Targeting LRRC15 Inhibits Metastatic Dissemination of Ovarian Cancer

Upasana Ray; Deok Beom Jung; Ling Jin; Yinan Xiao; Subramanyam Dasari; Sayantani Sarkar Bhattacharya; Prabhu Thirusangu; Julie K. Staub; Debarshi Roy; Bhaskar Roy; S. John Weroha; Xiaonan Hou; James W. Purcell; Jamie N. Bakkum-Gamez; Scott H. Kaufmann; Nagarajan Kannan; Anirban K. Mitra; Viji Shridhar

doi:10.1158/0008-5472.CAN-21-0622

Targeting LRRC15 Inhibits Metastatic Dissemination of Ovarian Cancer

Upasana Ray, Deok Beom Jung, Ling Jin, Yinan Xiao, Subramanyam Dasari, Sayantani Sarkar Bhattacharya, Prabhu Thirusangu, Julie K. Staub, Debarshi Roy, Bhaskar Roy, S. John Weroha, Xiaonan Hou, James W. Purcell, Jamie N. Bakkum-Gamez, Scott H. Kaufmann, Nagarajan Kannan, Anirban K. Mitra, Viji Shridhar

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

Abstract

Dissemination of ovarian cancer cells can lead to inoperable metastatic lesions in the bowel and omentum that cause patient death. Here we show that LRRC15, a type-I 15-leucine-rich repeatcontainingmembrane protein, highly overexpressed in ovarian cancer bowel metastases compared with matched primary tumors and acts as a potent promoter of omental metastasis. Complementary models of ovarian cancer demonstrated that LRRC15 expression leads to inhibition of anoikis-induced cell death and promotes adhesion and invasion through matrices that mimic omentum. Mechanistically, LRRC15 interacted with β1-integrin to stimulate activation of focal adhesion kinase (FAK) signaling. As a therapeutic proof of concept, targeting LRRC15 with the specific antibody-drug conjugate ABBV- 085 in both early and latemetastatic ovarian cancer cell line xenograft models prevented metastatic dissemination, and these results were corroborated in metastatic patient-derived ovarian cancer xenograft models. Furthermore, treatment of 3D-spheroid cultures of LRRC15- positive patient-derived ascites with ABBV-085 reduced cell viability. Overall, these data uncover a role for LRRC15 in promoting ovarian cancer metastasis and suggest a novel and promising therapy to target ovarian cancer metastases.

Original language	English (US)
Pages (from-to)	1038-1054
Number of pages	17
Journal	Cancer research
Volume	82
Issue number	6
DOIs	https://doi.org/10.1158/0008-5472.CAN-21-0622
State	Published - Mar 15 2022

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/0008-5472.CAN-21-0622

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Ray, U., Jung, D. B., Jin, L., Xiao, Y., Dasari, S., Bhattacharya, S. S., Thirusangu, P., Staub, J. K., Roy, D., Roy, B., Weroha, S. J., Hou, X., Purcell, J. W., Bakkum-Gamez, J. N., Kaufmann, S. H., Kannan, N., Mitra, A. K., & Shridhar, V. (2022). Targeting LRRC15 Inhibits Metastatic Dissemination of Ovarian Cancer. Cancer research, 82(6), 1038-1054. https://doi.org/10.1158/0008-5472.CAN-21-0622

Ray, U, Jung, DB, Jin, L, Xiao, Y, Dasari, S, Bhattacharya, SS, Thirusangu, P, Staub, JK, Roy, D, Roy, B, Weroha, SJ, Hou, X, Purcell, JW, Bakkum-Gamez, JN , Kaufmann, SH , Kannan, N, Mitra, AK & Shridhar, V 2022, 'Targeting LRRC15 Inhibits Metastatic Dissemination of Ovarian Cancer', Cancer research, vol. 82, no. 6, pp. 1038-1054. https://doi.org/10.1158/0008-5472.CAN-21-0622

