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首页> 外文期刊>Mechanisms of Ageing and Development >A mouse genetic locus with death clock and life clock features.
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A mouse genetic locus with death clock and life clock features.

机译:具有死亡时钟和生命时钟功能的小鼠遗传基因座。

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摘要

A senility syndrome, with weight loss and priapism, occurs in CBAT6/T6 mice, an exceptionally long-lived strain. Instead of dying at the expected time, these mice get senile weight loss and priapism and go on living. We have postulated that a mutant death clock kills the wrong neurons. Crosses with the NZW and C57BL/6 strains show causation by a single genetic locus (Priap1), with a pronounced gene dosage effect on timing. We report here that various cancers were the cause of death in 31 of 32 NZW mice, compared to only five of 22 CBAT6/T6 mice, a highly significant difference (P<0.001). The longevity of (CBAT6/T6xNZW)F1 hybrids, and the segregation of longevity with priapism and senile weight loss in (CBAT6/T6xNZW) F2 hybrids, indicates that Priap1, or a linked gene, inhibits the cancers that usually shorten the lives of NZW mice. If a timer gene is involved, the cancer resistance action could be because the locus impedes the normal mid-life regression of anti-cancer defence. The priapism suggests loss of the medullary reticular formation neurons which normally inhibit male spinal sexual reflexes. In this region of the medulla there are also the respiratory and cardiac control centres, where apoptotic neuron destruction by the wild-type locus could govern maximal life-span. The CBAT6/T6 locus may be a mutant life-stage control clock. Its discovery could be the revelation of a new, major class of aetiology of disease.
机译:CBAT6 / T6小鼠是一种寿命长的品系,具有体重减轻和阴茎异常勃勃的衰老综合征。这些小鼠没有在预期的时间死亡,而是出现了衰老的体重减轻和阴茎异常勃起,并继续生存。我们推测,突变死亡时钟会杀死错误的神经元。与NZW和C57BL / 6菌株的杂交显示出单个遗传基因座(Priap1)的因果关系,显着的基因剂量对时间有影响。我们在这里报告说,各种癌症是32只NZW小鼠中31只的死亡原因,而22只CBAT6 / T6小鼠中只有5只,差异非常显着(P <0.001)。 (CBAT6 / T6xNZW)F1杂种的寿命长,以及(CBAT6 / T6xNZW)F2杂种的长寿与阴茎异常勃起和衰老的体重分离,表明Priap1或相关基因抑制通常会缩短NZW寿命的癌症。老鼠。如果涉及计时器基因,则抗癌作用可能是因为该基因座阻碍了抗癌防御的正常中年消退。阴茎异常勃起提示通常会抑制男性脊柱性反射的髓样网状结构神经元丢失。在延髓的这个区域,还有呼吸和心脏控制中心,野生型基因座对凋亡神经元的破坏可以控制最长的寿命。 CBAT6 / T6基因座可能是突变的生命阶段控制时钟。它的发现可能是新的主要疾病病因学的启示。

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