Targeted Therapy to β3 Integrin Reduces Chemoresistance in Breast Cancer Bone Metastases

Gregory C. Fox; Xinming Su; Jennifer L. Davis; Yalin Xu; Kristin A. Kwakwa; Michael H. Ross; Francesca Fontana; Jingyu Xiang; Alison K. Esser; Elizabeth Cordell; Kristen Pagliai; Ha X. Dang; Jothilingam Sivapackiam; Sheila A. Stewart; Christopher A. Maher; Suzanne J. Bakewell; James A.J. Fitzpatrick; Vijay Sharma; Samuel Achilefu; Deborah J. Veis; Gregory M. Lanza; Katherine N. Weilbaecher

doi:10.1158/1535-7163.MCT-20-0931

Targeted Therapy to β3 Integrin Reduces Chemoresistance in Breast Cancer Bone Metastases

Gregory C. Fox, Xinming Su, Jennifer L. Davis, Yalin Xu, Kristin A. Kwakwa, Michael H. Ross, Francesca Fontana, Jingyu Xiang, Alison K. Esser, Elizabeth Cordell, Kristen Pagliai, Ha X. Dang, Jothilingam Sivapackiam, Sheila A. Stewart, Christopher A. Maher, Suzanne J. Bakewell, James A.J. Fitzpatrick, Vijay Sharma, Samuel Achilefu, Deborah J. VeisGregory M. Lanza, Katherine N. Weilbaecher

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Breast cancer bone metastases are common and incurable. Tumoral integrin b3 (b3) expression is induced through interaction with the bone microenvironment. Although b3 is known to promote bone colonization, its functional role during therapy of established bone metastases is not known. We found increased numbers of b3^þ tumor cells in murine bone metastases after docetaxel chemotherapy. b3^þ tumor cells were present in 97% of post-neoadjuvant chemotherapy triple-negative breast cancer patient samples (n ¼ 38). High tumoral b3 expression was associated with worse outcomes in both pre- and postchemotherapy triple-negative breast cancer groups. Genetic deletion of tumoral b3 had minimal effect in vitro, but significantly enhanced in vivo docetaxel activity, particularly in the bone. Rescue experiments confirmed that this effect required intact b3 signaling. Ultrastructural, transcriptomic, and functional analyses revealed an alternative metabolic response to chemotherapy in b3-expressing cells characterized by enhanced oxygen consumption, reactive oxygen species generation, and protein production. We identified mTORC1 as a candidate for therapeutic targeting of this b3-mediated, chemotherapy-induced metabolic response. mTORC1 inhibition in combination with docetaxel synergistically attenuated murine bone metastases. Furthermore, micelle nanoparticle delivery of mTORC1 inhibitor to cells expressing activated avb3 integrins enhanced docetaxel efficacy in bone metastases. Taken together, we show that b3 integrin induction by the bone microenvironment promotes resistance to chemotherapy through an altered metabolic response that can be defused by combination with avb3-targeted mTORC1 inhibitor nanotherapy. Our work demonstrates the importance of the metastatic microenvironment when designing treatments and presents new, bone-specific strategies for enhancing chemotherapeutic efficacy.

Original language	English (US)
Pages (from-to)	1183-1198
Number of pages	16
Journal	Molecular Cancer Therapeutics
Volume	20
Issue number	6
DOIs	https://doi.org/10.1158/1535-7163.MCT-20-0931
State	Published - Jun 2021
Externally published	Yes

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/1535-7163.MCT-20-0931

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Fox, G. C., Su, X., Davis, J. L., Xu, Y., Kwakwa, K. A., Ross, M. H., Fontana, F., Xiang, J., Esser, A. K., Cordell, E., Pagliai, K., Dang, H. X., Sivapackiam, J., Stewart, S. A., Maher, C. A., Bakewell, S. J., Fitzpatrick, J. A. J., Sharma, V., Achilefu, S., ... Weilbaecher, K. N. (2021). Targeted Therapy to β3 Integrin Reduces Chemoresistance in Breast Cancer Bone Metastases. Molecular Cancer Therapeutics, 20(6), 1183-1198. https://doi.org/10.1158/1535-7163.MCT-20-0931

Fox, GC, Su, X, Davis, JL, Xu, Y, Kwakwa, KA, Ross, MH, Fontana, F, Xiang, J, Esser, AK, Cordell, E, Pagliai, K, Dang, HX, Sivapackiam, J, Stewart, SA, Maher, CA, Bakewell, SJ, Fitzpatrick, JAJ, Sharma, V, Achilefu, S, Veis, DJ, Lanza, GM & Weilbaecher, KN 2021, 'Targeted Therapy to β3 Integrin Reduces Chemoresistance in Breast Cancer Bone Metastases', Molecular Cancer Therapeutics, vol. 20, no. 6, pp. 1183-1198. https://doi.org/10.1158/1535-7163.MCT-20-0931

