Syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer

Pancreatic ductal adenocarcinoma (PDAC) remains recalcitrant to all forms of cancer treatment and carries a dismal 5-year survival rate of 8%(1). Inhibition of oncogenic KRAS (hereafter KRAS*), the earliest lesion in disease development that is present in >90% of PDAC, and its signaling surrogate...

Descripción completa

Detalles Bibliográficos
Autores principales: Yao, Wantong, Rose, Johnathon L., Wang, Wei, Seth, Sahil, Jiang, Hong, Taguchi, Ayumu, Liu, Jintan, Yan, Liang, Kapoor, Avnish, Hou, Pingping, Chen, Ziheng, Wang, Qiuyun, Nezi, Luigi, Xu, Zhaohui, Yao, Jun, Hu, Baoli, Pettazzoni, Piergiorgio F., Ho, I Lin, Feng, Ningping, Ramamoorthy, Vandhana, Jiang, Shan, Deng, Pingna, Ma, Grace J., Den, Peter, Tan, Zhi, Zhang, Shu Xing, Wang, Huamin, Wang, Alan Y., Deem, Angela K., Fleming, Jason B., Carugo, Alessandro, Heffernan, Timothy P., Maitra, Anirban, Viale, Andrea, Ying, Haoqiang, Hanash, Samir, DePinho, Ronald A., Draetta, Giulio F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2019
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6661074/
https://www.ncbi.nlm.nih.gov/pubmed/30918400
http://dx.doi.org/10.1038/s41586-019-1062-1
_version_ 1783439402690674688
author Yao, Wantong
Rose, Johnathon L.
Wang, Wei
Seth, Sahil
Jiang, Hong
Taguchi, Ayumu
Liu, Jintan
Yan, Liang
Kapoor, Avnish
Hou, Pingping
Chen, Ziheng
Wang, Qiuyun
Nezi, Luigi
Xu, Zhaohui
Yao, Jun
Hu, Baoli
Pettazzoni, Piergiorgio F.
Ho, I Lin
Feng, Ningping
Ramamoorthy, Vandhana
Jiang, Shan
Deng, Pingna
Ma, Grace J.
Den, Peter
Tan, Zhi
Zhang, Shu Xing
Wang, Huamin
Wang, Alan Y.
Deem, Angela K.
Fleming, Jason B.
Carugo, Alessandro
Heffernan, Timothy P.
Maitra, Anirban
Viale, Andrea
Ying, Haoqiang
Hanash, Samir
DePinho, Ronald A.
Draetta, Giulio F.
author_facet Yao, Wantong
Rose, Johnathon L.
Wang, Wei
Seth, Sahil
Jiang, Hong
Taguchi, Ayumu
Liu, Jintan
Yan, Liang
Kapoor, Avnish
Hou, Pingping
Chen, Ziheng
Wang, Qiuyun
Nezi, Luigi
Xu, Zhaohui
Yao, Jun
Hu, Baoli
Pettazzoni, Piergiorgio F.
Ho, I Lin
Feng, Ningping
Ramamoorthy, Vandhana
Jiang, Shan
Deng, Pingna
Ma, Grace J.
Den, Peter
Tan, Zhi
Zhang, Shu Xing
Wang, Huamin
Wang, Alan Y.
Deem, Angela K.
Fleming, Jason B.
Carugo, Alessandro
Heffernan, Timothy P.
Maitra, Anirban
Viale, Andrea
Ying, Haoqiang
Hanash, Samir
DePinho, Ronald A.
Draetta, Giulio F.
author_sort Yao, Wantong
collection PubMed
description Pancreatic ductal adenocarcinoma (PDAC) remains recalcitrant to all forms of cancer treatment and carries a dismal 5-year survival rate of 8%(1). Inhibition of oncogenic KRAS (hereafter KRAS*), the earliest lesion in disease development that is present in >90% of PDAC, and its signaling surrogates has yielded encouraging preclinical results with experimental agents(2-4). However, KRAS*-independent disease recurrence following genetic extinction of Kras* in mouse models anticipates the need for co-extinction strategies(5,6). Multiple oncogenic processes are initiated at the cell surface, where KRAS* physically and functionally interacts to direct signaling essential for malignant transformation and tumor maintenance. Insights into the complexity of the functional surfaceome have been technologically limited until recently, and, in the case of PDAC, the genetic control of the function and composition of the PDAC surfaceome in the context of KRAS* signaling remains largely unexplored. Here, we developed an unbiased, functional target discovery platform to query KRAS*-dependent changes of the PDAC surfaceome, which uncovered syndecan-1 (SDC1) as a protein upregulated at the cell surface by KRAS*. Cell surface localization of SDC1 is essential for disease maintenance and progression, where it regulates macropinocytosis, an essential metabolic pathway that fuels PDAC cell growth. Thus, our study forges a mechanistic link between KRAS* signaling and a targetable molecule driving nutrient salvage pathways in PDAC and validates oncogene-driven surfaceome annotation as a strategy to identify cancer-specific vulnerabilities.
format Online
Article
Text
id pubmed-6661074
institution National Center for Biotechnology Information
language English
publishDate 2019
record_format MEDLINE/PubMed
spelling pubmed-66610742019-09-27 Syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer Yao, Wantong Rose, Johnathon L. Wang, Wei Seth, Sahil Jiang, Hong Taguchi, Ayumu Liu, Jintan Yan, Liang Kapoor, Avnish Hou, Pingping Chen, Ziheng Wang, Qiuyun Nezi, Luigi Xu, Zhaohui Yao, Jun Hu, Baoli Pettazzoni, Piergiorgio F. Ho, I Lin Feng, Ningping Ramamoorthy, Vandhana Jiang, Shan Deng, Pingna Ma, Grace J. Den, Peter Tan, Zhi Zhang, Shu Xing Wang, Huamin Wang, Alan Y. Deem, Angela K. Fleming, Jason B. Carugo, Alessandro Heffernan, Timothy P. Maitra, Anirban Viale, Andrea Ying, Haoqiang Hanash, Samir DePinho, Ronald A. Draetta, Giulio F. Nature Article Pancreatic ductal adenocarcinoma (PDAC) remains recalcitrant to all forms of cancer treatment and carries a dismal 5-year survival rate of 8%(1). Inhibition of oncogenic KRAS (hereafter KRAS*), the earliest lesion in disease development that is present in >90% of PDAC, and its signaling surrogates has yielded encouraging preclinical results with experimental agents(2-4). However, KRAS*-independent