@article{7041d94965e64071b4fc5bec5b2332d8,

title = "Targeting LRRC15 Inhibits Metastatic Dissemination of Ovarian Cancer",

abstract = "Dissemination of ovarian cancer cells can lead to inoperable metastatic lesions in the bowel and omentum that cause patient death. Here we show that LRRC15, a type-I 15-leucine-rich repeatcontainingmembrane protein, highly overexpressed in ovarian cancer bowel metastases compared with matched primary tumors and acts as a potent promoter of omental metastasis. Complementary models of ovarian cancer demonstrated that LRRC15 expression leads to inhibition of anoikis-induced cell death and promotes adhesion and invasion through matrices that mimic omentum. Mechanistically, LRRC15 interacted with β1-integrin to stimulate activation of focal adhesion kinase (FAK) signaling. As a therapeutic proof of concept, targeting LRRC15 with the specific antibody-drug conjugate ABBV- 085 in both early and latemetastatic ovarian cancer cell line xenograft models prevented metastatic dissemination, and these results were corroborated in metastatic patient-derived ovarian cancer xenograft models. Furthermore, treatment of 3D-spheroid cultures of LRRC15- positive patient-derived ascites with ABBV-085 reduced cell viability. Overall, these data uncover a role for LRRC15 in promoting ovarian cancer metastasis and suggest a novel and promising therapy to target ovarian cancer metastases.",

author = "Upasana Ray and Jung, {Deok Beom} and Ling Jin and Yinan Xiao and Subramanyam Dasari and Bhattacharya, {Sayantani Sarkar} and Prabhu Thirusangu and Staub, {Julie K.} and Debarshi Roy and Bhaskar Roy and Weroha, {S. John} and Xiaonan Hou and Purcell, {James W.} and Bakkum-Gamez, {Jamie N.} and Kaufmann, {Scott H.} and Nagarajan Kannan and Mitra, {Anirban K.} and Viji Shridhar",

note = "Funding Information: This work is supported in part by the grants from the Minnesota Ovarian Cancer Alliance and the Department of Experimental Pathology and Laboratory Medicine and the Mayo Clinic (V. Shridhar) and the NIH (grant no. P50CA136393 for providing the ascites cells from patients wih ovarian cancer. The authors acknowledge the support from Dr. A.K. Mitra [DoD OCRP Ovarian Cancer Academy Award (W81XWH-15-0253) and American Cancer Society (RSG-21-019-01-CSM)]. The authors thank Drs. Amy Skubitz and Kristin Boylan for providing the cryopreserved patient-derived ascites samples from the University of Minnesota, Minneapolis under an IRB-approved protocol. The normal FTE cells were obtained from Dr. Ronny Drapkin, University of Pennsylvania, Philadelphia, PA; NOF151hTERT cells, HeyA8, and HeyA8MDR cells were obtained from MD Anderson Cancer Center, Houston, TX; PEO 1/4 from Dr. Taniguchi, Fred Hutchinson Cancer Research Center, Seattle, Washington; OVCAR 8/4 cells from Fox Chase Cancer Center, Philadelphia, PA; LP9/TERT-1 mesothelial cells from Coriell Institute for Medical Research, Publisher Copyright: {\textcopyright} 2021 The Authors.",

year = "2022",

month = mar,

day = "15",

doi = "10.1158/0008-5472.CAN-21-0622",

language = "English (US)",

volume = "82",

pages = "1038--1054",

journal = "Cancer Research",

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T1 - Targeting LRRC15 Inhibits Metastatic Dissemination of Ovarian Cancer

AU - Ray, Upasana

AU - Jung, Deok Beom

AU - Jin, Ling

AU - Xiao, Yinan

AU - Dasari, Subramanyam

AU - Bhattacharya, Sayantani Sarkar

AU - Thirusangu, Prabhu

AU - Staub, Julie K.

AU - Roy, Debarshi

AU - Roy, Bhaskar

AU - Weroha, S. John

AU - Hou, Xiaonan

AU - Purcell, James W.

AU - Bakkum-Gamez, Jamie N.

AU - Kaufmann, Scott H.

