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Mutation analysis of p31comet gene, a negative regulator of Mad2, in human hepatocellular carcinoma
被引:0
|作者:
Mi-Yong Yun
Sang Bum Kim
Sunhoo Park
Chul Ju Han
Young-Hoon Han
Sun Hee Yoon
Sang Hoon Kim
Chang-Min Kim
Dong-Wook Choi
Myung-Haing Cho
Gil-Hong Park
Kee-Ho Lee
机构:
[1] Korea Institute of Radiological and Medical Sciences,Laboratory of Radiation Molecular Oncology, Division of Radiation Cancer Biology
来源:
关键词:
carcinoma, hepatocellular;
MAD2L1 protein, human;
mitosis;
mutation;
D O I:
暂无
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学科分类号:
摘要:
Failure of mitotic checkpoint machinery leads to the chromosomal missegregation and nuclear endoreduplication, thereby driving the emergence of aneuploidy and tetraploidy population. Although abnormal nuclear ploidy and the resulting impairment of mitotic checkpoint function are typical physiological event leading to human hepatocellular carcinoma, any mutational change of mitotic checkpoint regulators has not yet been discovered. Therefore, we investigated the mutation of p31comet, a recently identified mitotic checkpoint regulator, in human hepatocellular carcinoma. Of 51 human hepatocellular carcinoma tissue and 6 cell lines tested, five samples exhibited nucleotide sequence variations dispersed on four sites within the entire coding sequence. Among these sites with sequence substitutions, three were found to be missense mutation accompanied with amino acid change but one was a silent mutation. Of these sequence substitutions, two were present in both tumor and non-tumor liver tissues, suggesting the possibility of polymorphism. The present findings indicate that p31comet does not have an impact on the formation of aneuploidy and tetraploidy found in human hepatocellular carcinoma.
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页码:508 / 513
页数:5
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