Your search keyword '"Masanori Hayami"' showing total 19 results

1. A genetically engineered live-attenuated simian–human immunodeficiency virus that co-expresses the RANTES gene improves the magnitude of cellular immunity in rhesus macaques

Author

Yuya Shimizu, Masashi Okoba, Takeshi Haga, Kentaro Ibuki, Katsuhisa Inaba, Tomoyuki Miura, Masanori Hayami, Ai Himeno, Kentaro Kaneyasu, and Yoshitaka Goto

Subjects

CD4-Positive T-Lymphocytes, Male, Chemokine, Cellular immunity, HIV Antigens, T cell, viruses, animal diseases, T-Cell Antigen Receptor Specificity, Virus, Interferon-gamma, RANTES, Adjuvants, Immunologic, stomatognathic system, Immunity, Virology, medicine, Animals, HIV vaccine, Chemokine CCL5, Adjuvant, Acquired Immunodeficiency Syndrome, biology, SHIV, HIV-1, SIV, RANTES, Adjuvant, Vaccine, Chemokine, ELISPOT, Vaccination, virus diseases, hemic and immune systems, Viral Load, Macaca mulatta, CD4 Lymphocyte Count, medicine.anatomical_structure, SHIV, SIV, Immunology, biology.protein, HIV-1, Simian Immunodeficiency Virus, Vaccine, Reassortant Viruses

Abstract

Regulated-on-activation-normal-T-cell-expressed-and-secreted (RANTES), a CC-chemokine, enhances antigen-specific T helper (Th) type-1 responses against HIV-1. To evaluate the adjuvant effects of RANTES against HIV vaccine candidate in SHIV-macaque models, we genetically engineered a live-attenuated SHIV to express the RANTES gene (SHIV-RANTES) and characterized the virus's properties in vivo. After the vaccination, the plasma viral loads were same in the SHIV-RANTES-inoculated monkeys and the parental nef-deleted SHIV (SHIV-NI)-inoculated monkeys. SHIV-RANTES provided some immunity in monkeys by remarkably increasing the antigen-specific CD4+ Th cell-proliferative response and by inducing an antigen-specific IFN-gamma ELISpot response. The magnitude of the immunity in SHIV-RANTES-immunized animals, however, failed to afford greater protection against a heterologous pathogenic SHIV (SHIV-C2/1) challenge compared to control SHIV-NI-immunized animals. SHIV-RANTES immunized monkeys, elicited robust cellular CD4+ Th responses and IFN-gamma ELISpot responses after SHIV-C2/1 challenge. These findings suggest that the chemokine RANTES can augment vaccine-elicited, HIV-specific CD4+ T cell responses.

Published

2007

2. Comparative histopathological studies in the early stages of acute pathogenic and nonpathogenic SHIV-infected lymphoid organs

Author

Kentaro Ibuki, Toshihide Shimada, Hajime Suzuki, Manabu Fukumoto, Masanori Hayami, Makiko Motohara, Takeo Kuwata, Tomoyuki Miura, Tohko Iida, and Masahiro Ui

Subjects

Lymphoid Tissue, viruses, Simian Acquired Immunodeficiency Syndrome, HIV Infections, Biology, Simian, Virus, Acute Thymic Involution, Proviruses, Virology, Pathology, Animals, Animal model, Involution (medicine), Viremia, music, Medulla, music.instrument, Base Sequence, Virulence, Chimera, HIV, biology.organism_classification, Macaca mulatta, Follicular hyperplasia, CD4 Lymphocyte Count, AIDS, Disease Models, Animal, Microscopy, Electron, Lymphatic system, SIV, DNA, Viral, Immunology, Rhesus monkey, Simian Immunodeficiency Virus, Lymph

Abstract

To clarify the early pathological events in simian and human immunodeficiency chimeric virus (SHIV)-infected lymphoid organs, we examined rhesus macaques infected with an acute pathogenic SHIV (SHIV89.6P) or a nonpathogenic SHIV (NM-3rN) by sequential biopsies and serial necropsies. In the SHIV89.6P-infected monkeys, acute thymic involution as shown by increased cortical tingible-body macrophages and by neutrophilic infiltrates without follicular aggregation in the medulla began within 14 days postinoculation (dpi). Cells that were strongly positive for the virus were identified in the thymic medulla. SHIV89.6P-infected lymph nodes showed severe paracortical lymphadenitis with scattered virus-positive cells at 14 dpi and they developed paracortical depletion without the obvious follicular involution. In contrast, NM-3rN-infected monkeys showed no signs of thymic dysinvolution and the lymph nodes exhibited only follicular hyperplasia. NM-3rN-infected monkeys showed much fewer virus-positive cells in these lymphoid tissues than did SHIV89.6P-infected monkeys during the same period. These differences clearly reflect the difference in the virulence of these SHIVs.

