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抗糖蛋白41而非抗糖蛋白120免疫毒素在HIV感染小鼠模型中的体内疗效。

In vivo efficacy of anti-glycoprotein 41, but not anti-glycoprotein 120, immunotoxins in a mouse model of HIV infection.

作者信息

Pincus Seth H, Fang Hua, Wilkinson Royce A, Marcotte Tamera K, Robinson James E, Olson William C

机构信息

Department of Microbiology and Animal Resources Center, Montana State University, Bozeman, MT 59717, USA.

出版信息

J Immunol. 2003 Feb 15;170(4):2236-41. doi: 10.4049/jimmunol.170.4.2236.

Abstract

Immunotoxins (ITs) targeting the HIV envelope protein are among the most efficacious antiviral therapies when tested in vitro. Yet a first-generation IT targeted to gp120, CD4-PE40 (chimeric immunotoxin using CD4 and the translocation and enzymatic domains of Pseudomonas exotoxin A), showed limited promise in initial clinical testing, highlighting the need for improved ITs. We have used a new mouse model of HIV infection to test the comparative efficacy of anti-HIV ITs targeted to gp120 or to gp41. Irradiated SCID/nonobese diabetic mice are injected with a tumor of human CD4(+) cells susceptible to infection and at a separate site persistently HIV-infected cells. The spread of infection from infected to susceptible tumor is monitored by plasma p24 and the presence of HIV-infected cells in the spleen. Anti-gp41 ITs in combination with tetrameric CD4-human Ig fusion protein have pronounced anti-HIV effects. Little if any anti-HIV efficacy was found with either CD4-PE40 or an Ab-targeted anti-gp120 IT. These data support continued exploration of the utility of ITs for HIV infection, particularly the use of anti-gp41 ITs in combination with soluble CD4 derivatives.

摘要

在体外试验中,靶向HIV包膜蛋白的免疫毒素(ITs)是最有效的抗病毒疗法之一。然而,第一代靶向gp120的IT,即CD4-PE40(使用CD4以及绿脓杆菌外毒素A的易位和酶结构域的嵌合免疫毒素),在初始临床试验中显示出有限的前景,这突出了改进ITs的必要性。我们使用一种新的HIV感染小鼠模型来测试靶向gp120或gp41的抗HIV ITs的相对疗效。给经辐照的SCID/非肥胖糖尿病小鼠注射易受感染的人CD4(+)细胞肿瘤,并在另一个部位注射持续感染HIV的细胞。通过血浆p24以及脾脏中HIV感染细胞的存在情况来监测感染从受感染肿瘤向易感肿瘤的传播。抗gp41 ITs与四聚体CD4-人Ig融合蛋白联合使用具有显著的抗HIV作用。无论是CD4-PE40还是抗体靶向的抗gp120 IT,几乎都未发现抗HIV疗效。这些数据支持继续探索ITs在HIV感染治疗中的效用,特别是抗gp41 ITs与可溶性CD4衍生物联合使用的效用。

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