The aberrant upregulation of exon 10-inclusive SREK1 through SRSF10 acts as an oncogenic driver in human hepatocellular carcinoma

Cunjie Chang; Muthukumar Rajasekaran; Yiting Qiao; Heng Dong; Yu Wang; Hongping Xia; Amudha Deivasigamani; Minjie Wu; Karthik Sekar; Hengjun Gao; Mengqing Sun; Yuqin Niu; Qian Li; Lin Tao; Zhen Yan; Menglan Wang; Shasha Chen; Shujuan Zhao; Dajing Chen; Lina Li; Fan Yang; Haojin Gao; Baodong Chen; Ling Su; Liang Xu; Ye Chen; Veerabrahma Pratap Seshachalam; Gongxing Chen; Jayantha Gunaratne; Wanjin Hong; Junping Shi; Gongying Chen; David S. Grierson; Benoit Chabot; Tian Xie; Kam Man Hui; Jianxiang Chen

doi:10.1038/s41467-022-29016-x

The aberrant upregulation of exon 10-inclusive SREK1 through SRSF10 acts as an oncogenic driver in human hepatocellular carcinoma

Cunjie Chang
, Muthukumar Rajasekaran
, Yiting Qiao
, Heng Dong
, Yu Wang
, Hongping Xia
, Amudha Deivasigamani
, Minjie Wu
, Karthik Sekar
, Hengjun Gao
, Mengqing Sun
, Yuqin Niu
, Qian Li
, Lin Tao
, Zhen Yan
, Menglan Wang
, Shasha Chen
, Shujuan Zhao
, Dajing Chen
, Lina Li

Fan Yang, Haojin Gao, Baodong Chen, Ling Su, Liang Xu, Ye Chen, Veerabrahma Pratap Seshachalam, Gongxing Chen, Jayantha Gunaratne, Wanjin Hong, Junping Shi, Gongying Chen, David S. Grierson, Benoit Chabot, Tian Xie, Kam Man Hui, Jianxiang Chen

医学部

The Affiliated Hospital of Hangzhou Normal University
Hangzhou Normal University
National Cancer Centre
Zhejiang University
Shandong University
Shihezi University
Taizhou Cancer Hospital
National University of Singapore
Agency for Science, Technology and Research, Singapore
University of British Columbia
Université de Sherbrooke
Duke-NUS Medical School

科研成果: 期刊稿件 › 文章 › 同行评审

36 引用（Scopus）

摘要

Deregulation of alternative splicing is implicated as a relevant source of molecular heterogeneity in cancer. However, the targets and intrinsic mechanisms of splicing in hepatocarcinogenesis are largely unknown. Here, we report a functional impact of a Splicing Regulatory Glutamine/Lysine-Rich Protein 1 (SREK1) variant and its regulator, Serine/arginine-rich splicing factor 10 (SRSF10). HCC patients with poor prognosis express higher levels of exon 10-inclusive SREK1 (SREK1^L). SREK1^L can sustain BLOC1S5-TXNDC5 (B-T) expression, a targeted gene of nonsense-mediated mRNA decay through inhibiting exon-exon junction complex binding with B-T to exert its oncogenic role. B-T plays its competing endogenous RNA role by inhibiting miR-30c-5p and miR-30e-5p, and further promoting the expression of downstream oncogenic targets SRSF10 and TXNDC5. Interestingly, SRSF10 can act as a splicing regulator for SREK1^L to promote hepatocarcinogenesis via the formation of a SRSF10-associated complex. In summary, we demonstrate a SRSF10/SREK1^L/B-T signalling loop to accelerate the hepatocarcinogenesis.