@article{4e7eed8b398b48b5a5df8a8debe6410a,

title = "Targeted Therapy to β3 Integrin Reduces Chemoresistance in Breast Cancer Bone Metastases",

abstract = "Breast cancer bone metastases are common and incurable. Tumoral integrin b3 (b3) expression is induced through interaction with the bone microenvironment. Although b3 is known to promote bone colonization, its functional role during therapy of established bone metastases is not known. We found increased numbers of b3{\th} tumor cells in murine bone metastases after docetaxel chemotherapy. b3{\th} tumor cells were present in 97% of post-neoadjuvant chemotherapy triple-negative breast cancer patient samples (n ¼ 38). High tumoral b3 expression was associated with worse outcomes in both pre- and postchemotherapy triple-negative breast cancer groups. Genetic deletion of tumoral b3 had minimal effect in vitro, but significantly enhanced in vivo docetaxel activity, particularly in the bone. Rescue experiments confirmed that this effect required intact b3 signaling. Ultrastructural, transcriptomic, and functional analyses revealed an alternative metabolic response to chemotherapy in b3-expressing cells characterized by enhanced oxygen consumption, reactive oxygen species generation, and protein production. We identified mTORC1 as a candidate for therapeutic targeting of this b3-mediated, chemotherapy-induced metabolic response. mTORC1 inhibition in combination with docetaxel synergistically attenuated murine bone metastases. Furthermore, micelle nanoparticle delivery of mTORC1 inhibitor to cells expressing activated avb3 integrins enhanced docetaxel efficacy in bone metastases. Taken together, we show that b3 integrin induction by the bone microenvironment promotes resistance to chemotherapy through an altered metabolic response that can be defused by combination with avb3-targeted mTORC1 inhibitor nanotherapy. Our work demonstrates the importance of the metastatic microenvironment when designing treatments and presents new, bone-specific strategies for enhancing chemotherapeutic efficacy.",

author = "Fox, {Gregory C.} and Xinming Su and Davis, {Jennifer L.} and Yalin Xu and Kwakwa, {Kristin A.} and Ross, {Michael H.} and Francesca Fontana and Jingyu Xiang and Esser, {Alison K.} and Elizabeth Cordell and Kristen Pagliai and Dang, {Ha X.} and Jothilingam Sivapackiam and Stewart, {Sheila A.} and Maher, {Christopher A.} and Bakewell, {Suzanne J.} and Fitzpatrick, {James A.J.} and Vijay Sharma and Samuel Achilefu and Veis, {Deborah J.} and Lanza, {Gregory M.} and Weilbaecher, {Katherine N.}",

note = "Funding Information: This study was supported in whole or in part by the following grants: NCI R01 CA216840 (to G.C. Fox, X. Su, J.L. Davis, Y. Xu, K.A. Kwakwa, M.H. Ross, F. Fontana, J. Xiang, A.K. Esser, G.M. Lanza, K.N. Weilbaecher), NCI P01 CA100730 (to G.C. Fox, X. Su, Y. Xu, M.H. Ross, F. Fontana, J. Xiang, A.K. Esser, K.N. Weilbaecher), NIH U54CA199092 (S. Achilefu, K.N. Weilbaecher), DoD BCRP W81XWH-16-1-0286 (S. Achilefu, X. Su, K.N. Weilbaecher), NIAMS R21 AR073507 (to D.J. Veis), NIAMS R01 AR070030 (to D.J. Veis), NHLBI R01 HL111163 (to J. Sivapackiam, V. Sharma), NHLBI R01 HL142297 (to J. Sivapackiam, V. Sharma), NIBIB P41 EB025815 (to J. Sivapackiam, V. Sharma), and training grants NIAMS T32AR060719 (to G.C. Fox and M.H. Ross) and NIGMS GM07200 (to G.C. Fox). Additional support was provided by the Genome Technology Access Center for sequencing (NIDDK P30-CA91842, ICTS/CTSA UL1TR002345); the Washington University Center for Cellular Imaging (WUCCI) for contributions to preparation, acquisition, and interpretation of electron microscopy data (CDI-CORE-2015–505, CDI-CORE-2019–813, Foundation for Barnes-Jewish Hospital 3770, NCI P30-CA091842, NIH ORIP OD021694); the Musculoskeletal Research Center for histology and radiography (NIAMS P30-AR057235); the Molecular Imaging Center at Washington University for bioluminescence imaging (NCI S10 OD02742, to S. Achilefu); the Alvin J. Siteman Cancer Center Biostatistics Shared Resource for statistical analysis of patient clinical data (NCI P30 CA091842); the Pat Burkhart Breast Cancer Fund, the Barnes-Jewish Foundation, the St. Louis Men{\textquoteright}`s Group Against Cancer (to K.Weilbaecher). The authors also acknowledge Vecteezy and BioRender for graphics, and the Hope Center Alafi Neuroimaging Lab (NIH Shared Instrumentation Grant S10 RR027552). The authors thank Drs. Jason Mills, Kareem Azab, David Ornitz, Roberta Faccio, and Vivek Arora for their incisive suggestions and criticism. We gratefully acknowledge Crystal Idleburg, Lynne Collins, Julie Prior, Laura Luecking, Tom Walsh, Dr. Rosy Luo, Dr. Kathryn Tormos, Craig Smith, Dr. Erica Lantelme, Dorjan Brinja, Max Fisher, Dr. Sanja Sviben, Dr. Greg Strout, and Dr. Peter Bayguinov for their invaluable technical assistance and expertise. Publisher Copyright: {\textcopyright} 2021 American Association for Cancer Research.",

