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Cancer associated fibroblasts in pancreatic ductal adenocarcinoma determine response to SLC7A11 inhibition

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dc.contributor.coauthorSharbeen, G.
dc.contributor.coauthorMcCarroll, J. A.
dc.contributor.coauthorAkerman, A.
dc.contributor.coauthorKopecky, C.
dc.contributor.coauthorYoukhana, J.
dc.contributor.coauthorKokkinos, J.
dc.contributor.coauthorHolst, J.
dc.contributor.coauthorBoyer, C.
dc.contributor.coauthorGoldstein, D.
dc.contributor.coauthorTimpson, P.
dc.contributor.coauthorCox, T. R.
dc.contributor.coauthorPereira, B. A.
dc.contributor.coauthorChitty, J. L.
dc.contributor.coauthorFey, S. K.
dc.contributor.coauthorNajumudeen, A. K.
dc.contributor.coauthorCampbell, A. D.
dc.contributor.coauthorSansom, O. J.
dc.contributor.coauthorIgnacio, R. M. C.
dc.contributor.coauthorNaim, S.
dc.contributor.coauthorLiu, J.
dc.contributor.coauthorRussia, N.
dc.contributor.coauthorLee, J.
dc.contributor.coauthorChou, A.
dc.contributor.coauthorJohns, A.
dc.contributor.coauthorGill, A. J.
dc.contributor.coauthorGonzales-Aloy, E.
dc.contributor.coauthorGebski, V.
dc.contributor.coauthorGuan, Y. F.
dc.contributor.coauthorPajic, M.
dc.contributor.coauthorTurner, N.
dc.contributor.coauthorApte, M. V.
dc.contributor.coauthorDavis, T. P.
dc.contributor.coauthorMorton, J. P.
dc.contributor.coauthorHaghighi, K. S.
dc.contributor.coauthorKasparian, J.
dc.contributor.coauthorMcLean, B. J.
dc.contributor.coauthorSetargew, Y. F. I.
dc.contributor.coauthorApgi APCGI
dc.contributor.coauthorPhillips, P. A.
dc.contributor.kuauthorErkan, Murat Mert
dc.contributor.kuprofileFaculty Member
dc.contributor.researchcenterKoç University Research Center for Translational Medicine (KUTTAM) / Koç Üniversitesi Translasyonel Tıp Araştırma Merkezi (KUTTAM)
dc.contributor.schoolcollegeinstituteSchool of Medicine
dc.contributor.yokid214689
dc.date.accessioned2024-11-09T13:48:58Z
dc.date.issued2021
dc.description.abstractCancer-associated fibroblasts (CAF) are major contributors to pancreatic ductal adenocarcinoma (PDAC) progression through protumor signaling and the generation of fibrosis, the latter of which creates a physical barrier to drugs. CAF inhibition is thus an ideal component of any therapeutic approach for PDAC. SLC7A11 is a cystine transporter that has been identified as a potential therapeutic target in PDAC cells. However, no prior study has evaluated the role of SLC7A11 in PDAC tumor stroma and its prognostic significance. Here we show that high expression of SLC7A11 in human PDAC tumor stroma, but not tumor cells, is independently prognostic of poorer overall survival. Orthogonal approaches showed that PDAC-derived CAFs are highly dependent on SLC7A11 for cystine uptake and glutathione synthesis and that SLC7A11 inhibition significantly decreases CAF proliferation, reduces their resistance to oxidative stress, and inhibits their ability to remodel collagen and support PDAC cell growth. Importantly, specific ablation of SLC7A11 from the tumor compartment of transgenic mouse PDAC tumors did not affect tumor growth, suggesting the stroma can substantially influence PDAC tumor response to SLC7A11 inhibition. In a mouse orthotopic PDAC model utilizing human PDAC cells and CAFs, stable knockdown of SLC7A11 was required in both cell types to reduce tumor growth, metastatic spread, and intratumoral fibrosis, demonstrating the importance of targeting SLC7A11 in both compartments. Finally, treatment with a nanoparticle genesilencing drug against SLC7A11, developed by our laboratory, reduced PDAC tumor growth, incidence of metastases, CAF activation, and fibrosis in orthotopic PDAC tumors. Overall, these findings identify an important role of SLC7A11 in PDAC-derived CAFs in supporting tumor growth. Significance: this study demonstrates that SLC7A11 in PDAC stromal cells is important for the tumor-promoting activity of CAFs and validates a clinically translatable nanomedicine for therapeutic SLC7A11 inhibition in PDAC.
