Antitumor Activity of Vebreltinib and Characterization of Clinicogenomic Features in Solid Tumors with MET Rearrangements

Seshiru Nakazawa; Federica Pecci; Igor Odintsov; Dimitris Gazgalis; Felix H. Gottlieb; Biagio Ricciuti; Lodovica Zullo; Joao V. Alessi; Alessandro Di Federico; Mihaela Aldea; Edoardo Garbo; Malini M. Gandhi; Arushi Saini; William W. Feng; Jie Jiang; Simon Baldacci; Francesco Facchinetti; Maisam Makarem; Marie Anaïs Locquet; Koji Haratani; Danielle Haradon; Benjamin Besse; Antoine Italiano; Jordi Remon; Pernelle Lavaud; Damien Vasseur; David Planchard; Yusuke Sato; Yukako Watanabe; Scott Owen; Alexis B. Cortot; Hoda Mahran; Martin D. Forster; Jiaxin Niu; Pascale Tomasini; Swan Swan Leong; Kevin Tay; Emilio Esteban; Anna Minchom; Sani H. Kizilbash; Marcia Cruz-Correa; Kin Hung Peony Yu; Xiaoling Zhang; Pan Chen; Mythili Sangem; Jianwei Che; Lynette M. Sholl; Pasi A. Jänne; Mark M. Awad

doi:10.1158/2159-8290.CD-24-1726

Antitumor Activity of Vebreltinib and Characterization of Clinicogenomic Features in Solid Tumors with MET Rearrangements

Seshiru Nakazawa, Federica Pecci, Igor Odintsov, Dimitris Gazgalis, Felix H. Gottlieb, Biagio Ricciuti, Lodovica Zullo, Joao V. Alessi, Alessandro Di Federico, Mihaela Aldea, Edoardo Garbo, Malini M. Gandhi, Arushi Saini, William W. Feng, Jie Jiang, Simon Baldacci, Francesco Facchinetti, Maisam Makarem, Marie Anaïs Locquet, Koji HarataniDanielle Haradon, Benjamin Besse, Antoine Italiano, Jordi Remon, Pernelle Lavaud, Damien Vasseur, David Planchard, Yusuke Sato, Yukako Watanabe, Scott Owen, Alexis B. Cortot, Hoda Mahran, Martin D. Forster, Jiaxin Niu, Pascale Tomasini, Swan Swan Leong, Kevin Tay, Emilio Esteban, Anna Minchom, Sani H. Kizilbash, Marcia Cruz-Correa, Kin Hung Peony Yu, Xiaoling Zhang, Pan Chen, Mythili Sangem, Jianwei Che, Lynette M. Sholl, Pasi A. Jänne, Mark M. Awad

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Résumé

Oncogenic translocations involving the MET gene have been reported in several cancer types, but detailed clinicogenomic characterization of these cancers is not well defined. In addition, prospective clinical trials evaluating the antitumor activity of MET inhibitors in MET rearrangement–positive cancers are limited. In this study, in a pan-cancer analysis of >46,000 solid tumors with comprehensive genomic profiling, we identified oncogenic MET rearrangements in ∼0.04% of cancers. Preliminary analysis from a phase II clinical trial of the type I MET tyrosine kinase inhibitor (TKI) vebreltinib in MET fusion–positive solid tumors demonstrated an objective response rate of 50% and disease control rate of 79%, with antitumor activity seen in diverse cancer types, including lung adenocarcinoma and intrahepatic cholangiocarcinoma, among others. Similar to MET exon 14–altered lung cancer, secondary mutations in the kinase domain can confer resistance to MET TKIs in MET fusion–positive cancers. Overall, these data categorize MET rearrangements as actionable targets in solid tumors. Significance: MET rearrangement–positive cancers are not well-characterized, and optimal treatment strategies are yet to be defined. Through comprehensive genomic analysis, preclinical modeling, and preliminary results of a phase II clinical trial, we demonstrate that MET fusions are a unique molecular subtype of cancers targetable with vebreltinib, a TKI in development.

langue originale	Anglais
Pages (de - à)	1129-1140
Nombre de pages	12
journal	Cancer Discovery
Volume	15
Numéro de publication	6
Les DOIs	https://doi.org/10.1158/2159-8290.CD-24-1726
état	Publié - 1 juin 2025

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10.1158/2159-8290.CD-24-1726

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Nakazawa, S., Pecci, F., Odintsov, I., Gazgalis, D., Gottlieb, F. H., Ricciuti, B., Zullo, L., Alessi, J. V., Di Federico, A., Aldea, M., Garbo, E., Gandhi, M. M., Saini, A., Feng, W. W., Jiang, J., Baldacci, S., Facchinetti, F., Makarem, M., Locquet, M. A., ... Awad, M. M. (2025). Antitumor Activity of Vebreltinib and Characterization of Clinicogenomic Features in Solid Tumors with MET Rearrangements. Cancer Discovery, 15(6), 1129-1140. https://doi.org/10.1158/2159-8290.CD-24-1726

