HIV-1 Primarily Targets the Innate Immune System and Only Secondarily Modulates Adaptive Immune Cell Depletion

HIV-1 Primarily Targets the Innate Immune System and Only Secondarily Modulates Adaptive Immune Cell Depletion

下载PDF

导出

摘要 Persistence of HIV-1 infection allows for permissive microenvironmental conditioning in terms of contextual innate immune participation. The progression of host cell injury constitutes an additional parametric formulation in self-amplifying modulation of the adaptive immune response in a manner that inclusively promotes the emergence of a final stage of AIDS that is both depletive and permissive for opportunistic infections and various forms of neoplasia. It is within contextual indices of promotion of depleted T-helper lymphocytes and of augmented viremic loads that manifestations of classic lesions emerge as the AIDS phenomenon. It is further to be realized that an apoptotic response of multiple cell subtypes including T-lymphocytes includes host-cell participation within formulated settings of further persistence of the retroviral infection. An all-inclusive phenomenon of dendritic cell-lymphocyte synapse formulation corresponds to the establishment of HIV-1 infection that specifically conditions all subsequent stages in depletion of the injured host cells regardless of the dynamics or kinetics of the retroviral replicative infectious process itself. Persistence of HIV-1 infection allows for permissive microenvironmental conditioning in terms of contextual innate immune participation. The progression of host cell injury constitutes an additional parametric formulation in self-amplifying modulation of the adaptive immune response in a manner that inclusively promotes the emergence of a final stage of AIDS that is both depletive and permissive for opportunistic infections and various forms of neoplasia. It is within contextual indices of promotion of depleted T-helper lymphocytes and of augmented viremic loads that manifestations of classic lesions emerge as the AIDS phenomenon. It is further to be realized that an apoptotic response of multiple cell subtypes including T-lymphocytes includes host-cell participation within formulated settings of further persistence of the retroviral infection. An all-inclusive phenomenon of dendritic cell-lymphocyte synapse formulation corresponds to the establishment of HIV-1 infection that specifically conditions all subsequent stages in depletion of the injured host cells regardless of the dynamics or kinetics of the retroviral replicative infectious process itself.

作者 Lawrence M. Agius

机构地区 Department of Pathology University of Malta Medical School

出处《World Journal of AIDS》 2012年第3期226-231,共6页 艾滋病（英文）

关键词 HIV-1 INFECTION Aids IMMUNE PERSISTENCE HIV-1 Infection Aids Immune Persistence

分类号 R73 [医药卫生—肿瘤]

引文网络
相关文献

参考文献1

1Liguo Zhang,Lishan Su.HIV-1 immunopathogenesis in humanized mouse models[J].Cellular & Molecular Immunology,2012,9(3):237-244. 被引量：5

二级参考文献157

1United Nations Programme on HIV/AIDS. Global Facts & Figures [PDF on Internet], 2009. Available from= http://data.unaids.org/pub/factsheet/2009/20091124_ fs_global_en.pdf. Accessed date 15 Sep 2012.
2Ganick D J, Sarnwick RD, Shahidi NT, Manning DD. Inability of intravenously injected monocellular suspensions of human bone marrow to establish in the nude mouse. Int Arch Allergy Appl Irnmunol 1980; 62: 330-333.
3Bosma GC, Custer RP, Bosma MJ. A severe combined immunodeficiency mutation in the mouse. Nature 1983; 301: 527-530.
4Mosier DE, Gulizia R J, Baird SM, Wilson DB. Transfer of a functional human immune system to mice with severe combined immunodeficiency. Nature 1988; 335: 256- 259.
5McCune JM, Namikawa R, Kaneshima H, Shultz LD, Lieberman M, Weissman IL. The SCID-hu mouse: murine model for the analysis of human hematolymphoid differentiation and function. Science 1988; 241: 1632-1639.
6Shultz LD, Schweitzer PA, Christianson SW, Gott B, Schweitzer IB, Tennent B etal. Multiple defects in innate and adaptive immunologic function in NOD/LtSz-scid mice. J Immunol 1995; 154: 180-191.
7Hesselton RM, Greiner DL, Mordes JP, Rajah TV, Sullivan JL, Shultz LD. High levels of human peripheral blood mononuclear cell engraftment and enhanced susceptibility to human immunodeficiency virus type 1 infection in NOD/LtSz-scid/scid mice. J Infect Dis 1995; 172: 974-982.
8Pflumio F, Izac B, Katz A, Shultz LD, Vainchenker W, Coulombel L. Phenotype and function of human hematopoietic cells engrafting immune-deficient CB17-severe combined immunodeficiency mice and nonobese diabetic-severe combined immunodeficiency mice after transplantation of human cord blood mononuclear cells. Blood 1996; 88: 3731-3740.
9Yoshino H, Ueda T, Kawahata M, Kobayashi K, Ebihara Y, Manabe A et aL Natural killer cell depletion by anti-asialo GM1 antiserum treatment enhances human hematopoietic stem cell engraftment in NOD/Shi-scid mice. Bone Marrow Transplant2000; 26: 1211-1216.
10Ito M, Kobayashi K, Nakahata T. NOD/Shi-scid I L2rγ^null (NOG) mice more appropriate for humanized mouse models. Curr Top Microbiol Immunol 2008; 324: 53-76.

