Pharmacogenomic analysis of patient-derived tumor cells in gynecologic cancers

Jason K. Sa; Jae Ryoung Hwang; Young Jae Cho; Ji Yoon Ryu; Jung Joo Choi; Soo Young Jeong; Jihye Kim; Myeong Seon Kim; E. Sun Paik; Yoo Young Lee; Chel Hun Choi; Tae Joong Kim; Byoung Gie Kim; Duk Soo Bae; Yeri Lee; Nam Gu Her; Yong Jae Shin; Hee Jin Cho; Ja Yeon Kim; Yun Jee Seo; Harim Koo; Jeong Woo Oh; Taebum Lee; Hyun Soo Kim; Sang Yong Song; Joon Seol Bae; Woong Yang Park; Hee Dong Han; Hyung Jun Ahn; Anil K. Sood; Raul Rabadan; Jin Ku Lee; Do Hyun Nam; Jeong Won Lee

doi:10.1186/s13059-019-1848-3

Pharmacogenomic analysis of patient-derived tumor cells in gynecologic cancers

Jason K. Sa, Jae Ryoung Hwang, Young Jae Cho, Ji Yoon Ryu, Jung Joo Choi, Soo Young Jeong, Jihye Kim, Myeong Seon Kim, E. Sun Paik, Yoo Young Lee, Chel Hun Choi, Tae Joong Kim, Byoung Gie Kim, Duk Soo Bae, Yeri Lee, Nam Gu Her, Yong Jae Shin, Hee Jin Cho, Ja Yeon Kim, Yun Jee SeoHarim Koo, Jeong Woo Oh, Taebum Lee, Hyun Soo Kim, Sang Yong Song, Joon Seol Bae, Woong Yang Park, Hee Dong Han, Hyung Jun Ahn, Anil K. Sood, Raul Rabadan, Jin Ku Lee, Do Hyun Nam, Jeong Won Lee

Gynecological Oncology & Reproductive Medicine

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

17 Scopus citations

Abstract

Background: Gynecologic malignancy is one of the leading causes of mortality in female adults worldwide. Comprehensive genomic analysis has revealed a list of molecular aberrations that are essential to tumorigenesis, progression, and metastasis of gynecologic tumors. However, targeting such alterations has frequently led to treatment failures due to underlying genomic complexity and simultaneous activation of various tumor cell survival pathway molecules. A compilation of molecular characterization of tumors with pharmacological drug response is the next step toward clinical application of patient-tailored treatment regimens. Results: Toward this goal, we establish a library of 139 gynecologic tumors including epithelial ovarian cancers (EOCs), cervical, endometrial tumors, and uterine sarcomas that are genomically and/or pharmacologically annotated and explore dynamic pharmacogenomic associations against 37 molecularly targeted drugs. We discover lineage-specific drug sensitivities based on subcategorization of gynecologic tumors and identify TP53 mutation as a molecular determinant that elicits therapeutic response to poly (ADP-Ribose) polymerase (PARP) inhibitor. We further identify transcriptome expression of inhibitor of DNA biding 2 (ID2) as a potential predictive biomarker for treatment response to olaparib. Conclusions: Together, our results demonstrate the potential utility of rapid drug screening combined with genomic profiling for precision treatment of gynecologic cancers.

Original language	English (US)
Article number	253
Journal	Genome biology
Volume	20
Issue number	1
DOIs	https://doi.org/10.1186/s13059-019-1848-3
State	Published - Nov 26 2019

Keywords

Gynecologic malignancy
ID2
PARP inhibitor
Pharmacogenomic analysis
TP53 mutations

ASJC Scopus subject areas

Ecology, Evolution, Behavior and Systematics
Genetics
Cell Biology

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10.1186/s13059-019-1848-3

Cite this

Sa, J. K., Hwang, J. R., Cho, Y. J., Ryu, J. Y., Choi, J. J., Jeong, S. Y., Kim, J., Kim, M. S., Paik, E. S., Lee, Y. Y., Choi, C. H., Kim, T. J., Kim, B. G., Bae, D. S., Lee, Y., Her, N. G., Shin, Y. J., Cho, H. J., Kim, J. Y., ... Lee, J. W. (2019). Pharmacogenomic analysis of patient-derived tumor cells in gynecologic cancers. Genome biology, 20(1), Article 253. https://doi.org/10.1186/s13059-019-1848-3

