The Hippo pathway mediates Semaphorin signaling

Zhipeng Meng; Fu Long Li; Cao Fang; Benjamin Yeoman; Yunjiang Qiu; Ying Wang; Xiaomin Cai; Kimberly C. Lin; Di Yang; Min Luo; Vivian Fu; Xiaoxiao Ma; Yarui Diao; Filippo G. Giancotti; Bing Ren; Adam J. Engler; Kun Liang Guan

doi:10.1126/sciadv.abl9806

The Hippo pathway mediates Semaphorin signaling

Zhipeng Meng, Fu Long Li, Cao Fang, Benjamin Yeoman, Yunjiang Qiu, Ying Wang, Xiaomin Cai, Kimberly C. Lin, Di Yang, Min Luo, Vivian Fu, Xiaoxiao Ma, Yarui Diao, Filippo G. Giancotti, Bing Ren, Adam J. Engler, Kun Liang Guan

Cancer Biology

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

6 Scopus citations

Abstract

Semaphorins were originally identified as axonal guidance molecules, but they also control processes such as vascular development and tumorigenesis. The downstream signaling cascades of Semaphorins in these biological processes remain unclear. Here, we show that the class 3 Semaphorins (SEMA3s) activate the Hippo pathway to attenuate tissue growth, angiogenesis, and tumorigenesis. SEMA3B restoration in lung cancer cells with SEMA3B loss of heterozygosity suppresses cancer cell growth via activating the core Hippo kinases LATS1/2 (large tumor suppressor kinase 1/2). Furthermore, SEMA3 also acts through LATS1/2 to inhibit angiogenesis. We identified p190RhoGAPs as essential partners of the SEMA3A receptor PlexinA in Hippo regulation. Upon SEMA3 treatment, PlexinA interacts with the pseudo–guanosine triphosphatase (GTPase) domain of p190RhoGAP and simultaneously recruits RND GTPases to activate p190RhoGAP, which then stimulates LATS1/2. Disease-associated etiological factors, such as genetic lesions and oscillatory shear, diminish Hippo pathway regulation by SEMA3. Our study thus discovers a critical role of Hippo signaling in mediating SEMA3 physiological function.

Original language	English (US)
Article number	eabl9806
Journal	Science Advances
Volume	8
Issue number	21
DOIs	https://doi.org/10.1126/sciadv.abl9806
State	Published - May 2022

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title = "The Hippo pathway mediates Semaphorin signaling",

abstract = "Semaphorins were originally identified as axonal guidance molecules, but they also control processes such as vascular development and tumorigenesis. The downstream signaling cascades of Semaphorins in these biological processes remain unclear. Here, we show that the class 3 Semaphorins (SEMA3s) activate the Hippo pathway to attenuate tissue growth, angiogenesis, and tumorigenesis. SEMA3B restoration in lung cancer cells with SEMA3B loss of heterozygosity suppresses cancer cell growth via activating the core Hippo kinases LATS1/2 (large tumor suppressor kinase 1/2). Furthermore, SEMA3 also acts through LATS1/2 to inhibit angiogenesis. We identified p190RhoGAPs as essential partners of the SEMA3A receptor PlexinA in Hippo regulation. Upon SEMA3 treatment, PlexinA interacts with the pseudo–guanosine triphosphatase (GTPase) domain of p190RhoGAP and simultaneously recruits RND GTPases to activate p190RhoGAP, which then stimulates LATS1/2. Disease-associated etiological factors, such as genetic lesions and oscillatory shear, diminish Hippo pathway regulation by SEMA3. Our study thus discovers a critical role of Hippo signaling in mediating SEMA3 physiological function.",

author = "Zhipeng Meng and Li, {Fu Long} and Cao Fang and Benjamin Yeoman and Yunjiang Qiu and Ying Wang and Xiaomin Cai and Lin, {Kimberly C.} and Di Yang and Min Luo and Vivian Fu and Xiaoxiao Ma and Yarui Diao and Giancotti, {Filippo G.} and Bing Ren and Engler, {Adam J.} and Guan, {Kun Liang}",

note = "Publisher Copyright: Copyright {\textcopyright} 2022 The Authors, some rights reserved.",

year = "2022",

month = may,

doi = "10.1126/sciadv.abl9806",

language = "English (US)",

volume = "8",

journal = "Science Advances",

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T1 - The Hippo pathway mediates Semaphorin signaling

AU - Meng, Zhipeng

AU - Li, Fu Long

AU - Fang, Cao

AU - Yeoman, Benjamin

AU - Qiu, Yunjiang

AU - Wang, Ying

AU - Cai, Xiaomin

AU - Lin, Kimberly C.

AU - Yang, Di

AU - Luo, Min

AU - Fu, Vivian

AU - Ma, Xiaoxiao

AU - Diao, Yarui

AU - Giancotti, Filippo G.

AU - Ren, Bing

AU - Engler, Adam J.

AU - Guan, Kun Liang

PY - 2022/5

Y1 - 2022/5

N2 - Semaphorins were originally identified as axonal guidance molecules, but they also control processes such as vascular development and tumorigenesis. The downstream signaling cascades of Semaphorins in these biological processes remain unclear. Here, we show that the class 3 Semaphorins (SEMA3s) activate the Hippo pathway to attenuate tissue growth, angiogenesis, and tumorigenesis. SEMA3B restoration in lung cancer cells with SEMA3B loss of heterozygosity suppresses cancer cell growth via activating the core Hippo kinases LATS1/2 (large tumor suppressor kinase 1/2). Furthermore, SEMA3 also acts through LATS1/2 to inhibit angiogenesis. We identified p190RhoGAPs as essential partners of the SEMA3A receptor PlexinA in Hippo regulation. Upon SEMA3 treatment, PlexinA interacts with the pseudo–guanosine triphosphatase (GTPase) domain of p190RhoGAP and simultaneously recruits RND GTPases to activate p190RhoGAP, which then stimulates LATS1/2. Disease-associated etiological factors, such as genetic lesions and oscillatory shear, diminish Hippo pathway regulation by SEMA3. Our study thus discovers a critical role of Hippo signaling in mediating SEMA3 physiological function.

AB - Semaphorins were originally identified as axonal guidance molecules, but they also control processes such as vascular development and tumorigenesis. The downstream signaling cascades of Semaphorins in these biological processes remain unclear. Here, we show that the class 3 Semaphorins (SEMA3s) activate the Hippo pathway to attenuate tissue growth, angiogenesis, and tumorigenesis. SEMA3B restoration in lung cancer cells with SEMA3B loss of heterozygosity suppresses cancer cell growth via activating the core Hippo kinases LATS1/2 (large tumor suppressor kinase 1/2). Furthermore, SEMA3 also acts through LATS1/2 to inhibit angiogenesis. We identified p190RhoGAPs as essential partners of the SEMA3A receptor PlexinA in Hippo regulation. Upon SEMA3 treatment, PlexinA interacts with the pseudo–guanosine triphosphatase (GTPase) domain of p190RhoGAP and simultaneously recruits RND GTPases to activate p190RhoGAP, which then stimulates LATS1/2. Disease-associated etiological factors, such as genetic lesions and oscillatory shear, diminish Hippo pathway regulation by SEMA3. Our study thus discovers a critical role of Hippo signaling in mediating SEMA3 physiological function.

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The Hippo pathway mediates Semaphorin signaling

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