by small inframe amino acid insertions or replacements in the carboxy region of the thumb domain and the amino half of the connection domain of RT, but tRNA Lys3 incorporation is altered little, or not at all, by similar amino acid insertional mutations within other RT domains, such as the fingers, palm, RNase H, the amino portion of the thumb, and the carboxy region of the connection domain. The inability of connection domain mutant virus to incorporate tRNA Lys3 and to properly process precursor proteins in the virus is due to the inability of mutant Pr160 gag-pol to be incorporated into the virus. These mutant precursor proteins are maintained at levels in the cytoplasm similar to wild-type.

Published

1997

73. Clade C HIV-1 isolates circulating in Southern Africa exhibit a greater frequency of dicysteine motif-containing Tat variants than those in Southeast Asia and cause increased neurovirulence

Author

Ujjwal Neogi, Vinayaka R. Prasad, John A. Joska, Mustafizur Rahman, Tasnim Azim, Udaykumar Ranga, Ruth M. Ruprecht, Charles E. Wood, Heather A. Bimonte-Nelson, Sandra Gonzalez-Ramirez, Anita Shet, Eliseo A. Eugenin, William R. Tyor, Joshua S. Talboom, Anjali Verma, Vasudev R. Rao, Cari Fritz-French, Ligia Padilla, Department of Psychiatry and Mental Health, and Faculty of Health Sciences

Subjects

Adult, Male, Clade C HIV-1, AIDS Dementia Complex, Monocyte chemotaxis, HIV dementia, Genotype, SCID-HIVE mouse model, Molecular Sequence Data, HIV Infections, Biology, Southeast asian, Africa, Southern, Southeast asia, 03 medical and health sciences, Mice, 0302 clinical medicine, Virology, Prevalence, Animals, Humans, HIV-1 Tat, Clade, Gene, Asia, Southeastern, 030304 developmental biology, Subtype C HIV-1, 0303 health sciences, Phylogenetic tree, Research, HIV-1 Tat C31S polymorphism, Neuroaids, virus diseases, Sequence Analysis, DNA, Middle Aged, 3. Good health, Infectious Diseases, Tat dicysteine, biology.protein, HIV-1, Neuropathogenesis, Female, tat Gene Products, Human Immunodeficiency Virus, Antibody, 030217 neurology & neurosurgery

Abstract

Background HIV-1 Clade C (Subtype C; HIV-1C) is responsible for greater than 50% of infections worldwide. Unlike clade B HIV-1 (Subtype B; HIV-1B), which is known to cause HIV associated dementia (HAD) in approximately 15% to 30% of the infected individuals, HIV-1C has been linked with lower prevalence of HAD (0 to 6%) in India and Ethiopia. However, recent studies report a higher prevalence of HAD in South Africa, Zambia and Botswana, where HIV-1C infections predominate. Therefore, we examined whether Southern African HIV-1C is genetically distinct and investigated its neurovirulence. HIV-1 Tat protein is a viral determinant of neurocognitive dysfunction. Therefore, we focused our study on the variations seen in tat gene and its contribution to HIV associated neuropathogenesis. Results A phylogenetic analysis of tat sequences of Southern African (South Africa and Zambia) HIV isolates with those from the geographically distant Southeast Asian (India and Bangladesh) isolates revealed that Southern African tat sequences are distinct from Southeast Asian isolates. The proportion of HIV − 1C variants with an intact dicysteine motif in Tat protein (C30C31) was significantly higher in the Southern African countries compared to Southeast Asia and broadly paralleled the high incidence of HAD in these countries. Neuropathogenic potential of a Southern African HIV-1C isolate (from Zambia; HIV-1C1084i), a HIV-1C isolate (HIV-1IndieC1) from Southeast Asia and a HIV-1B isolate (HIV-1ADA) from the US were tested using in vitro assays to measure neurovirulence and a SCID mouse HIV encephalitis model to measure cognitive deficits. In vitro assays revealed that the Southern African isolate, HIV-1C1084i exhibited increased monocyte chemotaxis and greater neurotoxicity compared to Southeast Asian HIV-1C. In neurocognitive tests, SCID mice injected with MDM infected with Southern African HIV-1C1084i showed greater cognitive dysfunction similar to HIV-1B but much higher than those exposed to Southeast Asian HIV − 1C. Conclusions We report here, for the first time, that HIV-1C from Southern African countries is genetically distinct from Southeast Asian HIV-1C and that it exhibits a high frequency of variants with dicysteine motif in a key neurotoxic HIV protein, Tat. Our results indicate that Tat dicysteine motif determines neurovirulence. If confirmed in population studies, it may be possible to predict neurocognitive outcomes of individuals infected with HIV-1C by genotyping Tat.