year = "2021",

month = jun,

doi = "10.1158/1535-7163.MCT-20-0931",

language = "English (US)",

volume = "20",

pages = "1183--1198",

journal = "Molecular Cancer Therapeutics",

issn = "1535-7163",

publisher = "American Association for Cancer Research Inc.",

number = "6",

}

TY - JOUR

T1 - Targeted Therapy to β3 Integrin Reduces Chemoresistance in Breast Cancer Bone Metastases

AU - Fox, Gregory C.

AU - Su, Xinming

AU - Davis, Jennifer L.

AU - Xu, Yalin

AU - Kwakwa, Kristin A.

AU - Ross, Michael H.

AU - Fontana, Francesca

AU - Xiang, Jingyu

AU - Esser, Alison K.

AU - Cordell, Elizabeth

AU - Pagliai, Kristen

AU - Dang, Ha X.

AU - Sivapackiam, Jothilingam

AU - Stewart, Sheila A.

AU - Maher, Christopher A.

AU - Bakewell, Suzanne J.

AU - Fitzpatrick, James A.J.

AU - Sharma, Vijay

AU - Achilefu, Samuel

AU - Veis, Deborah J.

AU - Lanza, Gregory M.

AU - Weilbaecher, Katherine N.

N1 - Funding Information: This study was supported in whole or in part by the following grants: NCI R01 CA216840 (to G.C. Fox, X. Su, J.L. Davis, Y. Xu, K.A. Kwakwa, M.H. Ross, F. Fontana, J. Xiang, A.K. Esser, G.M. Lanza, K.N. Weilbaecher), NCI P01 CA100730 (to G.C. Fox, X. Su, Y. Xu, M.H. Ross, F. Fontana, J. Xiang, A.K. Esser, K.N. Weilbaecher), NIH U54CA199092 (S. Achilefu, K.N. Weilbaecher), DoD BCRP W81XWH-16-1-0286 (S. Achilefu, X. Su, K.N. Weilbaecher), NIAMS R21 AR073507 (to D.J. Veis), NIAMS R01 AR070030 (to D.J. Veis), NHLBI R01 HL111163 (to J. Sivapackiam, V. Sharma), NHLBI R01 HL142297 (to J. Sivapackiam, V. Sharma), NIBIB P41 EB025815 (to J. Sivapackiam, V. Sharma), and training grants NIAMS T32AR060719 (to G.C. Fox and M.H. Ross) and NIGMS GM07200 (to G.C. Fox). Additional support was provided by the Genome Technology Access Center for sequencing (NIDDK P30-CA91842, ICTS/CTSA UL1TR002345); the Washington University Center for Cellular Imaging (WUCCI) for contributions to preparation, acquisition, and interpretation of electron microscopy data (CDI-CORE-2015–505, CDI-CORE-2019–813, Foundation for Barnes-Jewish Hospital 3770, NCI P30-CA091842, NIH ORIP OD021694); the Musculoskeletal Research Center for histology and radiography (NIAMS P30-AR057235); the Molecular Imaging Center at Washington University for bioluminescence imaging (NCI S10 OD02742, to S. Achilefu); the Alvin J. Siteman Cancer Center Biostatistics Shared Resource for statistical analysis of patient clinical data (NCI P30 CA091842); the Pat Burkhart Breast Cancer Fund, the Barnes-Jewish Foundation, the St. Louis Men’`s Group Against Cancer (to K.Weilbaecher). The authors also acknowledge Vecteezy and BioRender for graphics, and the Hope Center Alafi Neuroimaging Lab (NIH Shared Instrumentation Grant S10 RR027552). The authors thank Drs. Jason Mills, Kareem Azab, David Ornitz, Roberta Faccio, and Vivek Arora for their incisive suggestions and criticism. We gratefully acknowledge Crystal Idleburg, Lynne Collins, Julie Prior, Laura Luecking, Tom Walsh, Dr. Rosy Luo, Dr. Kathryn Tormos, Craig Smith, Dr. Erica Lantelme, Dorjan Brinja, Max Fisher, Dr. Sanja Sviben, Dr. Greg Strout, and Dr. Peter Bayguinov for their invaluable technical assistance and expertise. Publisher Copyright: © 2021 American Association for Cancer Research.