AU - Kannan, Nagarajan

AU - Mitra, Anirban K.

AU - Shridhar, Viji

N1 - Funding Information: This work is supported in part by the grants from the Minnesota Ovarian Cancer Alliance and the Department of Experimental Pathology and Laboratory Medicine and the Mayo Clinic (V. Shridhar) and the NIH (grant no. P50CA136393 for providing the ascites cells from patients wih ovarian cancer. The authors acknowledge the support from Dr. A.K. Mitra [DoD OCRP Ovarian Cancer Academy Award (W81XWH-15-0253) and American Cancer Society (RSG-21-019-01-CSM)]. The authors thank Drs. Amy Skubitz and Kristin Boylan for providing the cryopreserved patient-derived ascites samples from the University of Minnesota, Minneapolis under an IRB-approved protocol. The normal FTE cells were obtained from Dr. Ronny Drapkin, University of Pennsylvania, Philadelphia, PA; NOF151hTERT cells, HeyA8, and HeyA8MDR cells were obtained from MD Anderson Cancer Center, Houston, TX; PEO 1/4 from Dr. Taniguchi, Fred Hutchinson Cancer Research Center, Seattle, Washington; OVCAR 8/4 cells from Fox Chase Cancer Center, Philadelphia, PA; LP9/TERT-1 mesothelial cells from Coriell Institute for Medical Research, Publisher Copyright: © 2021 The Authors.

PY - 2022/3/15

Y1 - 2022/3/15

N2 - Dissemination of ovarian cancer cells can lead to inoperable metastatic lesions in the bowel and omentum that cause patient death. Here we show that LRRC15, a type-I 15-leucine-rich repeatcontainingmembrane protein, highly overexpressed in ovarian cancer bowel metastases compared with matched primary tumors and acts as a potent promoter of omental metastasis. Complementary models of ovarian cancer demonstrated that LRRC15 expression leads to inhibition of anoikis-induced cell death and promotes adhesion and invasion through matrices that mimic omentum. Mechanistically, LRRC15 interacted with β1-integrin to stimulate activation of focal adhesion kinase (FAK) signaling. As a therapeutic proof of concept, targeting LRRC15 with the specific antibody-drug conjugate ABBV- 085 in both early and latemetastatic ovarian cancer cell line xenograft models prevented metastatic dissemination, and these results were corroborated in metastatic patient-derived ovarian cancer xenograft models. Furthermore, treatment of 3D-spheroid cultures of LRRC15- positive patient-derived ascites with ABBV-085 reduced cell viability. Overall, these data uncover a role for LRRC15 in promoting ovarian cancer metastasis and suggest a novel and promising therapy to target ovarian cancer metastases.

AB - Dissemination of ovarian cancer cells can lead to inoperable metastatic lesions in the bowel and omentum that cause patient death. Here we show that LRRC15, a type-I 15-leucine-rich repeatcontainingmembrane protein, highly overexpressed in ovarian cancer bowel metastases compared with matched primary tumors and acts as a potent promoter of omental metastasis. Complementary models of ovarian cancer demonstrated that LRRC15 expression leads to inhibition of anoikis-induced cell death and promotes adhesion and invasion through matrices that mimic omentum. Mechanistically, LRRC15 interacted with β1-integrin to stimulate activation of focal adhesion kinase (FAK) signaling. As a therapeutic proof of concept, targeting LRRC15 with the specific antibody-drug conjugate ABBV- 085 in both early and latemetastatic ovarian cancer cell line xenograft models prevented metastatic dissemination, and these results were corroborated in metastatic patient-derived ovarian cancer xenograft models. Furthermore, treatment of 3D-spheroid cultures of LRRC15- positive patient-derived ascites with ABBV-085 reduced cell viability. Overall, these data uncover a role for LRRC15 in promoting ovarian cancer metastasis and suggest a novel and promising therapy to target ovarian cancer metastases.

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ER -

Targeting LRRC15 Inhibits Metastatic Dissemination of Ovarian Cancer

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