Published

2013

74. Perspective: research highlights at the Albert Einstein College of Medicine Center for AIDS research. Approaches to control drug resistance in HIV: the role of increased polymerase fidelity

Author

Monica E. Hamburgh, Vinayaka R. Prasad, and William C. Drosopoulos

Subjects

medicine.medical_specialty, media_common.quotation_subject, Immunology, Human immunodeficiency virus (HIV), Fidelity, Drug resistance, Biology, medicine.disease_cause, symbols.namesake, Acquired immunodeficiency syndrome (AIDS), Virology, medicine, Animals, Humans, Einstein, media_common, Acquired Immunodeficiency Syndrome, Perspective (graphical), Drug Resistance, Microbial, RNA-Directed DNA Polymerase, medicine.disease, Negative therapeutic reaction, Infectious Diseases, Mutagenesis, Family medicine, Drug Design, symbols, HIV-1, Reverse Transcriptase Inhibitors, Drug Therapy, Combination

Published

1996

75. The nucleoside analog-resistant E89G mutant of human immunodeficiency virus type 1 reverse transcriptase displays a broader cross-resistance that extends to nonnucleoside inhibitors

Author

Yvonne Kew, Laurence R. Olsen, Vinayaka R. Prasad, Mark A. Wainberg, and Horacio Salomón

Subjects

Pharmacology, Nevirapine, Anti-HIV Agents, Mutant, Drug Resistance, Microbial, Nucleosides, Biology, Nucleotidyltransferase, Virology, Reverse transcriptase, Virus, HIV Reverse Transcriptase, Infectious Diseases, Viral replication, Mutation, medicine, HIV-1, Delavirdine, Pharmacology (medical), Enzyme Inhibitors, Nucleoside, medicine.drug, Research Article

Abstract

The alteration of a glutamic acid (E) to a glycine (G) amino acid residue at position 89 (E89G alteration) in the human immunodeficiency virus type 1 reverse transcriptase confers decreased susceptibility to several nucleoside analog inhibitors. Because the nonnucleoside inhibitor-binding pocket is adjacent to the deoxynucleoside triphosphate substrate-binding site, the impact of the E89G reverse transcriptase has decreased susceptibility to TIBO R82150, nevirapine, and to a lesser extent, delavirdine. Human immunodeficiency viruses bearing the same mutation displayed decreased susceptibility to inhibition by these compounds in a cell culture virus replication assay.

Published

1996

76. Use of chimeric human immunodeficiency virus types 1 and 2 reverse transcriptases for structure-function analysis and for mapping susceptibility to nonnucleoside inhibitors

Author

Vinayaka R. Prasad, Macarthur Charles, William C. Drosopoulos, Edward Arnold, Guozhe Yang, and Qingbin Song

Subjects

DNA polymerase, Protein Conformation, Recombinant Fusion Proteins, Immunology, Molecular Sequence Data, Mutagenesis (molecular biology technique), Context (language use), Virus, Benzodiazepines, Structure-Activity Relationship, Virology, Immunology and Allergy, Humans, Amino Acids, Polymerase, chemistry.chemical_classification, biology, Base Sequence, RNA-Directed DNA Polymerase, Imidazoles, virus diseases, Nucleotidyltransferase, HIV Reverse Transcriptase, Enzyme, chemistry, HIV-2, biology.protein, HIV-1, Mutagenesis, Site-Directed, Reverse Transcriptase Inhibitors

Abstract

The human immunodeficiency virus type 1 and type 2 (HIV-1 and HIV-2) reverse transcriptases (RTs) are evolutionary related. To study the effect of homologous sequence replacements on polymerase function and to map the determinants of the lack of susceptibility of HIV-2 RT to nonnucleoside drugs, a series of chimeric HIV-1/HIV-2 RTs were constructed. Analysis of the chimeric RTs showed that wild-type levels of RNA-dependent DNA polymerase activity were retained when both finger and palm subdomains were exchanged as a unit between the two parental RTs. Analysis of enzymatically active chimeras for inhibition by the thiobenzimidazolone derivative TIBO R82150 showed that a segment of HIV-2 RT at 212-250, when placed in the HIV-1 RT context, conferred a 40-fold decrease in susceptibility to TIBO R82150. Site-directed mutagenesis of this segment found Tyr227 to be a key residue in this segment for the natural resistance of HIV-2 RT to TIBO R82150.