Sa, JK, Hwang, JR, Cho, YJ, Ryu, JY, Choi, JJ, Jeong, SY, Kim, J, Kim, MS, Paik, ES, Lee, YY, Choi, CH, Kim, TJ, Kim, BG, Bae, DS, Lee, Y, Her, NG, Shin, YJ, Cho, HJ, Kim, JY, Seo, YJ, Koo, H, Oh, JW, Lee, T, Kim, HS, Song, SY, Bae, JS, Park, WY, Han, HD, Ahn, HJ, Sood, AK, Rabadan, R, Lee, JK, Nam, DH & Lee, JW 2019, 'Pharmacogenomic analysis of patient-derived tumor cells in gynecologic cancers', Genome biology, vol. 20, no. 1, 253. https://doi.org/10.1186/s13059-019-1848-3

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title = "Pharmacogenomic analysis of patient-derived tumor cells in gynecologic cancers",

abstract = "Background: Gynecologic malignancy is one of the leading causes of mortality in female adults worldwide. Comprehensive genomic analysis has revealed a list of molecular aberrations that are essential to tumorigenesis, progression, and metastasis of gynecologic tumors. However, targeting such alterations has frequently led to treatment failures due to underlying genomic complexity and simultaneous activation of various tumor cell survival pathway molecules. A compilation of molecular characterization of tumors with pharmacological drug response is the next step toward clinical application of patient-tailored treatment regimens. Results: Toward this goal, we establish a library of 139 gynecologic tumors including epithelial ovarian cancers (EOCs), cervical, endometrial tumors, and uterine sarcomas that are genomically and/or pharmacologically annotated and explore dynamic pharmacogenomic associations against 37 molecularly targeted drugs. We discover lineage-specific drug sensitivities based on subcategorization of gynecologic tumors and identify TP53 mutation as a molecular determinant that elicits therapeutic response to poly (ADP-Ribose) polymerase (PARP) inhibitor. We further identify transcriptome expression of inhibitor of DNA biding 2 (ID2) as a potential predictive biomarker for treatment response to olaparib. Conclusions: Together, our results demonstrate the potential utility of rapid drug screening combined with genomic profiling for precision treatment of gynecologic cancers.",

keywords = "Gynecologic malignancy, ID2, PARP inhibitor, Pharmacogenomic analysis, TP53 mutations",

author = "Sa, {Jason K.} and Hwang, {Jae Ryoung} and Cho, {Young Jae} and Ryu, {Ji Yoon} and Choi, {Jung Joo} and Jeong, {Soo Young} and Jihye Kim and Kim, {Myeong Seon} and Paik, {E. Sun} and Lee, {Yoo Young} and Choi, {Chel Hun} and Kim, {Tae Joong} and Kim, {Byoung Gie} and Bae, {Duk Soo} and Yeri Lee and Her, {Nam Gu} and Shin, {Yong Jae} and Cho, {Hee Jin} and Kim, {Ja Yeon} and Seo, {Yun Jee} and Harim Koo and Oh, {Jeong Woo} and Taebum Lee and Kim, {Hyun Soo} and Song, {Sang Yong} and Bae, {Joon Seol} and Park, {Woong Yang} and Han, {Hee Dong} and Ahn, {Hyung Jun} and Sood, {Anil K.} and Raul Rabadan and Lee, {Jin Ku} and Nam, {Do Hyun} and Lee, {Jeong Won}",

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doi = "10.1186/s13059-019-1848-3",

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T1 - Pharmacogenomic analysis of patient-derived tumor cells in gynecologic cancers

AU - Sa, Jason K.