源语言	英语
文章编号	1363
期刊	Nature Communications
卷	13
期	1
DOI	https://doi.org/10.1038/s41467-022-29016-x
出版状态	已出版 - 12月 2022

联合国可持续发展目标

此成果有助于实现下列可持续发展目标：

可持续发展目标 3 良好健康与福祉

访问文件

10.1038/s41467-022-29016-x

其它文件与链接

链接到 Scopus 的出版物

引用此

Chang, C., Rajasekaran, M., Qiao, Y., Dong, H., Wang, Y., Xia, H., Deivasigamani, A., Wu, M., Sekar, K., Gao, H., Sun, M., Niu, Y., Li, Q., Tao, L., Yan, Z., Wang, M., Chen, S., Zhao, S., Chen, D., ... Chen, J. (2022). The aberrant upregulation of exon 10-inclusive SREK1 through SRSF10 acts as an oncogenic driver in human hepatocellular carcinoma. Nature Communications, 13(1), 文章 1363. https://doi.org/10.1038/s41467-022-29016-x

@article{00a17c22260c4651bccb4e369dfae589,

title = "The aberrant upregulation of exon 10-inclusive SREK1 through SRSF10 acts as an oncogenic driver in human hepatocellular carcinoma",

abstract = "Deregulation of alternative splicing is implicated as a relevant source of molecular heterogeneity in cancer. However, the targets and intrinsic mechanisms of splicing in hepatocarcinogenesis are largely unknown. Here, we report a functional impact of a Splicing Regulatory Glutamine/Lysine-Rich Protein 1 (SREK1) variant and its regulator, Serine/arginine-rich splicing factor 10 (SRSF10). HCC patients with poor prognosis express higher levels of exon 10-inclusive SREK1 (SREK1L). SREK1L can sustain BLOC1S5-TXNDC5 (B-T) expression, a targeted gene of nonsense-mediated mRNA decay through inhibiting exon-exon junction complex binding with B-T to exert its oncogenic role. B-T plays its competing endogenous RNA role by inhibiting miR-30c-5p and miR-30e-5p, and further promoting the expression of downstream oncogenic targets SRSF10 and TXNDC5. Interestingly, SRSF10 can act as a splicing regulator for SREK1L to promote hepatocarcinogenesis via the formation of a SRSF10-associated complex. In summary, we demonstrate a SRSF10/SREK1L/B-T signalling loop to accelerate the hepatocarcinogenesis.",

author = "Cunjie Chang and Muthukumar Rajasekaran and Yiting Qiao and Heng Dong and Yu Wang and Hongping Xia and Amudha Deivasigamani and Minjie Wu and Karthik Sekar and Hengjun Gao and Mengqing Sun and Yuqin Niu and Qian Li and Lin Tao and Zhen Yan and Menglan Wang and Shasha Chen and Shujuan Zhao and Dajing Chen and Lina Li and Fan Yang and Haojin Gao and Baodong Chen and Ling Su and Liang Xu and Ye Chen and Seshachalam, \{Veerabrahma Pratap\} and Gongxing Chen and Jayantha Gunaratne and Wanjin Hong and Junping Shi and Gongying Chen and Grierson, \{David S.\} and Benoit Chabot and Tian Xie and Hui, \{Kam Man\} and Jianxiang Chen",

note = "Publisher Copyright: {\textcopyright} 2022, The Author(s).",

year = "2022",

month = dec,

doi = "10.1038/s41467-022-29016-x",

language = "英语",

volume = "13",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Research",

number = "1",

}

Chang, C, Rajasekaran, M, Qiao, Y, Dong, H, Wang, Y, Xia, H, Deivasigamani, A, Wu, M, Sekar, K, Gao, H, Sun, M, Niu, Y, Li, Q, Tao, L, Yan, Z, Wang, M, Chen, S, Zhao, S, Chen, D, Li, L, Yang, F, Gao, H, Chen, B, Su, L, Xu, L, Chen, Y, Seshachalam, VP, Chen, G, Gunaratne, J, Hong, W, Shi, J, Chen, G, Grierson, DS, Chabot, B, Xie, T, Hui, KM & Chen, J 2022, 'The aberrant upregulation of exon 10-inclusive SREK1 through SRSF10 acts as an oncogenic driver in human hepatocellular carcinoma', Nature Communications, 卷 13, 号码 1, 1363. https://doi.org/10.1038/s41467-022-29016-x

TY - JOUR

T1 - The aberrant upregulation of exon 10-inclusive SREK1 through SRSF10 acts as an oncogenic driver in human hepatocellular carcinoma