Published

1996

77. Isolation and characterization of a dideoxyguanosine triphosphate-resistant mutant of human immunodeficiency virus reverse transcriptase

Author

T de los Santos, I Lowy, S P Goff, L Chiang, and Vinayaka R. Prasad

Subjects

HIV antibodies--Testing, Immunology, Mutant, Deoxyribonucleotides, Mutagenesis (molecular biology technique), Drug resistance, Biology, Virus Replication, Antiviral Agents, Virus, Cell Line, Guanosine triphosphatase, Humans, Cloning, Molecular, Multidisciplinary, HIV (Viruses), FOS: Clinical medicine, Point mutation, Deoxyguanine Nucleotides, Drug Resistance, Microbial, RNA-Directed DNA Polymerase, Resistance mutation, Virology, Reverse transcriptase, Recombinant Proteins, Kinetics, Viral replication, Mutagenesis, HIV-1, Dideoxynucleotides, Plasmids, Research Article

Abstract

The appearance of drug-resistant strains of viral pathogens is a major difficulty confounding current efforts to block viral infections. The identification and analysis of mutations responsible for drug resistance can provide important clues helpful in understanding the mechanisms of resistance and in the eventual development of better therapies. We have used a direct screening method to scan libraries of mutagenized genes encoding the reverse transcriptase of human immunodeficiency virus type 1, and have recovered a variant enzyme that is resistant to the chain-terminator inhibitor 2',3'-dideoxyguanosine triphosphate. The single substitution mutation in this variant conferred broad crossresistance to a variety of other antiviral compounds currently in clinical trials. Virus carrying the mutation was fully infectious in cultured human lymphocytes. The replication of the mutant virus was highly resistant to phosphonoformic acid but did not show increased resistance to the prodrug dideoxyguanosine.

Published

1991

78. [28] Linker insertion mutagenesis as probe of structure-function relationships

Author

Stephen P. Goff and Vinayaka R. Prasad

Subjects

Genetics, chemistry.chemical_classification, chemistry.chemical_compound, Enzyme, Biochemistry, chemistry, Linker-Insertion Mutagenesis, Mutation (genetic algorithm), Structure function, Biology, Gene, DNA

Published

1991

79. Utilization of a Deoxynucleoside Diphosphate Substrate by HIV Reverse Transcriptase

Author

Scott J. Garforth, Vinayaka R. Prasad, and Michael A. Parniak

Subjects

Models, Molecular, DNA polymerase, lcsh:Medicine, Catalysis, Substrate Specificity, 03 medical and health sciences, Zidovudine, chemistry.chemical_compound, medicine, lcsh:Science, Biochemistry/Biomacromolecule-Ligand Interactions, Polymerase, Molecular Biology/DNA Replication, 030304 developmental biology, Phosphorolysis, Virology/Antivirals, including Modes of Action and Resistance, Biochemistry/Replication and Repair, 0303 health sciences, Multidisciplinary, biology, DNA synthesis, Lysine, lcsh:R, 030302 biochemistry & molecular biology, Virology/Mechanisms of Resistance and Susceptibility, including Host Genetics, Molecular biology, HIV Reverse Transcriptase, Reverse transcriptase, Protein Structure, Tertiary, 3. Good health, Diphosphates, Amino Acid Substitution, Virology/Viral Replication and Gene Regulation, chemistry, Biochemistry, Virology/Immunodeficiency Viruses, biology.protein, Mutant Proteins, lcsh:Q, Primer (molecular biology), Thymidine, Research Article, medicine.drug

Abstract

Background: Deoxynucleoside triphosphates (dNTPs) are the normal substrates for DNA synthesis catalyzed by polymerases such as HIV-1 reverse transcriptase (RT). However, substantial amounts of deoxynucleoside diphosphates (dNDPs) are also present in the cell. Use of dNDPs in HIV-1 DNA synthesis could have significant implications for the efficacy of nucleoside RT inhibitors such as AZT which are first line therapeutics for treatment of HIV infection. Our earlier work on HIV-1 reverse transcriptase (RT) suggested that the interaction between the c-phosphate of the incoming dNTP and RT residue K65 in the active site is not essential for dNTP insertion, implying that this polymerase may be able to insert dNDPs in addition to dNTPs. Methodology/Principal Findings: We examined the ability of recombinant wild type (wt) and mutant RTs with substitutions at residue K65 to utilize a dNDP substrate in primer extension reactions. We found that wild type HIV-1 RT indeed catalyzes incorporation of dNDP substrates whereas RT with mutations of residue K65 were unable to catalyze this reaction. Wild type HIV-1 RT also catalyzed the reverse reaction, inorganic phosphate-dependent phosphorolysis. Nucleotide-mediated phosphorolytic removal of chain-terminating 39-terminal nucleoside inhibitors such as AZT forms the basis for HIV-1 resistance to such drugs, and this removal is enhanced by thymidine analog mutations (TAMs). We found that both wt and TAM-containing RTs were able to catalyze Pi-mediated phosphorolysis of 39-terminal AZT at physiological levels of Pi with an efficacy similar to that for ATP-dependent AZT-excision. Conclusions: We have identified two new catalytic functions of HIV-1 RT, the use of dNDPs as substrates for DNA synthesis, and the use of Pi as substrate for phosphorolytic removal of primer 39-terminal nucleotides. The ability to insert dNDPs has been documented for only one other DNA polymerase, the RB69 DNA polymerase and the reverse reaction employing inorganic phosphate has not been documented for any DNA polymerase. Importantly, our results show that Pi-mediated phosphorolysis can contribute to AZT resistance and indicates that factors that influence HIV resistance to AZT are more complex than previously appreciated.

