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Genome-wide analysis of cutaneous T-cell lymphomas identifies three clinically relevant classes.对皮肤 T 细胞淋巴瘤的全基因组分析确定了三个具有临床意义的类别。
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2
Identification of key regions and genes important in the pathogenesis of sezary syndrome by combining genomic and expression microarrays.通过结合基因组和表达微阵列鉴定蕈样肉芽肿综合征发病机制中重要的关键区域和基因。
Cancer Res. 2009 Nov 1;69(21):8438-46. doi: 10.1158/0008-5472.CAN-09-2367. Epub 2009 Oct 20.
3
Downregulation of Fas gene expression in Sézary syndrome is associated with promoter hypermethylation.Fas 基因表达下调与 Sézary 综合征中启动子超甲基化有关。
J Invest Dermatol. 2010 Apr;130(4):1116-25. doi: 10.1038/jid.2009.301. Epub 2009 Sep 17.
4
Polymorphisms in the FAS and FASL genes and survival of early stage non-small cell lung cancer.FAS和FASL基因多态性与早期非小细胞肺癌的生存率
Clin Cancer Res. 2009 Mar 1;15(5):1794-800. doi: 10.1158/1078-0432.CCR-08-1770. Epub 2009 Feb 24.
5
Low FAS/CD95 expression by CTCL correlates with reduced sensitivity to apoptosis that can be restored by FAS upregulation.蕈样肉芽肿中低FAS/CD95表达与凋亡敏感性降低相关,而FAS上调可恢复这种敏感性。
J Invest Dermatol. 2009 May;129(5):1165-73. doi: 10.1038/jid.2008.309. Epub 2008 Oct 16.
6
Genetic variation in genes expressed in the germinal center and risk of B cell lymphoma among Caucasians.生发中心表达基因的遗传变异与高加索人群B细胞淋巴瘤风险
Haematologica. 2008 Oct;93(10):1597-600. doi: 10.3324/haematol.13159. Epub 2008 Jul 18.
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Protocols for cytogenetic studies of human embryonic stem cells.人类胚胎干细胞的细胞遗传学研究方案。
Methods. 2008 Jun;45(2):133-41. doi: 10.1016/j.ymeth.2008.03.005. Epub 2008 Jun 2.
8
Resistance to FasL and tumor necrosis factor-related apoptosis-inducing ligand-mediated apoptosis in Sezary syndrome T-cells associated with impaired death receptor and FLICE-inhibitory protein expression.蕈样肉芽肿T细胞中对FasL和肿瘤坏死因子相关凋亡诱导配体介导的凋亡产生抗性,这与死亡受体和FLICE抑制蛋白表达受损有关。
Blood. 2008 May 1;111(9):4780-7. doi: 10.1182/blood-2007-08-109074. Epub 2008 Feb 26.
9
Fas 670 promoter polymorphism is associated to susceptibility, clinical presentation, and survival in adult T cell leukemia.Fas 670启动子多态性与成人T细胞白血病的易感性、临床表现及生存率相关。
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10
Incidence of cutaneous T-cell lymphoma in the United States, 1973-2002.1973 - 2002年美国皮肤T细胞淋巴瘤的发病率
Arch Dermatol. 2007 Jul;143(7):854-9. doi: 10.1001/archderm.143.7.854.

皮肤 T 细胞淋巴瘤(CTCL)中 FAS 基因的结构改变。

Structural alterations of the FAS gene in cutaneous T-cell lymphoma (CTCL).

机构信息

Department of Dermatology, University of Wisconsin and VAMC, Madison, WI, United States.

出版信息

Arch Biochem Biophys. 2011 Apr 15;508(2):185-91. doi: 10.1016/j.abb.2010.10.020. Epub 2010 Oct 29.

DOI:10.1016/j.abb.2010.10.020
PMID:21036138
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3060968/
Abstract

FAS (TNF receptor superfamily member 6, also known as CD95) plays a major role in T-cell apoptosis and is often dysregulated in CTCL. We searched for structural alterations of the FAS gene with the potential to affect its function. Although several heterozygous FAS promoter single nucleotide polymorphisms (SNPs) were detected, the only homozygous one was the -671 GG SNP present in 24/80 CTCL cases (30%). This SNP maps to an interferon response element activated by STAT-1. EMSA and supershift EMSA showed decreased CTCL nuclear protein/STAT-1 binding to oligonucleotides bearing this SNP. Luciferase reporters showed significantly less interferon-alfa responsive expression by FAS promoter constructs containing this SNP in multiple CTCL lines. Finally, FAS was upregulated by interferon-alfa in wildtype CTCL cells but not those bearing the -671 GG SNP. These findings indicate that many CTCL patients harbor the homozygous FAS promoter -671 GG SNP capable of blunting its response to interferon. This may have implications for CTCL pathogenesis, racial incidence and the response of patients to interferon-alfa therapy. In contrast, functionally significant mutations in FAS coding sequences were detected uncommonly. Among CTCL lines with the potential to serve as models of FAS regulation, FAS-high MyLa had both FAS alleles, FAS-low HH was FAS-hemizygous and FAS-negative SeAx was FAS-null.

摘要

FAS(肿瘤坏死因子受体超家族成员 6,也称为 CD95)在 T 细胞凋亡中起主要作用,并且在 CTCL 中经常失调。我们搜索了具有潜在影响其功能的 FAS 基因结构改变。尽管检测到几种杂合 FAS 启动子单核苷酸多态性(SNP),但唯一的纯合 SNP 是存在于 24/80 例 CTCL 病例中的 -671 GG SNP(30%)。该 SNP 映射到由 STAT-1 激活的干扰素反应元件。EMSA 和超迁移 EMSA 显示,具有该 SNP 的寡核苷酸的 CTCL 核蛋白/STAT-1 结合减少。荧光素酶报告显示,包含该 SNP 的多个 CTCL 系中,FAS 启动子构建体的干扰素-α反应表达显着减少。最后,野生型 CTCL 细胞中干扰素-α上调了 FAS,但不具有 -671 GG SNP 的细胞则不行。这些发现表明,许多 CTCL 患者携带有能够使其对干扰素反应迟钝的纯合 FAS 启动子 -671 GG SNP。这可能对 CTCL 的发病机制、种族发生率以及患者对干扰素-α治疗的反应产生影响。相比之下,在 FAS 编码序列中检测到功能上重要的突变并不常见。在具有 FAS 调节模型潜力的 CTCL 系中,FAS-高 MyLa 具有两个 FAS 等位基因,FAS-低 HH 是 FAS 半合子,FAS-阴性 SeAx 是 FAS 缺失。