AU - Chang, Cunjie

AU - Rajasekaran, Muthukumar

AU - Qiao, Yiting

AU - Dong, Heng

AU - Wang, Yu

AU - Xia, Hongping

AU - Deivasigamani, Amudha

AU - Wu, Minjie

AU - Sekar, Karthik

AU - Gao, Hengjun

AU - Sun, Mengqing

AU - Niu, Yuqin

AU - Li, Qian

AU - Tao, Lin

AU - Yan, Zhen

AU - Wang, Menglan

AU - Chen, Shasha

AU - Zhao, Shujuan

AU - Chen, Dajing

AU - Li, Lina

AU - Yang, Fan

AU - Gao, Haojin

AU - Chen, Baodong

AU - Su, Ling

AU - Xu, Liang

AU - Chen, Ye

AU - Seshachalam, Veerabrahma Pratap

AU - Chen, Gongxing

AU - Gunaratne, Jayantha

AU - Hong, Wanjin

AU - Shi, Junping

AU - Chen, Gongying

AU - Grierson, David S.

AU - Chabot, Benoit

AU - Xie, Tian

AU - Hui, Kam Man

AU - Chen, Jianxiang

PY - 2022/12

Y1 - 2022/12

N2 - Deregulation of alternative splicing is implicated as a relevant source of molecular heterogeneity in cancer. However, the targets and intrinsic mechanisms of splicing in hepatocarcinogenesis are largely unknown. Here, we report a functional impact of a Splicing Regulatory Glutamine/Lysine-Rich Protein 1 (SREK1) variant and its regulator, Serine/arginine-rich splicing factor 10 (SRSF10). HCC patients with poor prognosis express higher levels of exon 10-inclusive SREK1 (SREK1L). SREK1L can sustain BLOC1S5-TXNDC5 (B-T) expression, a targeted gene of nonsense-mediated mRNA decay through inhibiting exon-exon junction complex binding with B-T to exert its oncogenic role. B-T plays its competing endogenous RNA role by inhibiting miR-30c-5p and miR-30e-5p, and further promoting the expression of downstream oncogenic targets SRSF10 and TXNDC5. Interestingly, SRSF10 can act as a splicing regulator for SREK1L to promote hepatocarcinogenesis via the formation of a SRSF10-associated complex. In summary, we demonstrate a SRSF10/SREK1L/B-T signalling loop to accelerate the hepatocarcinogenesis.

AB - Deregulation of alternative splicing is implicated as a relevant source of molecular heterogeneity in cancer. However, the targets and intrinsic mechanisms of splicing in hepatocarcinogenesis are largely unknown. Here, we report a functional impact of a Splicing Regulatory Glutamine/Lysine-Rich Protein 1 (SREK1) variant and its regulator, Serine/arginine-rich splicing factor 10 (SRSF10). HCC patients with poor prognosis express higher levels of exon 10-inclusive SREK1 (SREK1L). SREK1L can sustain BLOC1S5-TXNDC5 (B-T) expression, a targeted gene of nonsense-mediated mRNA decay through inhibiting exon-exon junction complex binding with B-T to exert its oncogenic role. B-T plays its competing endogenous RNA role by inhibiting miR-30c-5p and miR-30e-5p, and further promoting the expression of downstream oncogenic targets SRSF10 and TXNDC5. Interestingly, SRSF10 can act as a splicing regulator for SREK1L to promote hepatocarcinogenesis via the formation of a SRSF10-associated complex. In summary, we demonstrate a SRSF10/SREK1L/B-T signalling loop to accelerate the hepatocarcinogenesis.

UR - https://www.scopus.com/pages/publications/85126661719

U2 - 10.1038/s41467-022-29016-x

DO - 10.1038/s41467-022-29016-x

M3 - 文章

C2 - 35296659

AN - SCOPUS:85126661719

SN - 2041-1723

VL - 13

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 1363

ER -

The aberrant upregulation of exon 10-inclusive SREK1 through SRSF10 acts as an oncogenic driver in human hepatocellular carcinoma

摘要

联合国可持续发展目标

访问文件

其它文件与链接

学术指纹

引用此