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小鼠肉瘤病毒(MSV)诱导的AKR小鼠肿瘤的遗传学:晚期进展性肿瘤和早期消退性肿瘤受不同基因控制的证据。

Genetics of murine sarcoma virus (MSV)--induced tumors in AKR mice: Evidence that late progressing and early regressing tumors are controlled by different gents.

作者信息

Colombatti A, Chieco-Bianchi L, De Rossi A, D'Andrea E, Collavo D

出版信息

Int J Cancer. 1977 Apr 15;19(4):565-75. doi: 10.1002/ijc.2910190418.

Abstract

The genetics of late appearing MSV tumors showing a progressive growth pattern in AKR mice was investigated. The late MSV tumor response in F1 hybrids depended on the genetic background of the non-AKR parent. Within the 4-month observation period following virus injection, (CBA X AKR) F1, (DBA/2 X AKR)F1, and (NIH X AKR)F1 developed progressing MSV tumors, which exhibited latency and growth behavior comparable to that seen in AKR mice, (BALB X AKR)F1, (B6 X AKR)F1, and (B10br x akr)f1 mice did not show any late MSV tumors. In contrast to early regressing M-MSV tumors, whose development is independent of Fv-1 genotype, late MSV tumor progression is largely a function of this gene, since all late tumors which appeared in (B10BR x AKR) x AKR were observed in Fv-1n homozygous mice, H-2k halotype is a further factor in the occurrence of late MSV tumors, at least in (B6 x AKR) x AKR mice. In crosses of AKR with Fv-1 compatible mice, tumor appearance was strongly associated with inheritance of AKR-Mulv, and MSV recovered from late tumors of first back-cross animals appeared to be a new pseudotype with the endogenous AKR-MuLV. It is suggested that the host genetic control in both early and late MSV tumors is exerted mainly on the helper component of the leukemia-sarcoma complex.

摘要

对在AKR小鼠中呈现渐进性生长模式的晚期出现的MSV肿瘤的遗传学进行了研究。F1代杂种小鼠对晚期MSV肿瘤的反应取决于非AKR亲本的遗传背景。在注射病毒后的4个月观察期内,(CBA×AKR)F1、(DBA/2×AKR)F1和(NIH×AKR)F1出现了进行性MSV肿瘤,其潜伏期和生长行为与AKR小鼠中的情况相当,(BALB×AKR)F1、(B6×AKR)F1和(B10br×akr)F1小鼠未出现任何晚期MSV肿瘤。与早期消退的M-MSV肿瘤不同,其发展与Fv-1基因型无关,晚期MSV肿瘤的进展在很大程度上是该基因的作用,因为在(B10BR×AKR)×AKR中出现的所有晚期肿瘤均在Fv-1n纯合小鼠中观察到,H-2k单倍型是晚期MSV肿瘤发生的另一个因素,至少在(B6×AKR)×AKR小鼠中是这样。在AKR与Fv-1兼容小鼠的杂交中,肿瘤出现与AKR-Mulv的遗传密切相关,并且从第一代回交动物的晚期肿瘤中回收的MSV似乎是一种与内源性AKR-MuLV相关的新假型。有人提出,宿主对早期和晚期MSV肿瘤的遗传控制主要作用于白血病-肉瘤复合体的辅助成分。

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