Published

2008

80. Expression of enzymatically active reverse transcriptase of simian immunodeficiency virus in bacteria: sensitivity to nucleotide analogue inhibitors

Author

Kyl V. Myrick, William A. Haseltine, Vinayaka R. Prasad, and Stephen P. Goff

Subjects

DNA polymerase, Recombinant Fusion Proteins, Gene Expression, Molecular cloning, medicine.disease_cause, Virus, Virology, Murine leukemia virus, medicine, Escherichia coli, Thymine Nucleotides, chemistry.chemical_classification, Expression vector, biology, RNA-Directed DNA Polymerase, biology.organism_classification, Molecular biology, Reverse transcriptase, Enzyme, chemistry, biology.protein, Reverse Transcriptase Inhibitors, Simian Immunodeficiency Virus, Zidovudine, Dideoxynucleotides

Abstract

A fragment of the SIV mac251 pol gene was expressed in Escherichia coli as a trpE fusion protein. Analysis of extracts from bacteria containing this expression plasmid revealed the presence of a reverse transcriptase activity dependent on Mgt 2+ as divalent cation and active on both poly(rA) · oligo(dT) and poly(rC · oligo(dG) templates. In comparative studies, the SIV and HIV-1 reverse transcriptases expressed in bacteria displayed very similar high sensitivities to the chain terminator inhibitors AZTTP and ddTTP. The reverse transcriptase of Moloney murine leukemia virus and the DNA polymerase of E. coli were both more resistant to ddTTP, and the E. coli enzyme was significantly more resistant to AZTTP.

Published

1990

81. Structure-function studies of HIV reverse transcriptase

Author

Vinayaka R. Prasad and Stephen P. Goff

Subjects

chemistry.chemical_classification, biology, Base Sequence, DNA polymerase, General Neuroscience, Mutant, Molecular Sequence Data, Mutagenesis (molecular biology technique), Drug Resistance, Microbial, RNA-Directed DNA Polymerase, Computational biology, Phenotype, Antiviral Agents, General Biochemistry, Genetics and Molecular Biology, Reverse transcriptase, Structure-Activity Relationship, Enzyme, History and Philosophy of Science, chemistry, Viral replication, biology.protein, HIV-1, Humans, Function (biology)

Abstract

The retroviral RT is properly under intensive study as the major target of antiviral therapy. The enzyme exhibits a number of features that make it an attractive target: it is crucial for viral replication; its RNA-dependent DNA polymerase activity is probably unique to viral replication, or if not unique, is generally unimportant in host cell function; its activities are readily monitored; and powerful lead compounds in the form of nucleotide analogues are already in hand. Our laboratory has been involved in studies to elucidate the structure and function of the HIV-1 RT and to develop a formal genetics of the enzyme. Working with constructs expressing RT in bacteria, we been able to use in vitro mutagenesis to localize functions on the molecule; by coupling mutagenesis with high-throughput screening of colonies, we have been able to isolate mutants with specific, rare, phenotypes. We believe that extensions of these efforts will help us to understand the functions of the protein and, coupled to a detailed three-dimensional structure, should facilitate the development of new and better inhibitors.

Published

1990

82. A Novel in situ Colony Screening Method to Detect Human Immunodeficiency Virus Reverse Transcriptase Activity Expressed in Bacteria

Author

Stephen P. Goff and Vinayaka R. Prasad

Subjects

Mutation, biology, DNA polymerase, RNA-Directed DNA Polymerase, Mutant, Cell Biology, medicine.disease_cause, Biochemistry, Virology, Molecular biology, Reverse transcriptase, law.invention, Restriction map, law, medicine, Recombinant DNA, biology.protein, Molecular Biology, Escherichia coli

Abstract

An in situ screening procedure is described that permits the detection of RNA-dependent DNA polymerase activity in bacterial colonies expressing the reverse transcriptase of the human immunodeficiency virus. The procedure has been applied to the isolation of rare pseudorevertants of an inactive parental mutant.