dc.description.fulltextYES
dc.description.indexedbyWoS
dc.description.indexedbyScopus
dc.description.indexedbyPubMed
dc.description.issue13
dc.description.openaccessYES
dc.description.publisherscopeInternational
dc.description.sponsoredbyTubitakEuN/A
dc.description.sponsorshipNHMRC Project Grant
dc.description.sponsorshipAvner Innovation Grant
dc.description.sponsorshipNHMRC CDF-I
dc.description.sponsorshipNHMRC Ideas Grant
dc.description.sponsorshipCancer-Institute NSW ECF/CDFs
dc.description.sponsorshipCancer Institute NSW Innovation Grant
dc.description.sponsorshipCancer Institute NSW The Professor Rob Sutherland AO Make a Difference Award
dc.description.sponsorshipCancer Australia/Cancer Council
dc.description.sponsorshipCancer Australia/Kids Cancer Project
dc.description.sponsorshipCure Cancer Australia
dc.description.sponsorshipTour de Cure PhD Support Scholarship
dc.description.sponsorshipTour de Cure Established Research Grant
dc.description.sponsorshipTour de Cure Pioneering Research Grant
dc.description.sponsorshipUNSW Interlude Grant Scheme
dc.description.sponsorshipCancer Research UK Core Funding and Grand Challenge Grants
dc.description.sponsorshipNHMRC CDF-II
dc.description.sponsorshipNHMRC Senior Research Fellowship
dc.description.sponsorshipSuttons, Cancer Council NSW
dc.description.sponsorshipAvner Grant from PanKind
dc.description.sponsorshipAustralian Pancreatic Cancer Foundation
dc.description.sponsorshipTranslational Cancer Research Network and Australian Postgraduate Award Scholarships
dc.description.sponsorshipAustralian Government Research Training Program Scholarship
dc.description.sponsorshipUNSW Sydney Scientia PhD Scholarship
dc.description.sponsorshipPancreatic Cancer UK Future Leaders Academy
dc.description.sponsorshipLen Ainsworth Pancreatic Cancer Fellowship
dc.description.versionAuthor's final manuscript
dc.description.volume81
dc.formatpdf
dc.identifier.doi10.1158/0008-5472.CAN-20-2496
dc.identifier.eissn1538-7445
dc.identifier.embargoNO
dc.identifier.filenameinventorynoIR03239
dc.identifier.issn0008-5472
dc.identifier.linkhttps://doi.org/10.1158/0008-5472.CAN-20-2496
dc.identifier.quartileQ1
dc.identifier.scopus2-s2.0-85105783601
dc.identifier.urihttps://hdl.handle.net/20.500.14288/3846
dc.identifier.wos670539900006
dc.keywordsStellate cellscystine
dc.keywordsGlutamate antiporter
dc.keywordsGrowth
dc.keywordsTransporter
dc.keywordsMetabolism
dc.languageEnglish
dc.publisherAmerican Association for Cancer Research (AACR)
dc.relation.grantnoAPP1144108
dc.relation.grantnoAPP1140125
dc.relation.grantnoAPCF0050618
dc.relation.grantnoAPP1024896
dc.relation.grantnoAPP2002707
dc.relation.grantno08/ECF/1-37
dc.relation.grantnoCDF181166
dc.relation.grantnoCDF102
dc.relation.grantnoCDF171105
dc.relation.grantno09/RFG/2-58
dc.relation.grantno2017/AWD002
dc.relation.grantnoAPP1126736
dc.relation.grantnoAPP1184840
dc.relation.grantnoAPP1122758
dc.relation.grantnoRSP-011-18/19
dc.relation.grantnoUNSWR002
dc.relation.grantnoRSP-235-19/20
dc.relation.grantnoUNSWR004
dc.relation.grantnoRSP-255-19/20
dc.relation.grantnoRG210839
dc.relation.grantnoA17196
dc.relation.grantnoA21139
dc.relation.grantnoA25045
dc.relation.grantnoAPP1158590
dc.relation.grantnoAPP1136974
dc.relation.grantnoRG19-09
dc.relation.urihttp://cdm21054.contentdm.oclc.org/cdm/ref/collection/IR/id/10025
dc.sourceCancer Research
dc.subjectOncology
dc.titleCancer associated fibroblasts in pancreatic ductal adenocarcinoma determine response to SLC7A11 inhibition
dc.typeJournal Article
dspace.entity.typePublication
local.contributor.authorid0000-0002-2753-0234
local.contributor.kuauthorErkan, Murat Mert

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