共引文献4

1孙丽娜,孙晨鸣,赵勇.免疫系统人源化小鼠模型的现状及应用[J].实验动物科学,2012,29(6):52-55. 被引量：5
2乔卿华,韩佩君,汪爱勤,尹文.用于病毒研究的人源化小鼠研究进展[J].生物技术通讯,2014,25(1):112-117. 被引量：1
3Tian-Jiao Fan,Li Sun,Xian-Guang Yang,Xia Jin,Wei-Wei Sun,Jian-Hua Wang.The Establishment of an In Vivo HIV-1 Infection Model in Humanized B-NSG Mice[J].Virologica Sinica,2020,35(4):417-425.
4夏巍,周艳,龚睿,谢芳,郭晓萍,周立,冯勇.HIV-1感染人源化小鼠模型的建立与鉴定[J].口岸卫生控制,2019,0(3):22-29.

1Xin (Eric) Jiang,Ting Xu,Qingyi Wei,Peng Li,Daniel R. Gomez,Laurence E. Court,Zhongxing Liao.DNA repair capacity correlates with standardized uptake values from 18F-fluorodeoxyglucose positron emission tomography/CT in patients with advanced non-small-cell lung cancer[J].Chronic Diseases and Translational Medicine,2018,4(2):109-116.
2陈驰.美国PACE社区养老模式在我国的引进、改良与实践[J].中国护理管理,2019,19(2):168-172. 被引量：8
3Kevin J Zwezdaryk,Joseph A Combs,Cindy A Morris,Deborah E Sullivan.Regulation of Wnt/β-catenin signaling by herpesviruses[J].World Journal of Virology,2016,5(4):144-154. 被引量：3
4Bin Lu,Hong-Duo Chen,Hong-Guang Hong-Guang.The relationship between apoptosis and aging[J].Advances in Bioscience and Biotechnology,2012,3(6):705-711. 被引量：1
5CHEN Juan,CUI Jia-jia,ZHANG Jian-ting,ZHOU Hong-hao,LIU Zhao-qian,YIN Ji-ye.Translational regulation of DNA repair systems by eIF3a in cancer chemotherapeutic response[J].中国药理学与毒理学杂志,2016,30(10):1050-1051.
6武汉大学郑从义团队在宿主细胞异质性影响病毒感染方面取得新进展[J].健康之家,2018,0(3):94-94.
7Shamim Ahmed S.K. Barbhuiya,Sumana Chakraborty,Mahuya Sengupta.Studies of lead toxicity on inflammatory damage and innate immune functions in testicular macrophages of male Swiss albino mice[J].Modern Research in Inflammation,2013,2(4):75-81.
8Adam Marks,Kees Rietsema.Airport Information Systems—Airside Management Information Systems[J].Intelligent Information Management,2014,6(3):149-156. 被引量：1
9Kazue Takahashi,Wei-Chuan Chang,Patience Moyo,Mitchell R. White,Parool Meelu,Anamika Verma,Gregory L. Stahl,Kevan L. Hartshorn,Vijay Yajnik.Dietary sugars inhibit biologic functions of the pattern recognition molecule, mannose-binding lectin[J].Open Journal of Immunology,2011,1(2):41-49.
10Irina Livshitz.Preventative Strategies in the Management of ROP: A Review of Literature[J].Open Journal of Pediatrics,2015,5(2):121-127.

World Journal of AIDS

2012年第3期

浏览历史

内容加载中请稍等...

HIV-1 Primarily Targets the Innate Immune System and Only Secondarily Modulates Adaptive Immune Cell Depletion

参考文献1

二级参考文献157

共引文献4

相关作者

相关机构

相关主题

浏览历史