Dnaja3-Tp53 Double Deletion Drives Nash-Hcc Progression with Sex Disparity: Mechanistic Insights and Therapeutic Implications

Chang, Ching-Wen (PI)

Graduate Institute of Metabolism and Obesity Sciences

Project: A - Government Institution › b - National Science and Technology Council

Description

本計畫旨在探討TP53基因突變與粒線體功能障礙在非酒精性脂肪性肝炎（NASH）導致的肝細胞癌（HCC）發展中的角色，特別考量性別因素對疾病進程的影響。我們將透過肝細胞特異性Dnaja3/P53雙基因剔除（DKO）小鼠模型，剖析NASH相關HCC中性別特異性腫瘤發展的複雜機制。研究將對於促進男性和女性患者的精準治療提供重要資訊，並探索以性激素及粒線體功能作為標靶的治療新策略。

Status	Finished
Effective start/end date	4/1/24 → 7/31/25

Keywords

DnaJ Heat Shock Protein Family (Hsp40) Member A3 (Dnaja3)
Mitochondrial chaperone Hsp40 (HSP40)
TP53 mutation
double knockout (DKO) mouse model
nonalcoholic steatohepatitis (NASH)
Sex Disparity
Hepatocellular carcinoma (HCC)

Dnaja3-Tp53 Double Deletion Drives Nash-Hcc Progression with Sex Disparity: Mechanistic Insights and Therapeutic Implications

Project Details

Description

Keywords