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<博士論文>
Wild-Type p53-Induced Phosphatase 1の乳癌における臨床的意義

Clinical Significance of the Wild Type p53-Induced Phosphatase 1 Expression in Invasive Breast Cancer
作成者
作成者姓名
井上, 有香
Inoue, Yuka
イノウエ, ユカ
論文調査委員
岩城, 徹
中村, 雅史
康, 東天
本文言語
英語
学位授与年度
2017
学位授与大学
九州大学
Kyushu University
学位
博士(医学)
学位種別
課程博士
出版タイプ
Version of Record
アクセス権
open access
JaLC DOI
https://doi.org/10.15017/1931817
関連DOI
https://doi.org/10.1016/j.clbc.2017.11.008
概要 BACKGROUND:Wild type p53-induced phosphatase 1 (Wip1), encoded by the protein phosphatase magnesium dependent 1 delta (PPM1D), inhibits p53. PPM1D amplification has been reported in breast cancer. Bre...ast cancer can sometimes develop without a tumor protein 53 (TP53) mutation. In these cases, the p53 pathway might be disrupted by alternative mechanisms, and Wip1 is reported to be a key molecule involved.
MATERIALS AND METHODS:Primary invasive ductal carcinoma specimens were obtained from 201 cases, for which archival tissue samples for immunohistochemistry were available. We evaluated Wip1 and p21 protein expression (201 cases), Wip1 mRNA expression (63 cases), PPM1D DNA copy number (71 cases) and TP53 status (36 cases) using available samples among the 201 cases, and analyzed their relationships with clinicopathological factors and prognosis.
RESULTS:The nuclear expression of Wip1 protein was positive in 21 cases (10.4%). The PPM1D DNA copy number was significantly correlated with Wip1 protein expression. All cases with PPM1D amplification by single-nucleotide polymorphism comparative genomic hybridization array showed positive nuclear Wip1 expression. Wip1 protein expression was positively correlated with p21 expression. The tumors with positive Wip1 and negative p21 expression showed the poorest prognosis among all tumor types.
CONCLUSION:The protein expression of Wip1 might be regulated by PPM1D amplification, independent of TP53 status. Positive Wip1 and negative p21 expression was associated with the poorest prognosis and suggests the loss of p53 function.続きを見る

本文ファイル

pdf med3131 pdf 1.98 MB 654 本文
pdf med3131_abstract pdf 106 KB 190 要旨
pdf med3131_review pdf 161 KB 209 審査結果要旨

詳細

レコードID
1931817
査読有無
査読有
権利関係
(C) 2017 Elsevier Inc. All rights reserved
関連PubMed ID
29275106
報告番号
17102甲第13964号
学位記番号
医博甲第3131号
授与日(学位/助成/特許)
2018-03-31
受理日
2018-03-02
部局
医博
登録日 2018.05.30
更新日 2020.01.31

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