disease recurrence following genetic extinction of Kras* in mouse models anticipates the need for co-extinction strategies(5,6). Multiple oncogenic processes are initiated at the cell surface, where KRAS* physically and functionally interacts to direct signaling essential for malignant transformation and tumor maintenance. Insights into the complexity of the functional surfaceome have been technologically limited until recently, and, in the case of PDAC, the genetic control of the function and composition of the PDAC surfaceome in the context of KRAS* signaling remains largely unexplored. Here, we developed an unbiased, functional target discovery platform to query KRAS*-dependent changes of the PDAC surfaceome, which uncovered syndecan-1 (SDC1) as a protein upregulated at the cell surface by KRAS*. Cell surface localization of SDC1 is essential for disease maintenance and progression, where it regulates macropinocytosis, an essential metabolic pathway that fuels PDAC cell growth. Thus, our study forges a mechanistic link between KRAS* signaling and a targetable molecule driving nutrient salvage pathways in PDAC and validates oncogene-driven surfaceome annotation as a strategy to identify cancer-specific vulnerabilities. 2019-03-27 2019-04 /pmc/articles/PMC6661074/ /pubmed/30918400 http://dx.doi.org/10.1038/s41586-019-1062-1 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Yao, Wantong
Rose, Johnathon L.
Wang, Wei
Seth, Sahil
Jiang, Hong
Taguchi, Ayumu
Liu, Jintan
Yan, Liang
Kapoor, Avnish
Hou, Pingping
Chen, Ziheng
Wang, Qiuyun
Nezi, Luigi
Xu, Zhaohui
Yao, Jun
Hu, Baoli
Pettazzoni, Piergiorgio F.
Ho, I Lin
Feng, Ningping
Ramamoorthy, Vandhana
Jiang, Shan
Deng, Pingna
Ma, Grace J.
Den, Peter
Tan, Zhi
Zhang, Shu Xing
Wang, Huamin
Wang, Alan Y.
Deem, Angela K.
Fleming, Jason B.
Carugo, Alessandro
Heffernan, Timothy P.
Maitra, Anirban
Viale, Andrea
Ying, Haoqiang
Hanash, Samir
DePinho, Ronald A.
Draetta, Giulio F.
Syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer
title Syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer
title_full Syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer
title_fullStr Syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer
title_full_unstemmed Syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer
title_short Syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer
title_sort syndecan1 is a critical mediator of macropinocytosis in pancreatic cancer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6661074/
https://www.ncbi.nlm.nih.gov/pubmed/30918400
http://dx.doi.org/10.1038/s41586-019-1062-1
work_keys_str_mv AT yaowantong syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT rosejohnathonl syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT wangwei syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT sethsahil syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT jianghong syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT taguchiayumu syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT liujintan syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT yanliang syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT kapooravnish syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT houpingping syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT chenziheng syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT wangqiuyun syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT neziluigi syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT xuzhaohui syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT yaojun syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT hubaoli syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT pettazzonipiergiorgiof syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT hoilin syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT fengningping syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT ramamoorthyvandhana syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT jiangshan syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT dengpingna syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT magracej syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT denpeter syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT tanzhi syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT zhangshuxing syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT wanghuamin syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT wangalany syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT deemangelak syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT flemingjasonb syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT carugoalessandro syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT heffernantimothyp syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT maitraanirban syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT vialeandrea syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT yinghaoqiang syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT hanashsamir syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT depinhoronalda syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer
AT draettagiuliof syndecan1isacriticalmediatorofmacropinocytosisinpancreaticcancer

Ejemplares similares