Published

2003

3. Characterization of Less Pathogenic Infectious Molecular Clones Derived from Acute-Pathogenic SHIV-89.6P Stock Virus

Author

Taichiro Takemura, Iouri L. Kozyrev, Tomoyuki Miura, Takeo Kuwata, Toshihide Shimada, Masanori Hayami, and Kentaro Ibuki

Subjects

Time Factors, Lymphoid Tissue, viruses, HIV Antibodies, Virus Replication, Virus, Cell Line, Virology, Animals, Recombination, Genetic, Acquired Immunodeficiency Syndrome, biology, Inoculation, Antiviral antibody, Viral Load, Macaca mulatta, In vitro, CD4 Lymphocyte Count, Disease Models, Animal, Polyclonal antibodies, Cell culture, DNA, Viral, Cd4 cell, biology.protein, HIV-1, Simian Immunodeficiency Virus, Viral load

Abstract

For a better understanding of the acute pathogenicity of SHIV-89.6P stock virus, which induces prominent CD4 cell loss within a month after inoculation in monkeys, we have constructed four infectious molecular clones (cl 18, cl 64, cl 69, and cl 71). Cl 64, cl 69, and cl 71, like the parental virus, showed a high in vitro replication ability and a pathogenic-like effect (CD4 downmodulation) in a monkey CD4 + cell line, whereas cl 18 showed a lower replication ability and could not downmodulate CD4. Cl 64, which has characteristics similar to those of the parental virus in vitro, was inoculated into four rhesus monkeys. All monkeys showed a plasma viral load similar to that of the parental virus with a peak at 2 weeks after inoculation. However, the viral load gradually decreased and the virus failed to cause an AIDS-like disease in infected monkeys, but it induced a strong antiviral antibody response. These results demonstrate the polyclonal nature of the parental SHIV-89.6P virus stock and demonstrate that cl 64, aside from its high replicability, may differ qualitatively from the parental virus.

Published

2001

4. DNA Vaccination of Macaques by a Full Genome HIV-1 Plasmid Which Produces Noninfectious Virus Particles

Author

Hiroshi Yamamoto, Masanori Hayami, Kazuki Katsuyama, Hidemi Takahashi, Takeo Kuwata, Masahiro Ui, Hiromi Uesaka, Toshihide Shimada, Eiji Ido, and Wataru Akahata

Subjects

Male, HIV Antigens, T-Lymphocytes, Molecular Sequence Data, Simian Acquired Immunodeficiency Syndrome, Gene Products, gag, HIV Infections, Genome, Viral, HIV Antibodies, Biology, Macaque, Virus, DNA vaccination, law.invention, Viral vector, Interferon-gamma, Plasmid, Proviruses, Neutralization Tests, law, Virology, biology.animal, Vaccines, DNA, Animals, Amino Acid Sequence, Cells, Cultured, AIDS Vaccines, Vaccination, Gene Products, env, Zinc Fingers, Viral Load, Macaca mulatta, Killer Cells, Natural, Naked DNA, DNA, Viral, HIV-1, Recombinant DNA, RNA, Viral, Sequence Alignment, Viral load, Plasmids

Abstract

In this study, we tried a DNA vaccination regime in rhesus macaques using a full genome HIV-1 plasmid. The HIV-1 genome is under the control of its original LTR promoter, but has a mutated zinc finger motif gene in the nucleocapsid region. Due to the lack of genomic RNA packaging, the plasmid produces only noninfectious viral particles. We repeatedly injected four macaque monkeys intramuscularly with the naked DNA over a period of 40 weeks. To evaluate the humoral and cell-mediated immunity provided by this DNA vaccination, no other booster or other recombinant viral vectors were used. Immunological responses against HIV-1 were elicited in all of the vaccinated monkeys: stable anti-HIV-1 Env antibodies were raised in two monkeys and CTL activities were induced in the other monkeys. The macaques were intravenously challenged at 54 weeks with 100 TCID50 of SHIV-NM-3rN, which possesses an envelope gene homologous to the one in the vaccinated plasmid. In all of the vaccinated macaques, the peak plasma viral loads induced by the challenge virus were two to three orders of magnitude lower than those of the naive controls. These results suggest that a DNA vaccination regime with a full genome plasmid alone is potentially efficacious and provides a new possibility for the development of an AIDS vaccine.

