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一种B型逆转录病毒在胸腺淋巴瘤诱导中的作用。

The involvement of a type-B retrovirus in the induction of thymic lymphomas.

作者信息

Ball J K, Arthur L O, Dekaban G A

出版信息

Virology. 1985 Jan 15;140(1):159-72. doi: 10.1016/0042-6822(85)90455-6.

Abstract

A highly leukemogenic virus (DMBA-LV) (in vivo leukemogenic titer 1-5 X 10(6) IU/ml, and 35-40 days to thymic lymphoma detection) is produced by a chemical carcinogen-induced transplanted thymic lymphoma. The virus preparation is a mixture of a type-B retrovirus highly related to exogenous type-B retroviral isolates and a biologically defective type-C retrovirus. The DNA of DMBA-LV-induced-tumors contains new type-B proviruses but no additional type-C proviruses could be detected. The leukemogenicity of DMBA-LV was completely neutralized by a monoclonal antibody against MMTV envelope glycoprotein, but was not affected by a broadly reacting Friend MuLV anti-gp70 serum which effectively neutralizes type-C ecotropic, xenotropic, and recombinant retroviruses and which completely abolishes the leukemogenic activity of Moloney leukemia virus. Three type-B mammary tumor-inducing retroviral isolates, while containing type-C retroviral sequences, were not leukemogenic. A further characterization of the type-C retroviral sequences present in DMBA-LV indicated that sequences characteristic of endogenous, nonxenotropic proviruses are present. In addition, using a variety of type-C-specific retroviral DNA probes, no evidence was obtained for the presence of a type-B-C-recombinant genome in DMBA-LV. Leukemogenesis was absolutely dependent upon the presence of a functional type-B retroviral envelope gp 52 and DMBA-LV does not appear to contain a leukemogenic retroviral type-C genome.

摘要

一种高度致白血病病毒(DMBA-LV)(体内致白血病滴度为1 - 5×10⁶ IU/ml,检测到胸腺淋巴瘤需35 - 40天)由化学致癌物诱导的移植性胸腺淋巴瘤产生。该病毒制剂是一种与外源性B型逆转录病毒分离株高度相关的B型逆转录病毒和一种生物学缺陷型C型逆转录病毒的混合物。DMBA-LV诱导肿瘤的DNA含有新型B型前病毒,但未检测到额外的C型前病毒。DMBA-LV的致白血病性被抗MMTV包膜糖蛋白的单克隆抗体完全中和,但不受能有效中和C型亲嗜性、异嗜性和重组逆转录病毒并完全消除莫洛尼白血病病毒致白血病活性的广泛反应性Friend MuLV抗gp70血清的影响。三种诱导乳腺肿瘤的B型逆转录病毒分离株虽含有C型逆转录病毒序列,但不具有致白血病性。对DMBA-LV中存在的C型逆转录病毒序列的进一步表征表明存在内源性、非异嗜性前病毒的特征序列。此外,使用多种C型特异性逆转录病毒DNA探针,未获得DMBA-LV中存在B-C重组基因组的证据。白血病发生绝对依赖于功能性B型逆转录病毒包膜gp 52的存在,且DMBA-LV似乎不包含致白血病的C型逆转录病毒基因组。

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