Published

1989

83. Linker insertion mutagenesis of the human immunodeficiency virus reverse transcriptase expressed in bacteria: definition of the minimal polymerase domain

Author

Stephen P. Goff and Vinayaka R. Prasad

Subjects

Molecular biology, DNA polymerase, Protein subunit, Ribonuclease H, DNA-Directed DNA Polymerase, Insertional mutagenesis, DNA polymerases, Virology, Endoribonucleases, Escherichia coli, Site-directed mutagenesis, RNase H, HIV (Viruses)--Treatment, Polymerase, Multidisciplinary, biology, RNA-Directed DNA Polymerase, HIV, Reverse transcriptase, Gene Expression Regulation, Mutation, biology.protein, Transformation, Bacterial, Research Article, Plasmids

Abstract

A plasmid construct expressing the p66 version of the human immunodeficiency virus reverse transcriptase as a bacterial fusion protein was subjected to in vitro mutagenesis, and the resulting variant proteins were assayed to define the locations of the two major enzymatic activities. The DNA polymerase activity was localized to the N-terminal portion of the protein; mutations altering or eliminating the C-terminal portion had little or no effect on that activity. The results suggest that, in contrast with previous reports, the p51 subunit found in virions should exhibit DNA polymerase activity. Mutations in many parts of the protein eliminated RNase H activity, suggesting that several areas are needed for proper folding and generation of that activity.

Published

1989

84. Purification of a retinol binding protein from the hen-oviduct cytosol and its immunological cross-reactivity with those from the nucleus

Author

Vinayaka R. Prasad, J. Ganguly, and Manchanahalli R. Satyanarayana Rao

Subjects

Immunodiffusion, Biophysics, Antigen-Antibody Complex, Oviducts, Cross Reactions, Biochemistry, Cytosol, Structural Biology, Animals, Vitamin A, Molecular Biology, Conalbumin, Cell Nucleus, Antiserum, biology, Immune Sera, Binding protein, Retinol-Binding Proteins, Cellular, Retinol-Binding Proteins, Ovalbumin, Retinol binding protein, Sephadex, biology.protein, Oviduct, Female, Chickens

Abstract

Cellular retinol-binding protein was purified from the cytosol of the oviducts of laying hens by ammonium sulphate fractionation and chromatography on Sephadex G-75 and DEAE-Sephadex A-50 columns. Analysis of the purified retinol-binding protein on 10% SDS-polyacrylamide gel revealed the presence of a doublet representing very similar molecular sizes. Antiserum was prepared against the purified cellular retinoi-binding protein, and on the basis of (a) immunodiffusion test and (b) immunoneutralization of 3H-labelled retinol-cellular retinol-binding protein complex on a column of Sephadex G-75, the antiserum appeared to be specific. The antiserum showed cross-reactivity with the nucleosol and a 0.4 M NaCl extract of the chromatin of the oviduct nuclei, while it did not react with the major egg-white proteins such as ovalbumin, conalbumin and ovomucoid.

Published

1983

85. Enhanced fidelity of 3TC-selected mutant HIV-1 reverse transcriptase

Author

Vinayaka R. Prasad, Gadi Borkow, Qingbin Song, William C. Drosopoulos, Jayanthi Manne, Sabina A. Islam, Mayla Hsu, Michael A. Parniak, Gino Castriota, Zhengxian Gu, Mark A. Wainberg, and Horacio Salomón

Subjects

Nevirapine, viruses, Deoxyribonucleotides, Molecular Sequence Data, HIV Infections, Drug resistance, Biology, HIV Antibodies, Virus Replication, Antiviral Agents, Virus, Neutralization Tests, medicine, Delavirdine, Humans, Saquinavir, Base Composition, Multidisciplinary, Base Sequence, Zalcitabine, virus diseases, Drug Resistance, Microbial, RNA-Directed DNA Polymerase, HIV Protease Inhibitors, biochemical phenomena, metabolism, and nutrition, Resistance mutation, Isoquinolines, Virology, Molecular biology, Reverse transcriptase, HIV Reverse Transcriptase, Lamivudine, Mutation, HIV-1, Quinolines, Reverse Transcriptase Inhibitors, Viral load, medicine.drug

Abstract

Monotherapy with (−)2′,3′-dideoxy-3′-thiacytidine (3TC) leads to the appearance of a drug-resistant variant of human immunodeficiency virus-type 1 (HIV-1) with the methionine-184 → valine (M184V) substitution in the reverse transcriptase (RT). Despite resulting drug resistance, treatment for more than 48 weeks is associated with a lower plasma viral burden than that at baseline. Studies to investigate this apparent contradiction revealed the following. (i) Titers of HIV-neutralizing antibodies remained stable in 3TC-treated individuals in contrast to rapid declines in those treated with azidothymidine (AZT). (ii) Unlike wild-type HIV, growth of M184V HIV in cell culture in the presence of d4T, AZT, Nevirapine, Delavirdine, or Saquinavir did not select for variants displaying drug resistance. (iii) There was an increase in fidelity of nucleotide insertion by the M184V mutant compared with wild-type enzyme.