Published

2000

5. Dox-Dependent SIVmac with Tetracycline-Inducible Promoter in the U3 Promoter Region

Author

Hisatoshi Shida, Yong Xiao, Tomoyuki Miura, Masanori Hayami, and Takeo Kuwata

Subjects

Gene Expression Regulation, Viral, Transcription, Genetic, Viral protein, T-Lymphocytes, viruses, TATA box, Biology, medicine.disease_cause, Chloramphenicol acetyltransferase, Virology, medicine, Humans, Promoter Regions, Genetic, Enhancer, Reporter gene, Terminal Repeat Sequences, Viral Vaccines, Promoter, Tetracycline, Molecular biology, Long terminal repeat, Viral replication, Doxycycline, Simian Immunodeficiency Virus, HeLa Cells

Abstract

An attenuated live vaccine is a candidate in developing vaccines against human immunodeficiency virus type 1 (HIV-1). The study using macaques and simian immunodeficiency virus (SIVmac) showed an attenuated virus to be more effective than any other vaccine candidate. However, development of a safer vaccine is required for clinical application. In this study, we constructed pSIVmac Delta nef with tetracycline inducible promoter (pTet) and tried to control viral expression in a drug-dependent manner. Promoter/enhancer motifs in the U3 region of the long terminal repeats (LTRs) were serially deleted and replaced with pTet. In mutant LTRs, which lack NF-kappaB and Sp1 binding sites, TATA box motifs, and the 5' half of the U3 region, promoter activity was stringently controlled by doxycycline (Dox). Their activities were similar to or higher than that of wild-type LTR in the presence of Dox, based on the transient chloramphenicol acetyltransferase reporter assay. Three of these mutant LTRs were introduced into the pSIVmac239 Delta nef genome. Viral protein from these viruses was efficiently expressed in a Dox-dependent manner after transfection to a HeLa cell, which expresses reverse tetracycline transactivator (rtTA). The 2-LTR-form viral DNA of these viruses could be detected in M8166 cells that had been infected with supernatants from the transfected rtTA HeLa cell. These results suggest that pSIVmac Delta nef containing mutant LTRs can proceed through one viral replication cycle consisting of transcription, formation of viral particles, infection to cells, and reverse transcription. Although continuous replication of these Dox-dependent viruses requires a supply of rtTA as a constituent for the pTet-On viral genome, the successful replacement of the original promoter with a drug-dependent promoter suggests a new possibility for developing a safer attenuated live virus.

Published

2000

6. Protection of Macaques against a SHIV with a Homologous HIV-1 Env and a Pathogenic SHIV-89.6P with a Heterologous Env by Vaccination with Multiple Gene-Deleted SHIVs

Author

Yasuyuki Miyazaki, Kentaro Ibuki, Masahiro Ui, Tomoyuki Miura, Takeo Kuwata, Hiroshi Yamamoto, Toshihide Shimada, Yoshimi Enose, Iouly L. Kozyrev, Tatsuhiko Igarashi, Masanori Hayami, and Hiromi Uesaka

Subjects

Male, animal diseases, viruses, Simian Acquired Immunodeficiency Syndrome, Heterologous, Gene Products, nef, Virus, Microbiology, Viral Envelope Proteins, stomatognathic system, Virology, Homologous chromosome, Animals, Humans, Viral Regulatory and Accessory Proteins, nef Gene Products, Human Immunodeficiency Virus, Antigens, Viral, Gene, AIDS Vaccines, Vaccines, Synthetic, Innate immune system, biology, Gene Products, vpr, virus diseases, vpr Gene Products, Human Immunodeficiency Virus, Macaca mulatta, Vaccination, HIV-1, biology.protein, Simian Immunodeficiency Virus, Antibody, Viral load, Gene Deletion

Abstract

To evaluate the potential of SHIVs as anti-HIV-1 live vaccines, we constructed two gene-deleted SHIVs, designated SHIV-drn and SHIV-dxrn. The former lacks vpr/nef and the latter lacks vpx/vpr/nef. Four macaques that had been vaccinated with SHIV-drn were challenged with SHIV-NM-3rN, which has an HIV-1 Env that is the same as that of SHIV-drn. No challenge virus was detected by DNA PCR in, or recovered from, two of the macaques. In the other two, challenge virus was detected once and twice, respectively. Plasma viral loads were much lower than those in unvaccinated controls. Another four macaques were vaccinated with SHIV-dxrn. These macaques showed resistance but less than that of SHIV-drn-vaccinated macaques. When the two SHIV-drn-vaccinated macaques were challenged with pathogenic SHIV-89.6P, which has an HIV-1 Env that is antigenically different from that of SHIV-drn, replication of the challenge virus was restricted, and the usual decrease in the number of CD4 + cells was prevented. In this protection, it is noteworthy that protection involved not only neutralizing antibodies and killer cell activity, but also other unknown specific and nonspecific immunity elicited by the infection.

