Mice deficient in the candidate tumor suppressor gene Hic1 exhibit developmental defects of structures affected in the Miller-Dieker syndrome.

Carter MG; Johns MA; Zeng X; Zhou L; Zink MC; Mankowski JL; Donovan DM; Baylin SB

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Mice deficient in the candidate tumor suppressor gene Hic1 exhibit developmental defects of structures affected in the Miller-Dieker syndrome.

机译：候选肿瘤抑制基因Hic1缺乏的小鼠表现出受米勒-迪克综合症影响的结构的发育缺陷。

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HIC1 is a candidate tumor suppressor gene which is frequently hypermethylated in human tumors, and its location within the Miller-Dieker syndrome's critical deletion region at chromosome 17p13.3 makes it a candidate gene for involvement in this gene deletion syndrome. To study the function of murine Hic1 in development, we have created Hic1 -deficient mice. These animals die perinatally and exhibit varying combinations of gross developmental defects throughout the second half of development, including acrania, exencephaly, cleft palate, limb abnormalities and omphalocele. These findings demonstrate a role for Hic1 in the development of structures affected in the Miller-Dieker syndrome, and provide functional evidence to strengthen its candidacy as a gene involved in this disorder.

机译：HIC1是一种候选抑癌基因，在人类肿瘤中经常甲基化，并且它在Miller-Dieker综合征的17p13.3染色体关键缺失区域内的位置使其成为参与该基因缺失综合征的候选基因。为了研究鼠Hic1在发育中的功能，我们创建了Hic1缺陷小鼠。这些动物在围产期死亡，并且在整个发育的后半段表现出各种发育缺陷的组合，包括头皮萎缩症，运动障碍、,裂，肢体畸形和卵裂。这些发现证明了Hic1在受Miller-Dieker综合征影响的结构发展中的作用，并提供了功能证据来增强其作为该疾病相关基因的候选资格。

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《Human Molecular Genetics》 |2000年第3期|共7页
作者
Carter MG; Johns MA; Zeng X; Zhou L; Zink MC; Mankowski JL; Donovan DM; Baylin SB;
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正文语种 eng
中图分类医学遗传学;
关键词
Genes; Suppressor; Tumor; Transcription Factors; transcription factor HIC-1; 基因; 抑制; 肿瘤; 转录因子;

机译：Genes;Suppressor;Tumor;Transcription Factors;transcription factor HIC-1;基因;抑制;肿瘤;转录因子;

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1. Mice deficient in the candidate tumor suppressor gene Hic1 exhibit developmental defects of structures affected in the Miller-Dieker syndrome. [J] . Carter MG, Johns MA, Zeng X, Human Molecular Genetics . 2000,第3期

机译：候选肿瘤抑制基因Hic1缺乏的小鼠表现出受米勒-迪克综合症影响的结构的发育缺陷。
2. Array comparative genomic hybridization characterization of a 3.3-Mb 17p13.3-p13.2 deletion encompassing YWHAE , CRK , HIC1 and PAFAH1B1 in an 8-year-old girl with Miller-Dieker lissencephaly syndrome, congenital heart defects, growth restriction and developmental delay [J] . Chih-Ping Chen, Shu-Yuan Chang, Shuan-Pei Lin, Taiwanese journal of obstetrics and gynecology . 2018,第5期

机译：阵列比较基因组杂交表征一个8岁女孩Miller-Dieker lissencephaly综合征，先天性心脏缺陷，生长受限和发育延迟的3.3-Mb 17p13.3-p13.2缺失，包括YWHAE，CRK，HIC1和PAFAH1B1
3. YWHAE , CRK , HIC1 and PAFAH1B1 in an 8-year-old girl with Miller-Dieker lissencephaly syndrome, congenital heart defects, growth restriction and developmental delay [J] . Chih-Ping Chen, Shu-Yuan Chang, Shuan-Pei Lin, Taiwanese journal of obstetrics and gynecology . 2018,第5期

机译：Ywhae，Crk，Hic1和Pafah1b1在一个8岁的女孩，米勒死牌展示症综合征，先天性心脏缺陷，增长限制和发育延迟
4. Identification of candidate tumor suppressor genes from critical deletions of long arm of chromosome 6 in hematopoietic neoplasm [C] . Seishi Ogawa, Akira Hangaishi, Hisamaru Hirai Uehara Memorial Foundation Symposium on Genome Science . 2002

机译：鉴定致染色体肿瘤长臂临时缺失造血肿瘤的临界肿瘤抑制基因
5. Genome-wide identification of novel candidate tumor suppressor genes in Hong Kong common tumors through integrative cancer epigenetics and genomics. [D] . Ying, Jianming. 2007

机译：通过综合的癌症表观遗传学和基因组学，全基因组鉴定香港常见肿瘤中的新型候选肿瘤抑制基因。
6. Small mitochondrial Arf (smArf) protein corrects p53-independent developmental defects of Arf tumor suppressor-deficient mice [O] . Jolieke G. van Oosterwijk, Chunliang Li, Xue Yang, 2017

机译：线粒体Arf（smArf）小蛋白可纠正Arf抑癌基因缺陷小鼠的p53独立发育缺陷
7. Mice deficient in the candidate tumor suppressor gene Hic1 exhibit developmental defects of structures affected in the Miller-Dieker syndrome [O] . M. G. Carter 2000

机译：候选肿瘤抑制基因HIC1缺乏的小鼠表现出在Miller-Dieger综合征中受影响的结构的发育缺陷

Mice deficient in the candidate tumor suppressor gene Hic1 exhibit developmental defects of structures affected in the Miller-Dieker syndrome.

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