86. Multivariable analysis to determine if HIV-1 Tat dicysteine motif is associated with neurodevelopmental delay in HIV-infected children in Malawi

Author

Anna Dow, Annelies Van Rie, Jasmeen Dara, Elizabeth A. Cromwell, Christa Buckheit Sturdevant, Macpherson Mallewa, Vinayaka R. Prasad, and Ronald Swanstrom

Subjects

Male, Malawi, Pediatrics, medicine.medical_specialty, Genotype, Cross-sectional study, Developmental Disabilities, Cognitive Neuroscience, Neurodevelopment, Amino Acid Motifs, Dicysteine motif, HIV Infections, Neuropathology, Encephalopathy, Bayley Scales of Infant Development, 03 medical and health sciences, Behavioral Neuroscience, 0302 clinical medicine, Internal medicine, medicine, Humans, HIV-1 subtype C, Genotyping, Biological Psychiatry, 030304 developmental biology, 0303 health sciences, business.industry, Research, Infant, General Medicine, Viral Load, 3. Good health, Cross-Sectional Studies, Cohort, HIV-1, Female, tat Gene Products, Human Immunodeficiency Virus, Tat, business, Viral load, Neurocognitive, 030217 neurology & neurosurgery

Abstract

Background HIV-1 Tat protein is implicated in HIV-neuropathogenesis. Tat C31S polymorphism (TatCS) has been associated with milder neuropathology in vitro and in animal models but this has not been addressed in a cohort of HIV-infected adults or children. Methods HIV viral load (VL) in plasma and cerebrospinal fluid (CSF) were determined and plasma HIV tat gene was sequenced. Neurodevelopmental assessment was performed using Bayley Scales of Infant Development III (BSID-III), with scores standardized to Malawian norms. The association between TatCS and BSID-III scores was evaluated using multivariate linear regression. Results Neurodevelopmental assessment and HIV tat genotyping were available for 33 children. Mean age was 19.4 (SD 7.1) months, mean log VL was 5.9 copies/mL (SD 0.1) in plasma and 3.9 copies/mL (SD 0.9) in CSF. The prevalence of TatCC was 27 %. Z-scores for BSID-III subtests ranged from −1.3 to −3.9. TatCC was not associated with higher BSID-III z-scores. Conclusions The hypothesis of milder neuropathology in individuals infected with HIV TatCS was not confirmed in this small cohort of Malawian children. Future studies of tat genotype and neurocognitive disorder should be performed using larger sample sizes and investigate if this finding is due to differences in HIV neuropathogenesis between children and adults.

87. Splice acceptor site for the env message of Moloney murine leukemia virus

Author

Vinayaka R. Prasad, Philip N. Tsichlis, and Pedro A. Lazo

Subjects

Genes, Viral, RNA Splicing, Immunology, Clone (cell biology), Microbiology, Genome, Viral Envelope Proteins, Virology, Complementary DNA, Murine leukemia virus, splice, RNA, Messenger, Base Sequence, biology, Intron, DNA, biology.organism_classification, Molecular biology, Restriction site, Genes, Insect Science, DNA, Viral, RNA splicing, RNA, Viral, Moloney murine leukemia virus, Research Article

Abstract

We report the isolation and sequence of a cDNA clone containing part of the env message of the Moloney murine leukemia virus (MoMuLV). This clone was derived from a rat thymic lymphoma induced by MoMuLV. The AG acceptor site employed in this message is located at position 5490 in the MoMuLV genome. This splice site is detectable at the cDNA level by the creation of a novel SacI restriction site not present in the viral genome. In the -1 to -40 region, this AG acceptor site is preceded by four conserved heptanucleotides (PyXPyTPuAPy) that may function as acceptors for removal of the 5' end of the intron.

88. Viral and cellular factors underlying neuropathogenesis in HIV associated neurocognitive disorders (HAND)

Author

Vinayaka R. Prasad, Arthur P Ruiz, and Vasudev R. Rao

Subjects

0303 health sciences, Chemokine, Cell type, biology, Microglia, business.industry, Review, Blood–brain barrier, Phenotype, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Immune system, Virology, Immunology, biology.protein, Medicine, Molecular Medicine, Pharmacology (medical), Neuropathogenesis, business, Neurocognitive, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

As the HIV-1 epidemic enters its fourth decade, HIV-1 associated neurological disorders (HAND) continue to be a major concern in the infected population, despite the widespread use of anti-retroviral therapy. Advancing age and increased life expectancy of the HIV-1 infected population have been shown to increase the risk of cognitive dysfunction. Over the past 10 years, there has been a significant progress in our understanding of the mechanisms and the risk factors involved in the development of HAND. Key events that lead up to neuronal damage in HIV-1 infected individuals can be categorized based on the interaction of HIV-1 with the various cell types, including but not limited to macrophages, brain endothelial cells, microglia, astrocytes and the neurons. This review attempts to decipher these interactions, beginning with HIV-1 infection of macrophages and ultimately resulting in the release of neurotoxic viral and host products. These include: interaction with endothelial cells, resulting in the impairment of the blood brain barrier; interaction with the astrocytes, leading to metabolic and neurotransmitter imbalance; interactions with resident immune cells in the brain, leading to release of toxic cytokines and chemokines. We also review the mechanisms underlying neuronal damage caused by the factors mentioned above. We have attempted to bring together recent findings in these areas to help appreciate the viral and host factors that bring about neurological dysfunction. In addition, we review host factors and viral genotypic differences that affect phenotypic pathological outcomes, as well as recent advances in treatment options to specifically address the neurotoxic mechanisms in play.