Published

1999

7. Small Amino Acid Changes in the V3 Loop of Human Immunodeficiency Virus Type 2 Determines the Coreceptor Usage for CXCR4 and CCR5

Author

Yoshitaka Isaka, Tamio Fujiwara, Masanori Hayami, Takashi Uchiyama, Toshiyuki Hori, Shinobu Kawauchi, Osamu Yoshie, Akihiko Sato, Shigeru Miki, Hitoshi Sakaida, and Akio Adachi

Subjects

CD4-Positive T-Lymphocytes, Receptors, CXCR4, Receptors, CCR5, viruses, Molecular Sequence Data, Cell, Clone (cell biology), HIV Envelope Protein gp120, Biology, V3 loop, Transfection, Ghana, CXCR4, Jurkat Cells, Chemokine receptor, Genes, Reporter, Virology, medicine, Humans, Amino Acid Sequence, HIV Long Terminal Repeat, chemistry.chemical_classification, Acquired Immunodeficiency Syndrome, Reporter gene, Sequence Homology, Amino Acid, virus diseases, beta-Galactosidase, Recombinant Proteins, Amino acid, medicine.anatomical_structure, chemistry, HIV-2, HIV-1, Sequence Alignment, HeLa Cells

Abstract

HIV-2 GH-1 is a molecular clone derived from an AIDS patient from Ghana. In contrast to the prototypic molecular clone ROD, GH-1 exhibits a narrow range of target cell specificity. By an infectious assay using HeLa-CD4 cells stably transfected with an HIV-1 LTR-β-galactosidase reporter gene and transiently expressing various cloned chemokine receptors, we have examined the coreceptor usage of GH-1. In contrast to ROD, which uses principally CXCR4, GH-1 was found to use mainly if not exclusively CCR5 but not CXCR4. The distinct coreceptor usage of these two molecular clones allowed us to further map the region of gp120 that is important for the coreceptor specificity. By constructing a series of chimeric viruses between GH-1 and ROD, we have demonstrated that the C-terminal half of the V3 loop region of gp120 determines the differential coreceptor usage between GH-1 and ROD, and only a few amino acid differences in this region appear to be able to shift the specificity between CCR5 and CXCR4. Notably, the shift in the coreceptor usage from CCR5 to CXCR4 is associated with an increase in the net positive charge in the V3 region.

Published

1999

8. Functional classification of simian immunodeficiency virus isolated from a chimpanzee by transactivators

Author

Akio Adachi, Hiroyuki Sakai, Masanori Hayami, Simon Wain-Hobson, Jun-Ichi Sakuragi, Riri Shibata, and Sayuri Sakuragi

Subjects

Chloramphenicol O-Acetyltransferase, Gene Expression Regulation, Viral, Pan troglodytes, viruses, Molecular Sequence Data, DNA, Recombinant, Human immunodeficiency virus (HIV), Biology, Rev Protein, medicine.disease_cause, Virus, Sequence Homology, Nucleic Acid, Virology, medicine, Animals, Amino Acid Sequence, Gene, Genetics, Base Sequence, virus diseases, rev Gene Products, Human Immunodeficiency Virus, Simian immunodeficiency virus, Primate Lentiviruses, Gene Products, rev, Gene Products, tat, HIV-1, Trans-Activators, Nucleic Acid Conformation, RNA, Viral, Simian Immunodeficiency Virus, tat Gene Products, Human Immunodeficiency Virus

Abstract

In reporter-based transient expression systems, we characterized simian immunodeficiency virus from a chimpanzee (SIVCPZ), with special reference to the human immunodeficiency virus type 1 (HIV-1). SIVCPZ was not equally activated by tat and rev transactivators derived from representative primate lentiviruses. HIV-1 alone activated SIVCPZ to the full extent in both tat and rev assays. The tat and rev gene products of SIVCPZ, as well as those of HIV-1, efficiently transactivated the other viruses. These results indicate that SIVCPZ is identical to HIV-1 with regard to the compatibility of tat and rev gene activities among four subgroups of primate lentiviruses.

Published

1992

9. Functional analysis of long terminal repeats derived from four strains of simian immunodeficiency virus SIVAGM in Relation to Other Primate Lentiviruses

Author

T Kiyomasu, Jun-Ichi Sakuragi, Hiroyuki Sakai, Akio Adachi, Akinori Ishimoto, Masanori Hayami, Meiko Kawamura, Hirofumi Akari, Riri Shibata, and Masashi Fukasawa

Subjects

Chloramphenicol O-Acetyltransferase, animal structures, animal diseases, viruses, Molecular Sequence Data, Biology, Transfection, medicine.disease_cause, Virus, Chloramphenicol acetyltransferase, Plasmid, Sequence Homology, Nucleic Acid, Virology, Chlorocebus aethiops, medicine, Animals, Promoter Regions, Genetic, Gene, HIV Long Terminal Repeat, Repetitive Sequences, Nucleic Acid, Base Sequence, Lentivirus, virus diseases, Promoter, biochemical phenomena, metabolism, and nutrition, Simian immunodeficiency virus, Macaca mulatta, Molecular biology, Recombinant Proteins, Long terminal repeat, Models, Structural, HIV-2, HIV-1, Nucleic Acid Conformation, RNA, Viral, Simian Immunodeficiency Virus, Papio

