Ectopic JAK–STAT activation enables the transition to a stem-like and multilineage state conferring AR-targeted therapy resistance

Su Deng; Choushi Wang; Yunguan Wang; Yaru Xu; Xiaoling Li; Nickolas A. Johnson; Atreyi Mukherji; U. Ging Lo; Lingfan Xu; Julisa Gonzalez; Lauren A. Metang; Jianfeng Ye; Carla Rodriguez Tirado; Kathia Rodarte; Yinglu Zhou; Zhiqun Xie; Carlos Arana; Valli Annamalai; Xihui Liu; Donald J. Vander Griend; Douglas Strand; Jer Tsong Hsieh; Bo Li; Ganesh Raj; Tao Wang; Ping Mu

doi:10.1038/s43018-022-00431-9

Ectopic JAK–STAT activation enables the transition to a stem-like and multilineage state conferring AR-targeted therapy resistance

Su Deng, Choushi Wang, Yunguan Wang, Yaru Xu, Xiaoling Li, Nickolas A. Johnson, Atreyi Mukherji, U. Ging Lo, Lingfan Xu, Julisa Gonzalez, Lauren A. Metang, Jianfeng Ye, Carla Rodriguez Tirado, Kathia Rodarte, Yinglu Zhou, Zhiqun Xie, Carlos Arana, Valli Annamalai, Xihui Liu, Donald J. Vander GriendDouglas Strand, Jer Tsong Hsieh, Bo Li, Ganesh Raj, Tao Wang, Ping Mu

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

35 Scopus citations

Abstract

Emerging evidence indicates that various cancers can gain resistance to targeted therapies by acquiring lineage plasticity. Although various genomic and transcriptomic aberrations correlate with lineage plasticity, the molecular mechanisms enabling the acquisition of lineage plasticity have not been fully elucidated. We reveal that Janus kinase (JAK)–signal transducer and activator of transcription (STAT) signaling is a crucial executor in promoting lineage plasticity-driven androgen receptor (AR)-targeted therapy resistance in prostate cancer. Importantly, ectopic JAK–STAT activation is specifically required for the resistance of stem-like subclones expressing multilineage transcriptional programs but not subclones exclusively expressing the neuroendocrine-like lineage program. Both genetic and pharmaceutical inhibition of JAK–STAT signaling resensitizes resistant tumors to AR-targeted therapy. Together, these results suggest that JAK–STAT are compelling therapeutic targets for overcoming lineage plasticity-driven AR-targeted therapy resistance.

Original language	English (US)
Pages (from-to)	1071-1087
Number of pages	17
Journal	Nature Cancer
Volume	3
Issue number	9
DOIs	https://doi.org/10.1038/s43018-022-00431-9
State	Published - Sep 2022

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1038/s43018-022-00431-9

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Deng, S., Wang, C., Wang, Y., Xu, Y., Li, X., Johnson, N. A., Mukherji, A., Lo, U. G., Xu, L., Gonzalez, J., Metang, L. A., Ye, J., Tirado, C. R., Rodarte, K., Zhou, Y., Xie, Z., Arana, C., Annamalai, V., Liu, X., ... Mu, P. (2022). Ectopic JAK–STAT activation enables the transition to a stem-like and multilineage state conferring AR-targeted therapy resistance. Nature Cancer, 3(9), 1071-1087. https://doi.org/10.1038/s43018-022-00431-9

Deng, S, Wang, C, Wang, Y, Xu, Y, Li, X, Johnson, NA, Mukherji, A, Lo, UG, Xu, L, Gonzalez, J, Metang, LA, Ye, J, Tirado, CR, Rodarte, K, Zhou, Y, Xie, Z, Arana, C, Annamalai, V, Liu, X, Vander Griend, DJ, Strand, D , Hsieh, JT, Li, B, Raj, G , Wang, T & Mu, P 2022, 'Ectopic JAK–STAT activation enables the transition to a stem-like and multilineage state conferring AR-targeted therapy resistance', Nature Cancer, vol. 3, no. 9, pp. 1071-1087. https://doi.org/10.1038/s43018-022-00431-9