89. Exceptional molecular and coreceptor-requirement properties of molecular clones isolated from an Human Immunodeficiency Virus Type-1 subtype C infection

Author

Udaykumar Ranga, Vinayaka R. Prasad, Padmanabhan Roshan, Aruna V Mahendarkar, Susarla K. Shankar, Prasanta K. Dash, Anita Mahadevan, Parthasarathy Satishchandra, Krishnamurthy Kumar Anand, Nagadenahalli B. Siddappa, and Asokan Mangaiarkarasi

Subjects

Adult, Male, lcsh:Immunologic diseases. Allergy, AIDS Dementia Complex, Receptors, CCR5, Sequence analysis, T-Lymphocytes, viruses, HIV Enhancer, Virus, Cell Line, 03 medical and health sciences, Receptors, HIV, Proviruses, Phylogenetics, Virology, HIV Seropositivity, Humans, Cloning, Molecular, Phylogeny, 030304 developmental biology, HIV Long Terminal Repeat, Genetics, 0303 health sciences, biology, 030306 microbiology, Research, env Gene Products, Human Immunodeficiency Virus, Genetic Variation, rev Gene Products, Human Immunodeficiency Virus, Reverse transcriptase, 3. Good health, Infectious Diseases, Cell culture, biology.protein, HIV-1, Leukocytes, Mononuclear, Antibody, lcsh:RC581-607, Sequence Analysis

Abstract

Background The pathogenic significance of coreceptor switch in the viral infection of HIV-1 is not completely understood. This situation is more complex in subtype C infection where coreceptor switch is either absent or extremely rare. To gain insights into the mechanisms that underlie coreceptor requirement of subtype C, we screened several primary viral isolates and identified a clinical sample that demonstrated a potential to grow on standard T-cell lines with no detectable CCR5 expression. The subject was diagnosed with HIV-1 associated dementia in the absence of opportunistic infections of the brain. To isolate molecular clones from this virus, we devised a novel strategy based on anchor primers that target a sequence in the reverse transcriptase, highly conserved among diverse subtypes of HIV-1. Results Using this strategy, we isolated 8 full-length molecular clones from the donor. Two of the eight molecular clones, 03In94_D17 and 03In94_D24, (D17 and D24) generated replication-competent viruses. Phylogenetic analysis of the full-length viral sequences revealed that both clones were non-recombinant subtype C viruses. They contain intact open reading frames in all the viral proteins. Both the viral clones are endowed with several unique molecular and biological properties. The viral promoter of the clones is characterized by the presence of four NF-kB binding elements, a feature rarely seen in the subtype C HIV-1 LTR. Interestingly, we identified the coexistence of two different forms of Rev, a truncated form common to subtype C and a full-length form less common for this subtype, in both proviral and plasma virus compartments. An exceptional property of the viruses, atypical of subtype C, is their ability to use a wide range of coreceptors including CCR5, CXCR4, and several others tested. Sequence analysis of Env of D17 and D24 clones identified differences within the variable loops providing important clues for the expanded coreceptor use. The V1, V2 and V4 loops in both of the molecular clones are longer due to the insertion of several amino acid residues that generated potential N-linked glycosylation sites. Conclusion The exceptional biological and molecular properties of these clones make them invaluable tools to understand the unique pathogenic characteristics of subtype C.

90. CCL2 mobilizes ALIX to facilitate Gag-p6 mediated HIV-1 virion release

Author

David O Ajasin, Vasudev R Rao, Xuhong Wu, Santhamani Ramasamy, Mario Pujato, Arthur P Ruiz, Andras Fiser, Anne R Bresnick, Ganjam V Kalpana, and Vinayaka R Prasad

Subjects

CCL2, ALIX, HIV-1, HIV-1 clade C, Gag p6, late domain, Medicine, Science, Biology (General), QH301-705.5