Abstract

The promoter activity of long terminal repeats (LTRs) of four strains of the simian immunodeficiency virus isolated from African green monkeys (SIVAGM) was compared with those of various LTRs derived from the other representative primate lentiviruses: human immunodeficiency virus type 1 (HIV-1), type 2 (HIV-2), SIV from a rhesus monkey (SIVMAC), and SIV from a mandrill (SIVMND). The expression of the LTRs was evaluated by monitoring chloramphenicol acetyltransferase production after transfection of reporter plasmid clones. In the absence of viral tat, all SIVAGM LTRs acted as much more efficient promoters than any of the other LTRs. When tat gene products were supplied in trans, LTRs of SIVAGM and SIVMND were activated inefficiently relative to high responder LTRs of HIV-2 and SIVMAC. The LTR of HIV-1 was highly activated by HIV-1 tat, but not so much by HIV-2, SIVAGM, and SIVMND tat.

Published

1991

10. Compatibility of rev gene activity in the four groups of primate lentiviruses

Author

Hiroyuki Sakai, Meiko Kawamura, Akinori Ishimoto, Masanori Hayami, Jun-Ichi Sakuragi, Akio Adachi, Riri Shibata, and T Kiyomasu

Subjects

Gene Expression Regulation, Viral, viruses, Molecular Sequence Data, Mutant, Biology, medicine.disease_cause, Marker gene, Virus, Cell Line, Virology, medicine, Cloning, Molecular, Gene, Regulator gene, Genetics, Base Sequence, Genetic Complementation Test, Lentivirus, RNA-Directed DNA Polymerase, Simian immunodeficiency virus, Genes, gag, Genes, rev, Complementation, Cell culture, HIV-2, Mutation, HIV-1, RNA, Viral, Simian Immunodeficiency Virus

Abstract

The compatibility of rev genes derived from various primate immunodeficiency viruses of all distinct subgroups identified was assessed in three experimental systems: complementation experiments between proviral rev and gag mutants, evaluation of the ability of the rev gene products to activate proviral reporters, and examination of the capacity of various viruses to augment marker gene expression in the infected reporter cell lines. In all systems, human immunodeficiency virus type 1 (HIV-1) rev was not substantially substituted or was extremely poorly substituted by the rev of the other viruses. The rev of simian immunodeficiency virus (SIV) from a mandrill could be exchanged by HIV-1 rev. In contrast, the rev gene products of all viruses efficiently activate HIV-2 and SIV from an African green monkey.

Published

1991

11. Induction of immune response in macaque monkeys infected with simian-human immunodeficiency virus having the TNF-alpha gene at an early stage of infection

Author

Takeshi Haga, Tomoyuki Miura, Yasuyuki Miyazaki, Kentaro Kaneyasu, Kentaro Ibuki, Yuya Shimizu, Yoshitaka Goto, Masanori Hayami, and Hajime Suzuki

Subjects

Chemokine, viruses, animal diseases, Proliferation, DNA, Recombinant, Simian Acquired Immunodeficiency Syndrome, HIV Infections, Biology, HIV Antibodies, Antibodies, Viral, Lymphocyte Activation, Macaque, Virus, RANTES, Immune system, stomatognathic system, Immunity, biology.animal, Virology, Animals, Humans, Lymphocytes, Immune response, Chemokine CCL5, Base Sequence, Tumor Necrosis Factor-alpha, Lymphokine, virus diseases, Macaca mulatta, SHIV, SIV, Gene Expression Regulation, TNF-α, Immunology, biology.protein, HIV-1, Cytokines, Tumor necrosis factor alpha, Female, Simian Immunodeficiency Virus, Genetic Engineering, Viral load

Abstract

TNF-alpha has been implicated in the pathogenesis of, and the immune response against, HIV-1 infection. To clarify the roles of TNF-alpha against HIV-1-related virus infection in an SHIV-macaque model, we genetically engineered an SHIV to express the TNF-alpha gene (SHIV-TNF) and characterized the virus's properties in vivo. After the acute viremic stage, the plasma viral loads declined earlier in the SHIV-TNF-inoculated monkeys than in the parental SHIV (SHIV-NI)-inoculated monkeys. SHIV-TNF induced cell death in the lymph nodes without depletion of circulating CD4(+) T cells. SHIV-TNF provided some immunity in monkeys by increasing the production of the chemokine RANTES and by inducing an antigen-specific proliferation of lymphocytes. The monkeys immunized with SHIV-TNF were partly protected against a pathogenic SHIV (SHIV-C2/1) challenge. These findings suggest that TNF-alpha contributes to the induction of an effective immune response against HIV-1 rather than to the progression of disease at the early stage of infection.

