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人类TP53基因的变异会影响老年生存率和癌症死亡率。

Variation in the human TP53 gene affects old age survival and cancer mortality.

作者信息

van Heemst Diana, Mooijaart Simon P, Beekman Marian, Schreuder Jeroen, de Craen Anton J M, Brandt Bernd W, Slagboom P Eline, Westendorp Rudi G J

出版信息

Exp Gerontol. 2005 Jan-Feb;40(1-2):11-5. doi: 10.1016/j.exger.2004.10.001.

DOI:10.1016/j.exger.2004.10.001
PMID:15732191
Abstract

Longevity may depend on a balance between tumor suppression and tissue renewal mechanisms [Campisi, J., 2003. Cancer and ageing: rival demons? Nat. Rev. Cancer 3 (5), 339-349]. Mice with constitutively activated p53 are almost cancer free but their life span is reduced and accompanied by early tissue atrophy [Tyner et al., 2002. p53 mutant mice that display early ageing-associated phenotypes. Nature 415 (6867) 45-53]. Replacement of arginine (Arg) by proline (Pro) at position 72 of human p53 decreases its apoptotic potential [Dumont et al., 2003. The codon 72 polymorphic variants of p53 have markedly different apoptotic potential. Nat. Genet. 33 (3), 357-365] providing a tool to test for a similar trade-off in humans. Using a formal meta-analysis of the published literature we show that carriers of the TP53 codon 72 Pro/Pro genotype have an increased cancer risk compared to Arg/Arg carriers (p<0.05). Next, in a prospective study of 1226 people aged 85 years and over we show that carriers of the Pro/Pro genotype have a 41% increased survival (p = 0.032) despite a 2.54 fold increased (p = 0.007) proportional mortality from cancer. It is suggested that human p53 protect against cancer but at a cost of longevity.

摘要

长寿可能取决于肿瘤抑制和组织更新机制之间的平衡[坎皮西,J.,2003年。癌症与衰老:相互竞争的恶魔?《自然综述:癌症》3(5),339 - 349]。p53持续激活的小鼠几乎没有癌症,但它们的寿命缩短,并伴有早期组织萎缩[泰纳等人,2002年。表现出早期衰老相关表型的p53突变小鼠。《自然》415(6867)45 - 53]。人类p53第72位的精氨酸(Arg)被脯氨酸(Pro)取代会降低其凋亡潜力[杜蒙等人,2003年。p53密码子72的多态性变体具有明显不同的凋亡潜力。《自然遗传学》33(3),357 - 365],这为测试人类中类似的权衡提供了一个工具。通过对已发表文献进行正式的荟萃分析,我们发现与Arg/Arg携带者相比,TP53密码子72 Pro/Pro基因型的携带者患癌风险增加(p<0.05)。接下来,在一项对1226名85岁及以上人群的前瞻性研究中,我们发现尽管Pro/Pro基因型携带者因癌症导致的比例死亡率增加了2.54倍(p = 0.007),但其生存率提高了41%(p = 0.032)。这表明人类p53能预防癌症,但要以长寿为代价。

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