@article{871224cd1a8644cca5c3f8f764702125,

title = "Antitumor Activity of Vebreltinib and Characterization of Clinicogenomic Features in Solid Tumors with MET Rearrangements",

abstract = "Oncogenic translocations involving the MET gene have been reported in several cancer types, but detailed clinicogenomic characterization of these cancers is not well defined. In addition, prospective clinical trials evaluating the antitumor activity of MET inhibitors in MET rearrangement–positive cancers are limited. In this study, in a pan-cancer analysis of >46,000 solid tumors with comprehensive genomic profiling, we identified oncogenic MET rearrangements in ∼0.04\% of cancers. Preliminary analysis from a phase II clinical trial of the type I MET tyrosine kinase inhibitor (TKI) vebreltinib in MET fusion–positive solid tumors demonstrated an objective response rate of 50\% and disease control rate of 79\%, with antitumor activity seen in diverse cancer types, including lung adenocarcinoma and intrahepatic cholangiocarcinoma, among others. Similar to MET exon 14–altered lung cancer, secondary mutations in the kinase domain can confer resistance to MET TKIs in MET fusion–positive cancers. Overall, these data categorize MET rearrangements as actionable targets in solid tumors. Significance: MET rearrangement–positive cancers are not well-characterized, and optimal treatment strategies are yet to be defined. Through comprehensive genomic analysis, preclinical modeling, and preliminary results of a phase II clinical trial, we demonstrate that MET fusions are a unique molecular subtype of cancers targetable with vebreltinib, a TKI in development.",

author = "Seshiru Nakazawa and Federica Pecci and Igor Odintsov and Dimitris Gazgalis and Gottlieb, \{Felix H.\} and Biagio Ricciuti and Lodovica Zullo and Alessi, \{Joao V.\} and \{Di Federico\}, Alessandro and Mihaela Aldea and Edoardo Garbo and Gandhi, \{Malini M.\} and Arushi Saini and Feng, \{William W.\} and Jie Jiang and Simon Baldacci and Francesco Facchinetti and Maisam Makarem and Locquet, \{Marie Ana{\"i}s\} and Koji Haratani and Danielle Haradon and Benjamin Besse and Antoine Italiano and Jordi Remon and Pernelle Lavaud and Damien Vasseur and David Planchard and Yusuke Sato and Yukako Watanabe and Scott Owen and Cortot, \{Alexis B.\} and Hoda Mahran and Forster, \{Martin D.\} and Jiaxin Niu and Pascale Tomasini and Leong, \{Swan Swan\} and Kevin Tay and Emilio Esteban and Anna Minchom and Kizilbash, \{Sani H.\} and Marcia Cruz-Correa and Yu, \{Kin Hung Peony\} and Xiaoling Zhang and Pan Chen and Mythili Sangem and Jianwei Che and Sholl, \{Lynette M.\} and J{\"a}nne, \{Pasi A.\} and Awad, \{Mark M.\}",

year = "2025",

month = jun,

day = "1",

doi = "10.1158/2159-8290.CD-24-1726",

language = "English",

volume = "15",

pages = "1129--1140",

journal = "Cancer Discovery",

issn = "2159-8274",

number = "6",

}

Nakazawa, S, Pecci, F, Odintsov, I, Gazgalis, D, Gottlieb, FH, Ricciuti, B, Zullo, L, Alessi, JV, Di Federico, A, Aldea, M, Garbo, E, Gandhi, MM, Saini, A, Feng, WW, Jiang, J, Baldacci, S, Facchinetti, F, Makarem, M, Locquet, MA, Haratani, K, Haradon, D, Besse, B, Italiano, A, Remon, J, Lavaud, P, Vasseur, D, Planchard, D, Sato, Y, Watanabe, Y, Owen, S, Cortot, AB, Mahran, H, Forster, MD, Niu, J, Tomasini, P, Leong, SS, Tay, K, Esteban, E, Minchom, A, Kizilbash, SH, Cruz-Correa, M, Yu, KHP, Zhang, X, Chen, P, Sangem, M, Che, J, Sholl, LM, Jänne, PA & Awad, MM 2025, 'Antitumor Activity of Vebreltinib and Characterization of Clinicogenomic Features in Solid Tumors with MET Rearrangements', Cancer Discovery, VOL. 15, Numéro 6, p. 1129-1140. https://doi.org/10.1158/2159-8290.CD-24-1726

TY - JOUR

T1 - Antitumor Activity of Vebreltinib and Characterization of Clinicogenomic Features in Solid Tumors with MET Rearrangements

AU - Nakazawa, Seshiru

AU - Pecci, Federica

AU - Odintsov, Igor

AU - Gazgalis, Dimitris

AU - Gottlieb, Felix H.

