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衰老加速小鼠(SAM):一种新型的衰老小鼠模型。

Senescence-accelerated mouse (SAM): a novel murine model of senescence.

作者信息

Takeda T, Hosokawa M, Higuchi K

机构信息

Department of Senescence Biology, Kyoto University, Japan.

出版信息

Exp Gerontol. 1997 Jan-Apr;32(1-2):105-9. doi: 10.1016/s0531-5565(96)00036-8.

Abstract

The Senescence-Accelerated Mouse (SAM) has been under development by our research team at Kyoto University since 1970 through the selective inbreeding of the AKR/J strain of mice donated by the Jackson Laboratory in 1968, based on a graded score for senescence, life span, and pathologic phenotype. At present, there are 12 lines of SAM: nine senescence-prone inbred strains (SAMP) including SAMP1, SAMP2, SAMP3, SAMP6, SAMP7, SAMP8, SAMP9, SAMP10, and SAMP11; and three senescence-resistant inbred strains (SAMR) including SAMR1, SAMR4, and SAMR5. Data from survival curves, Gompertzian function, and grading score of senescence, together with growth patterns of body weight of these SAMP and SAMR, revealed that the characteristic feature of aging common to all SAMP mice is "accelerated senescence;" early onset and irreversible advance of senescence manifested by several signs and gross lesions such as the loss of normal behavior, various skin lesions, increased lordokyphosis, etc., after a period of normal development. In the course of SAM development, it became evident that SAMP strains manifest various pathologic phenotypes that are characteristic enough to differentiate the SAM strains. The genetic background and significance of SAM development are discussed.

摘要

自1970年以来,京都大学的研究团队通过对1968年由杰克逊实验室捐赠的AKR/J品系小鼠进行选择性近亲繁殖,基于衰老、寿命和病理表型的分级评分,培育出了衰老加速小鼠(SAM)。目前,SAM有12个品系:9个衰老易感性近交系(SAMP),包括SAMP1、SAMP2、SAMP3、SAMP6、SAMP7、SAMP8、SAMP9、SAMP10和SAMP11;以及3个衰老抗性近交系(SAMR),包括SAMR1、SAMR4和SAMR5。这些SAMP和SAMR的生存曲线、冈珀茨函数、衰老分级评分数据,以及体重增长模式显示,所有SAMP小鼠衰老的共同特征是“加速衰老”;在一段正常发育后,衰老以早期发作且不可逆转的方式推进,表现为多种体征和大体病变,如正常行为丧失、各种皮肤病变、脊柱后凸增加等。在SAM的培育过程中,很明显SAMP品系表现出各种具有足够特征性以区分SAM品系的病理表型。本文讨论了SAM培育的遗传背景及意义。

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