Published

2005

12. Various types of HIV mixed infections in Cameroon

Author

Lutz G. Gürtler, Tomoyuki Miura, Lazare Kaptue, Hiroyuki Moriyama, Leopold Zekeng, Masahiro Yamashita, Innocent Mboudjeka, Eiji Ido, Masanori Hayami, and Jun Takehisa

Subjects

Adult, Male, Adolescent, Molecular Sequence Data, Human immunodeficiency virus (HIV), HIV Infections, Genome, Viral, Biology, medicine.disease_cause, Genes, env, Acquired immunodeficiency syndrome (AIDS), Virology, Genotype, medicine, Humans, Amino Acid Sequence, Cameroon, Phylogeny, Genetic diversity, Molecular epidemiology, Incidence (epidemiology), Central africa, virus diseases, Middle Aged, medicine.disease, HIV-2, HIV-1, Female, Sequence Alignment, Sequence Analysis, Mixed infection

Abstract

In order to assess the incidence of HIV mixed infection as well as to clarify the molecular epidemiology of HIV in central Africa, we investigated 43 HIVs obtained from 211 Cameroonian AC, ARC, and AIDS patients in 1994 and 1995. Part of the pol region and part of the env region were phylogenetically analyzed. The genotypes observed were varied: of 43 specimens, 28 (65%) were subtype A, 1 (2%) was subtype B, 2 (5%) were subtype D, 3 (7%) were subtype F, and 2 (5%) were group O. Of the remaining 7 specimens, 3 were mixed infections with HIV-1 subtypes A and C, HIV-1 subtypes C and F, and HIV-2 subtype A and HIV-1 subtype A; 1 was a mixed infection with HIV-1 subtypes A and D and the highly divergent group O (triple infection); another 3 appeared to consist of mosaic genomes (A/G, A/E, and B/A recombinant). These data show that various types of mixed infection, such as between different subtypes of HIV-1 group M, between HIV-1 and HIV-2, and even between HIV-1 groups O and M, were confirmed at a rather high frequency (approximately 10%). The mixed infection is particularly significant where there is a greater variety of HIV-1 subtypes circulating, since it results in new genetic diversity generated by intersubtype recombination.

Published

1998

13. Evidence for direct association of Vpr and matrix protein p17 within the HIV-1 virion

Author

Akemi Suyama, Tamio Fujiwara, Jun Yoshimoto, Shigeru Miki, Osamu Yoshie, Masanori Hayami, Akio Adachi, Yoshitaka Isaka, and Akihiko Sato

Subjects

Immunoprecipitation, HIV Antigens, viruses, Guinea Pigs, Molecular Sequence Data, Human immunodeficiency virus (HIV), Gene Products, gag, Biology, medicine.disease_cause, gag Gene Products, Human Immunodeficiency Virus, Cell Line, Viral Proteins, immune system diseases, Virology, Cricetinae, medicine, Tumor Cells, Cultured, Animals, Humans, Viral matrix protein, Base Sequence, Gene Products, vpr, virus diseases, vpr Gene Products, Human Immunodeficiency Virus, biochemical phenomena, metabolism, and nutrition, Precipitin Tests, Yeast, Cell biology, Capsid, Cell culture, DNA, Viral, HIV-1, Nuclear transport

Abstract

Vpr is one of the auxiliary proteins of HIV-1 and is selectively incorporated into the virion by a process involving the C-terminal p6 portion of the Gag precursor Pr55. Vpr and the matrix protein p17 are the components of the viral preintegration complex and appear to play important roles in the nuclear transport of proviral DNA in nondividing cells. In the present study, we have demonstrated by coimmunoprecipitation experiments that Vpr associates with matrix protein p17 but not with capsid protein p24 within the HIV-1 virion. Experiments employing the yeast two-hybrid GAL4 assay for protein–protein interactions also demonstrated a direct association between Vpr and the C-terminal region of matrix protein p17. Association of Vpr and the matrix protein p17 within the mature virion is consistent with their collaborative role in the nuclear transportation of the viral preintegration complex in nondividing cells such as macrophages.

Published

1996

14. Isolation and characterization of a highly divergent HIV-2[GH-2]: generation of an infectious molecular clone and functional analysis of its rev-responsive element in response to primate retrovirus transactivators (Rev and Rex)

Author

Keizo Tomonaga, Victor B.A. Netty, Mubarak Osei-Kwasi, Masuyo Nakai, Koh-Ichi Ishikawa, Osamu Hishida, J. A. A. Mingle, Masanori Hayami, Tomoyuki Miura, Jun-Ichi Sakuragi, Jun Katahira, Masashi Fukasawa, Hirofumi Akari, and Meiko Kawamura

Subjects

Genetics, Gene Expression Regulation, Viral, biology, TATA box, Genes, pX, Restriction Mapping, Clone (cell biology), Nucleic acid sequence, virus diseases, Genetic Variation, Molecular biology, Integrase, Genes, rev, Restriction site, Restriction map, Virology, Sequence Homology, Nucleic Acid, DNA, Viral, HIV-2, biology.protein, HIV Long Terminal Repeat, Cloning, Molecular, Enhancer