Abstract

Cellular ESCRT machinery plays pivotal role in HIV-1 budding and release. Extracellular stimuli that modulate HIV-1 egress are currently unknown. We found that CCL2 induced by HIV-1 clade B (HIV-1B) infection of macrophages enhanced virus production, while CCL2 immuno-depletion reversed this effect. Additionally, HIV-1 clade C (HIV-1C) was refractory to CCL2 levels. We show that CCL2-mediated increase in virus production requires Gag late motif LYPX present in HIV-1B, but absent in HIV-1C, and ALIX protein that recruits ESCRT III complex. CCL2 immuno-depletion sequestered ALIX to F-actin structures, while CCL2 addition mobilized it to cytoplasm facilitating Gag-ALIX binding. The LYPX motif improves virus replication and its absence renders the virus less fit. Interestingly, novel variants of HIV-1C with PYRE/PYKE tetrapeptide insertions in Gag-p6 conferred ALIX binding, CCL2-responsiveness and enhanced virus replication. These results, for the first time, indicate that CCL2 mediates ALIX mobilization from F-actin and enhances HIV-1 release and fitness.

Published

2019

91. High-affinity RNA Aptamers Against the HIV-1 Protease Inhibit Both In Vitro Protease Activity and Late Events of Viral Replication

Author

Sonald Duclair, Archana Gautam, Andrew Ellington, and Vinayaka R Prasad

Subjects

anti-HIV-1 gene therapy, HIV-1 inhibitor, HIV-1 PR inhibitor, RNA aptamer structure, RNA aptamer, Therapeutics. Pharmacology, RM1-950

Abstract

HIV-1 aspartyl protease (PR) plays a key role in virion morphogenesis, underscoring the effectiveness of protease inhibitors (PI). Despite their utility, side effects and drug-resistance remains a problem. We report the development of RNA aptamers as inhibitors of HIV-1 PR for potential use in anti-HIV gene therapy. Employing Systematic Evolution of Ligands by Exponential Enrichment (SELEX), we isolated four unique families of anti-HIV-1 PR RNA aptamers displaying moderate binding affinities (Kd = 92–140 nmol/l) and anti-PR inhibitory activity (Kis = 138–647 nmol/l). Second-generation RNA aptamers selected from partially randomized pools based on two of the aptamer sequences displayed striking enhancements in binding (Kds = 2–22 nmol/l) and inhibition (Kis = 31–49 nmol/l). The aptamers were specific in that they did not bind either the related HIV-2 protease, or the cellular aspartyl protease, Cathepsin D. Site-directed mutagenesis of a second-generation aptamer to probe the predicted secondary structure indicated that the stem-loops SL2 and SL3 and the stem P1 were essential for binding and that only the 3’-most 17 nucleotides were dispensable. Anti-PR aptamers inhibited HIV replication in vitro and the degree of inhibition was higher for second-generation aptamers with greater affinity and the inhibition was abrogated for a nonbinding aptamer variant.

Published

2015

92. The gp120 protein is a second determinant of decreased neurovirulence of Indian HIV-1C isolates compared to southern African HIV-1C isolates.

Author

Vasudev R Rao, Ujjwal Neogi, Eliseo Eugenin, and Vinayaka R Prasad

Subjects

Medicine, Science

Abstract

Regional differences in neurovirulence have been documented among subtype/clade-C HIV-1 isolates in India and Southern Africa. We previously demonstrated that a C31S substitution in Clade-C Tat dicysteine motif reduces monocyte recruitment, cytokine induction and direct neurotoxicity. Therefore, this polymorphism is considered to be a causative factor for these differences in neurovirulence. We previously reported on the genotypic differences in Tat protein between clade-C and rest of the clades showing that approximately 90% of clade-C HIV-1 Tat sequences worldwide contained this C31S polymorphism, while 99% of non-clade C isolates lacked this Tat polymorphism at C31 residue (Ranga et al. (2004) J Virol 78:2586-2590). Subsequently, we documented intra-clade-C differences in the frequency of Tat dicysteine variants between India and Southern Africa, as the basis for differential disease severity and showed the importance of the Tat dicysteine motif for neuropathogenesis using small animal models. We have now examined if determinants of neurovirulence besides Tat are different between the clade-C HIV-1 isolates from Southern Africa and India. Envelope glycoprotein gp120 is a well-documented contributor to neurotoxicity. We found that gp120 sequences of HIV-1 isolates from these two regions are genetically distinct. In order to delineate the contribution of gp120 to neurovirulence, we compared direct in vitro neurotoxicity of HIV-infected supernatants of a representative neurovirulent US clade-B isolate with two isolates each from Southern Africa and India using primary human neurons and SH-SY5Y neuroblastoma cells. Immunodepletion of gp120 of both US clade B and the Southern African clade C isolates revealed robust decreases in neurotoxicity, while that of the Indian isolates showed minimal effect on neurotoxicity. The gp120 as a cause of differential neurotoxicity was further confirmed using purified recombinant gp120 from HIV isolates from these regions. We conclude that gp120 is one of the key factors responsible for the decreased neurovirulence of Indian clade C HIV-1 isolates when compared to South African clade C HIV-1.

Published

2014