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title = "Ectopic JAK–STAT activation enables the transition to a stem-like and multilineage state conferring AR-targeted therapy resistance",

abstract = "Emerging evidence indicates that various cancers can gain resistance to targeted therapies by acquiring lineage plasticity. Although various genomic and transcriptomic aberrations correlate with lineage plasticity, the molecular mechanisms enabling the acquisition of lineage plasticity have not been fully elucidated. We reveal that Janus kinase (JAK)–signal transducer and activator of transcription (STAT) signaling is a crucial executor in promoting lineage plasticity-driven androgen receptor (AR)-targeted therapy resistance in prostate cancer. Importantly, ectopic JAK–STAT activation is specifically required for the resistance of stem-like subclones expressing multilineage transcriptional programs but not subclones exclusively expressing the neuroendocrine-like lineage program. Both genetic and pharmaceutical inhibition of JAK–STAT signaling resensitizes resistant tumors to AR-targeted therapy. Together, these results suggest that JAK–STAT are compelling therapeutic targets for overcoming lineage plasticity-driven AR-targeted therapy resistance.",

author = "Su Deng and Choushi Wang and Yunguan Wang and Yaru Xu and Xiaoling Li and Johnson, {Nickolas A.} and Atreyi Mukherji and Lo, {U. Ging} and Lingfan Xu and Julisa Gonzalez and Metang, {Lauren A.} and Jianfeng Ye and Tirado, {Carla Rodriguez} and Kathia Rodarte and Yinglu Zhou and Zhiqun Xie and Carlos Arana and Valli Annamalai and Xihui Liu and {Vander Griend}, {Donald J.} and Douglas Strand and Hsieh, {Jer Tsong} and Bo Li and Ganesh Raj and Tao Wang and Ping Mu",

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year = "2022",

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doi = "10.1038/s43018-022-00431-9",

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T1 - Ectopic JAK–STAT activation enables the transition to a stem-like and multilineage state conferring AR-targeted therapy resistance

AU - Deng, Su

AU - Wang, Choushi

AU - Wang, Yunguan

AU - Xu, Yaru

AU - Li, Xiaoling

AU - Johnson, Nickolas A.

AU - Mukherji, Atreyi

AU - Lo, U. Ging

AU - Xu, Lingfan

AU - Gonzalez, Julisa

AU - Metang, Lauren A.

AU - Ye, Jianfeng

AU - Tirado, Carla Rodriguez

AU - Rodarte, Kathia

AU - Zhou, Yinglu

AU - Xie, Zhiqun

AU - Arana, Carlos

AU - Annamalai, Valli

AU - Liu, Xihui

AU - Vander Griend, Donald J.

AU - Strand, Douglas

AU - Hsieh, Jer Tsong

AU - Li, Bo

AU - Raj, Ganesh

AU - Wang, Tao

AU - Mu, Ping

PY - 2022/9

Y1 - 2022/9

N2 - Emerging evidence indicates that various cancers can gain resistance to targeted therapies by acquiring lineage plasticity. Although various genomic and transcriptomic aberrations correlate with lineage plasticity, the molecular mechanisms enabling the acquisition of lineage plasticity have not been fully elucidated. We reveal that Janus kinase (JAK)–signal transducer and activator of transcription (STAT) signaling is a crucial executor in promoting lineage plasticity-driven androgen receptor (AR)-targeted therapy resistance in prostate cancer. Importantly, ectopic JAK–STAT activation is specifically required for the resistance of stem-like subclones expressing multilineage transcriptional programs but not subclones exclusively expressing the neuroendocrine-like lineage program. Both genetic and pharmaceutical inhibition of JAK–STAT signaling resensitizes resistant tumors to AR-targeted therapy. Together, these results suggest that JAK–STAT are compelling therapeutic targets for overcoming lineage plasticity-driven AR-targeted therapy resistance.

AB - Emerging evidence indicates that various cancers can gain resistance to targeted therapies by acquiring lineage plasticity. Although various genomic and transcriptomic aberrations correlate with lineage plasticity, the molecular mechanisms enabling the acquisition of lineage plasticity have not been fully elucidated. We reveal that Janus kinase (JAK)–signal transducer and activator of transcription (STAT) signaling is a crucial executor in promoting lineage plasticity-driven androgen receptor (AR)-targeted therapy resistance in prostate cancer. Importantly, ectopic JAK–STAT activation is specifically required for the resistance of stem-like subclones expressing multilineage transcriptional programs but not subclones exclusively expressing the neuroendocrine-like lineage program. Both genetic and pharmaceutical inhibition of JAK–STAT signaling resensitizes resistant tumors to AR-targeted therapy. Together, these results suggest that JAK–STAT are compelling therapeutic targets for overcoming lineage plasticity-driven AR-targeted therapy resistance.

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Ectopic JAK–STAT activation enables the transition to a stem-like and multilineage state conferring AR-targeted therapy resistance

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