Abstract

A highly divergent HIV-2 designated as HIV-2[GH-2] was obtained from an AIDS-related complex (ARC) patient in Ghana. A full-length molecular clone of this isolate was obtained and a biologically active clone was constructed. Its restriction pattern differed from that of prototype HIV-2[GH-1] in 25 of 35 restriction sites, but was strikingly similar to a previously characterized HIV-2 isolate from a Ghanaian (HIV-2ALT). The conserved integrase region (288-bp fragment) previously displayed 95% identity with that of ALT but 17-20% divergence from the HIV-2 prototype member, and a new distinct subgroup (HIV-2b) of HIV-2 consisting of GH-2 and ALT was postulated (Miura et al. 1991.) These isolates, however, were biologically distinguishable from each other by its replication capacity in a monocyte line, U937, in which GH-2 could not grow but ALT grew well. In addition, the nucleotide sequence of the LTR of this new isolate displays 21% divergence from that of prototype HIV-2[GH-1], but the core enhancer, Sp1 binding sites and TATA box were conserved. Although the 3' half of the env gene sequence which is deleted in HIV-2ALT clone showed 27% diversity from the prototype, functional differences in the rev-responsive element were not observed.

Published

1992

15. Detection and characterization of simian retroviruses homologous to human T-cell leukemia virus type I

Author

Isao Miyoshi, Motoharu Seiki, Mitsuaki Yoshida, Toshiki Watanabe, Masanori Hayami, Atsumi Komuro, and Hajime Tsujimoto

Subjects

viruses, Gene Products, gag, Simian, Deltaretrovirus, Viral Proteins, Restriction map, Viral Envelope Proteins, hemic and lymphatic diseases, Virology, Homologous chromosome, medicine, Animals, Humans, biology, virus diseases, DNA Restriction Enzymes, Haplorhini, Provirus, biology.organism_classification, medicine.disease, Human T cell leukemia virus, Leukemia, Retroviridae, Cell culture, DNA, Viral, biology.protein, Antibody

Abstract

Lymphoid cell lines were established from five different species of monkeys which were positive in antibodies cross-reactive with human T-cell leukemia virus type I (HTLV-I) and were shown to contain provirus sequences homologous to HTLV-I. Gene-specific probes of HTLV-I, gag, pol, env, pX, and LTR, hybridized efficiently with monkey DNAs from these cell lines under stringent conditions, indicating that the proviruses are very similar to HTLV-I along with whole viral genomes. However, the preliminary restriction mapping turned out the difference between simian retroviruses and HTLV-I and also among simian retroviruses. These findings suggest a common ancestor of simian and human retroviruses, but exclude the recent interspecies transmission between monkeys and humans.

Published

1984

16. Human T-Cell leukemia virus type I isolates from Gabon and Ghana: Comparative analysis of proviral genomes

Author

Masanori Hayami, Koh-Ichi Ishikawa, Tomoyuki Miura, Robert W. Cooper, Masashi Fukasawa, Eric Delaporte, Hajime Tsujimoto, B Ivanoff, J. A. A. Mingle, Eric Frost, and Francis C. Grant

Subjects

Genetics, biology, viruses, Nucleic Acid Hybridization, virus diseases, DNA Restriction Enzymes, Simian, Provirus, biology.organism_classification, Biological Evolution, Deltaretrovirus, Ghana, Virology, Genome, Virus, Sierra leone, Restriction enzyme, Restriction map, immune system diseases, hemic and lymphatic diseases, DNA, Viral, Gabon, Southern blot

Abstract

Two isolates of human T-cell leukemia virus type I (HTLV-I) were obtained from lymphocyte cultures of a healthy carrier in Gabon and another in Ghana. Their proviruses were analyzed by Southern blot hybridization and compared with prototypical HTLV-I isolated in Japan and the United States. The provirus genomes of both strains were highly homologous to the prototype HTLV-I along the whole viral genome. The restriction endonuclease sites of the Ghanian isolate were almost identical with those of the prototype HTLV-I, but 10 of 26 sites of the Gabonese isolate were different from those of the prototype. Furthermore, the restriction map of the Gabonese isolate resembled those of a simian T-cell leukemia virus (STLV-I) isolated from a chimpanzee from Sierra Leone and a variant of HTLV-I from Zaire (HTLV-Ib) more closely than those of any other known HTLV-I. These results indicated the existence of some unique strains of HTLV-I transmitted among African people, and the importance of clarifying the origin and transmission of HTLV group viruses.

