Reduction of unscheduled DNA synthesis and plasminogen activator activity in Hutchinson-Gilford fibroblasts during passaging in vitro: partial correction by interferon-β

Katsuo Sugita , Nobuo Suzuki , Katsunori Fujii , Hiroo Niimi
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引用次数: 8

Abstract

Two fibroblast cell lines (PG3KT and PG1NA) deruved from Hutchinson-Gilford syndrome (progeria) cases were characterized, at various population doubling levels (PDL), with respect to the capacity of ultraviolet light (UV, mainly 254 nm wavelength)-induced unschedules DNA synthesis (UDS) and plasminogen activator-like protease activity (PA). The UDS levels in PG3KT and PG1NA cells at PDL 2–3 were only slightly less than those in normal fibroblasts. With increasing PDL. both prgeria cell lines exhibited reduction of the UDS levels and undetectable ones at PDL 9–11. Prompt and transient induction of PA was also detectable at less than PDL 5, whereas it was undetectable at higher PDL. However, the levels of UDS and PA induction were increased about 3–7 times after pretreatment with 100 IU/ml human interferon (HuIFN)-β preparations for more than 24 h prior to UV irradiation, although UDS and PA were undetectable at more than PDL 10. These results suggest that cytokines such as HuIFN-β transiently compensate for the decreases in UDS and PA inducibility in progeria cells with aging.

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体外传代过程中Hutchinson-Gilford成纤维细胞非计划DNA合成和纤溶酶原激活物活性的减少:干扰素-β的部分纠正
从Hutchinson-Gilford综合征(早衰症)患者中提取的两种成纤维细胞系(PG3KT和PG1NA),在不同的群体翻倍水平(PDL)下,对紫外光(UV,主要是254 nm波长)诱导的非排程DNA合成(UDS)和纤溶酶原激活物样蛋白酶活性(PA)进行了表征。PDL 2 ~ 3段PG3KT和PG1NA细胞的UDS水平仅略低于正常成纤维细胞。随着PDL的增加。两种早衰细胞系均表现出UDS水平的降低和PDL 9-11的检测不到。在低于PDL 5的情况下,也可检测到PA的快速和瞬时诱导,而在较高的PDL下则无法检测到。然而,在紫外线照射前,用100 IU/ml人干扰素(HuIFN)-β制剂预处理24 h后,UDS和PA诱导水平增加了约3-7倍,尽管UDS和PA在PDL 10以上无法检测到。这些结果表明,随着年龄的增长,HuIFN-β等细胞因子暂时补偿了UDS和PA诱导能力的下降。
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