PY - 2021/6

Y1 - 2021/6

N2 - Breast cancer bone metastases are common and incurable. Tumoral integrin b3 (b3) expression is induced through interaction with the bone microenvironment. Although b3 is known to promote bone colonization, its functional role during therapy of established bone metastases is not known. We found increased numbers of b3þ tumor cells in murine bone metastases after docetaxel chemotherapy. b3þ tumor cells were present in 97% of post-neoadjuvant chemotherapy triple-negative breast cancer patient samples (n ¼ 38). High tumoral b3 expression was associated with worse outcomes in both pre- and postchemotherapy triple-negative breast cancer groups. Genetic deletion of tumoral b3 had minimal effect in vitro, but significantly enhanced in vivo docetaxel activity, particularly in the bone. Rescue experiments confirmed that this effect required intact b3 signaling. Ultrastructural, transcriptomic, and functional analyses revealed an alternative metabolic response to chemotherapy in b3-expressing cells characterized by enhanced oxygen consumption, reactive oxygen species generation, and protein production. We identified mTORC1 as a candidate for therapeutic targeting of this b3-mediated, chemotherapy-induced metabolic response. mTORC1 inhibition in combination with docetaxel synergistically attenuated murine bone metastases. Furthermore, micelle nanoparticle delivery of mTORC1 inhibitor to cells expressing activated avb3 integrins enhanced docetaxel efficacy in bone metastases. Taken together, we show that b3 integrin induction by the bone microenvironment promotes resistance to chemotherapy through an altered metabolic response that can be defused by combination with avb3-targeted mTORC1 inhibitor nanotherapy. Our work demonstrates the importance of the metastatic microenvironment when designing treatments and presents new, bone-specific strategies for enhancing chemotherapeutic efficacy.

AB - Breast cancer bone metastases are common and incurable. Tumoral integrin b3 (b3) expression is induced through interaction with the bone microenvironment. Although b3 is known to promote bone colonization, its functional role during therapy of established bone metastases is not known. We found increased numbers of b3þ tumor cells in murine bone metastases after docetaxel chemotherapy. b3þ tumor cells were present in 97% of post-neoadjuvant chemotherapy triple-negative breast cancer patient samples (n ¼ 38). High tumoral b3 expression was associated with worse outcomes in both pre- and postchemotherapy triple-negative breast cancer groups. Genetic deletion of tumoral b3 had minimal effect in vitro, but significantly enhanced in vivo docetaxel activity, particularly in the bone. Rescue experiments confirmed that this effect required intact b3 signaling. Ultrastructural, transcriptomic, and functional analyses revealed an alternative metabolic response to chemotherapy in b3-expressing cells characterized by enhanced oxygen consumption, reactive oxygen species generation, and protein production. We identified mTORC1 as a candidate for therapeutic targeting of this b3-mediated, chemotherapy-induced metabolic response. mTORC1 inhibition in combination with docetaxel synergistically attenuated murine bone metastases. Furthermore, micelle nanoparticle delivery of mTORC1 inhibitor to cells expressing activated avb3 integrins enhanced docetaxel efficacy in bone metastases. Taken together, we show that b3 integrin induction by the bone microenvironment promotes resistance to chemotherapy through an altered metabolic response that can be defused by combination with avb3-targeted mTORC1 inhibitor nanotherapy. Our work demonstrates the importance of the metastatic microenvironment when designing treatments and presents new, bone-specific strategies for enhancing chemotherapeutic efficacy.

UR - http://www.scopus.com/inward/record.url?scp=85106995149&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85106995149&partnerID=8YFLogxK

U2 - 10.1158/1535-7163.MCT-20-0931

DO - 10.1158/1535-7163.MCT-20-0931

M3 - Article

C2 - 33785647

AN - SCOPUS:85106995149

SN - 1535-7163

VL - 20

SP - 1183

EP - 1198

JO - Molecular Cancer Therapeutics

JF - Molecular Cancer Therapeutics

IS - 6

ER -

Targeted Therapy to β3 Integrin Reduces Chemoresistance in Breast Cancer Bone Metastases

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