AU - Ricciuti, Biagio

AU - Zullo, Lodovica

AU - Alessi, Joao V.

AU - Di Federico, Alessandro

AU - Aldea, Mihaela

AU - Garbo, Edoardo

AU - Gandhi, Malini M.

AU - Saini, Arushi

AU - Feng, William W.

AU - Jiang, Jie

AU - Baldacci, Simon

AU - Facchinetti, Francesco

AU - Makarem, Maisam

AU - Locquet, Marie Anaïs

AU - Haratani, Koji

AU - Haradon, Danielle

AU - Besse, Benjamin

AU - Italiano, Antoine

AU - Remon, Jordi

AU - Lavaud, Pernelle

AU - Vasseur, Damien

AU - Planchard, David

AU - Sato, Yusuke

AU - Watanabe, Yukako

AU - Owen, Scott

AU - Cortot, Alexis B.

AU - Mahran, Hoda

AU - Forster, Martin D.

AU - Niu, Jiaxin

AU - Tomasini, Pascale

AU - Leong, Swan Swan

AU - Tay, Kevin

AU - Esteban, Emilio

AU - Minchom, Anna

AU - Kizilbash, Sani H.

AU - Cruz-Correa, Marcia

AU - Yu, Kin Hung Peony

AU - Zhang, Xiaoling

AU - Chen, Pan

AU - Sangem, Mythili

AU - Che, Jianwei

AU - Sholl, Lynette M.

AU - Jänne, Pasi A.

AU - Awad, Mark M.

PY - 2025/6/1

Y1 - 2025/6/1

N2 - Oncogenic translocations involving the MET gene have been reported in several cancer types, but detailed clinicogenomic characterization of these cancers is not well defined. In addition, prospective clinical trials evaluating the antitumor activity of MET inhibitors in MET rearrangement–positive cancers are limited. In this study, in a pan-cancer analysis of >46,000 solid tumors with comprehensive genomic profiling, we identified oncogenic MET rearrangements in ∼0.04% of cancers. Preliminary analysis from a phase II clinical trial of the type I MET tyrosine kinase inhibitor (TKI) vebreltinib in MET fusion–positive solid tumors demonstrated an objective response rate of 50% and disease control rate of 79%, with antitumor activity seen in diverse cancer types, including lung adenocarcinoma and intrahepatic cholangiocarcinoma, among others. Similar to MET exon 14–altered lung cancer, secondary mutations in the kinase domain can confer resistance to MET TKIs in MET fusion–positive cancers. Overall, these data categorize MET rearrangements as actionable targets in solid tumors. Significance: MET rearrangement–positive cancers are not well-characterized, and optimal treatment strategies are yet to be defined. Through comprehensive genomic analysis, preclinical modeling, and preliminary results of a phase II clinical trial, we demonstrate that MET fusions are a unique molecular subtype of cancers targetable with vebreltinib, a TKI in development.

AB - Oncogenic translocations involving the MET gene have been reported in several cancer types, but detailed clinicogenomic characterization of these cancers is not well defined. In addition, prospective clinical trials evaluating the antitumor activity of MET inhibitors in MET rearrangement–positive cancers are limited. In this study, in a pan-cancer analysis of >46,000 solid tumors with comprehensive genomic profiling, we identified oncogenic MET rearrangements in ∼0.04% of cancers. Preliminary analysis from a phase II clinical trial of the type I MET tyrosine kinase inhibitor (TKI) vebreltinib in MET fusion–positive solid tumors demonstrated an objective response rate of 50% and disease control rate of 79%, with antitumor activity seen in diverse cancer types, including lung adenocarcinoma and intrahepatic cholangiocarcinoma, among others. Similar to MET exon 14–altered lung cancer, secondary mutations in the kinase domain can confer resistance to MET TKIs in MET fusion–positive cancers. Overall, these data categorize MET rearrangements as actionable targets in solid tumors. Significance: MET rearrangement–positive cancers are not well-characterized, and optimal treatment strategies are yet to be defined. Through comprehensive genomic analysis, preclinical modeling, and preliminary results of a phase II clinical trial, we demonstrate that MET fusions are a unique molecular subtype of cancers targetable with vebreltinib, a TKI in development.

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U2 - 10.1158/2159-8290.CD-24-1726

DO - 10.1158/2159-8290.CD-24-1726

M3 - Article

C2 - 40202082

AN - SCOPUS:105008357974

SN - 2159-8274

VL - 15

SP - 1129

EP - 1140

JO - Cancer Discovery

JF - Cancer Discovery

IS - 6

ER -