Published

1987

17. In vivo analysis of a new R5 tropic SHIV generated from the highly pathogenic SHIV-KS661, a derivative of SHIV-89.6

Author

Megumi Matsuyama, Tatsuhiko Igarashi, Masanori Hayami, Kenta Matsuda, Kentaro Ibuki, Tomoyuki Miura, Naoki Saito, Mariko Horiike, Katsuhisa Inaba, and Yoshinori Fukazawa

Subjects

CD4-Positive T-Lymphocytes, animal diseases, viruses, Simian Acquired Immunodeficiency Syndrome, Mutagenesis (molecular biology technique), CCR5 tropic, Biology, Virus Replication, Virus, Viral Proteins, Species Specificity, Virology, Animals, Amino Acid Sequence, Peptide sequence, Tropism, chemistry.chemical_classification, virus diseases, Viral Load, Macaca mulatta, Phenotype, Amino acid, AIDS, V3 region, chemistry, Viral replication, SHIV, Mutagenesis, Mutagenesis, Site-Directed, Simian Immunodeficiency Virus, Sequence Alignment, Viral load

Abstract

Although X4 tropic SHIVs have been studied extensively, they show distinct infection phenotypes from those of R5 tropic viruses, which play an important role in HIV-1 transmission and pathogenesis. To augment the variety of R5 tropic SHIVs, we generated a new R5 tropic SHIV from the highly pathogenic X4 tropic SHIV-KS661, a derivative of SHIV-89.6. Based on consensus amino acid alignment analyses of subtype B R5 tropic HIV-1, five amino acid substitutions in the third variable region successfully changed the secondary receptor preference from X4 to R5. Improvements in viral replication were observed in infected rhesus macaques after two passages, and reisolated virus was designated SHIV-MK38. SHIV-MK38 maintained R5 tropism through in vivo passages and showed robust replication in infected monkeys. Our study clearly demonstrates that a minimal number of amino acid substitutions in the V3 region can alter secondary receptor preference and increase the variety of R5 tropic SHIVs.

18. Sequence homology of the simian retrovirus genome with human T-cell leukemia virus type I

Author

Masanori Hayami, Motoharu Seiki, Mitsuaki Yoshida, Hajime Tsujimoto, I. Miyoshi, and Toshiki Watanabe

Subjects

Genes, Viral, viruses, Genome, Deltaretrovirus, Homology (biology), Virus, Cell Line, Retrovirus, Simian retrovirus, Species Specificity, immune system diseases, hemic and lymphatic diseases, Virology, Sequence Homology, Nucleic Acid, Animals, Humans, Cloning, Molecular, Serotyping, Genetics, biology, Base Sequence, Nucleic acid sequence, virus diseases, Provirus, biology.organism_classification, Retroviridae, Macaca nemestrina

Abstract

A retrovirus highly related to human T-cell leukemia virus type I (HTLV-I) was isolated from a T-cell line established from a seropositive pig-tailed monkey and the provirus genome was molecularly cloned using HTLV-I as a probe. The monkey virus (STLV) had the genomic structure of the LTR-gag-pol-env-pX-LTR. Analysis of the env-pX-LTR region revealed the 90% homology of the nucleotide sequence with that of HTLV-I in each region. This high homology of the sequence indicates that STLV is a member of the HTLV family, but apparently different from HTLV-I. This suggests that the possibility of recent interspecies transmission from monkeys to humans in the endemic area is very small. From its similarity to HTLV, STLV should be useful as an animal model in studies on natural HTLV infection and leukemogenesis of HTLV in humans.

Published

1985

19. Molecular cloning of a feline leukemia provirus integrated adjacent to the c-myc gene in a feline T-cell leukemia cell line and the unique structure of its long terminal repeat

Author

Tomoyuki Miura, Masanori Hayami, Masashi Fukasawa, Hajime Tsujimoto, and Masabumi Shibuya

Subjects

Leukemia, T-Cell, viruses, T-cell leukemia, Molecular Sequence Data, Restriction Mapping, Molecular cloning, Biology, Feline leukemia virus, Proto-Oncogene Proteins c-myc, hemic and lymphatic diseases, Virology, Proto-Oncogene Proteins, Tumor Cells, Cultured, Cloning, Molecular, Gene, Southern blot, Repetitive Sequences, Nucleic Acid, Base Sequence, Leukemia Virus, Feline, Nucleic acid sequence, Provirus, biology.organism_classification, Cell Transformation, Viral, Molecular biology, Long terminal repeat, DNA, Viral

Abstract

This paper reports the molecular cloning of a rearranged c-myc region from the FT-1 cell line, which was derived from a spontaneous feline T-cell leukemia carrying the feline leukemia virus (FeLV). An abnormal c-myc EcoRI fragment of about 18 kilobases, detected by Southern blotting, was molecularly cloned from the DNA of the FT-1 cell line. The c-myc rearrangement in FT-1 was due to direct integration of the FeLV provirus genome immediately upstream of the c-myc gene in the opposite transcriptional orientation. Nucleotide sequencing showed that the LTR of this provirus had three copies of an enhancer-like sequence, unlike the sequences of FeLVs reported previously, which have only a single copy of this enhancer-like sequence.

Published

1989