AU - Hwang, Jae Ryoung

AU - Cho, Young Jae

AU - Ryu, Ji Yoon

AU - Choi, Jung Joo

AU - Jeong, Soo Young

AU - Kim, Jihye

AU - Kim, Myeong Seon

AU - Paik, E. Sun

AU - Lee, Yoo Young

AU - Choi, Chel Hun

AU - Kim, Tae Joong

AU - Kim, Byoung Gie

AU - Bae, Duk Soo

AU - Lee, Yeri

AU - Her, Nam Gu

AU - Shin, Yong Jae

AU - Cho, Hee Jin

AU - Kim, Ja Yeon

AU - Seo, Yun Jee

AU - Koo, Harim

AU - Oh, Jeong Woo

AU - Lee, Taebum

AU - Kim, Hyun Soo

AU - Song, Sang Yong

AU - Bae, Joon Seol

AU - Park, Woong Yang

AU - Han, Hee Dong

AU - Ahn, Hyung Jun

AU - Sood, Anil K.

AU - Rabadan, Raul

AU - Lee, Jin Ku

AU - Nam, Do Hyun

AU - Lee, Jeong Won

PY - 2019/11/26

Y1 - 2019/11/26

N2 - Background: Gynecologic malignancy is one of the leading causes of mortality in female adults worldwide. Comprehensive genomic analysis has revealed a list of molecular aberrations that are essential to tumorigenesis, progression, and metastasis of gynecologic tumors. However, targeting such alterations has frequently led to treatment failures due to underlying genomic complexity and simultaneous activation of various tumor cell survival pathway molecules. A compilation of molecular characterization of tumors with pharmacological drug response is the next step toward clinical application of patient-tailored treatment regimens. Results: Toward this goal, we establish a library of 139 gynecologic tumors including epithelial ovarian cancers (EOCs), cervical, endometrial tumors, and uterine sarcomas that are genomically and/or pharmacologically annotated and explore dynamic pharmacogenomic associations against 37 molecularly targeted drugs. We discover lineage-specific drug sensitivities based on subcategorization of gynecologic tumors and identify TP53 mutation as a molecular determinant that elicits therapeutic response to poly (ADP-Ribose) polymerase (PARP) inhibitor. We further identify transcriptome expression of inhibitor of DNA biding 2 (ID2) as a potential predictive biomarker for treatment response to olaparib. Conclusions: Together, our results demonstrate the potential utility of rapid drug screening combined with genomic profiling for precision treatment of gynecologic cancers.

AB - Background: Gynecologic malignancy is one of the leading causes of mortality in female adults worldwide. Comprehensive genomic analysis has revealed a list of molecular aberrations that are essential to tumorigenesis, progression, and metastasis of gynecologic tumors. However, targeting such alterations has frequently led to treatment failures due to underlying genomic complexity and simultaneous activation of various tumor cell survival pathway molecules. A compilation of molecular characterization of tumors with pharmacological drug response is the next step toward clinical application of patient-tailored treatment regimens. Results: Toward this goal, we establish a library of 139 gynecologic tumors including epithelial ovarian cancers (EOCs), cervical, endometrial tumors, and uterine sarcomas that are genomically and/or pharmacologically annotated and explore dynamic pharmacogenomic associations against 37 molecularly targeted drugs. We discover lineage-specific drug sensitivities based on subcategorization of gynecologic tumors and identify TP53 mutation as a molecular determinant that elicits therapeutic response to poly (ADP-Ribose) polymerase (PARP) inhibitor. We further identify transcriptome expression of inhibitor of DNA biding 2 (ID2) as a potential predictive biomarker for treatment response to olaparib. Conclusions: Together, our results demonstrate the potential utility of rapid drug screening combined with genomic profiling for precision treatment of gynecologic cancers.

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KW - ID2

KW - PARP inhibitor

KW - Pharmacogenomic analysis

KW - TP53 mutations

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Pharmacogenomic analysis of patient-derived tumor cells in gynecologic cancers

Abstract

Keywords

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