Deciphering resistance mechanisms in cancer: final report of MATCH-R study with a focus on molecular drivers and PDX development

Damien Vasseur; Ludovic Bigot; Kristi Beshiri; Juan Flórez-Arango; Francesco Facchinetti; Antoine Hollebecque; Lambros Tselikas; Mihaela Aldea; Felix Blanc-Durand; Anas Gazzah; David Planchard; Ludovic Lacroix; Noémie Pata-Merci; Catline Nobre; Alice Da Silva; Claudio Nicotra; Maud Ngo-Camus; Floriane Braye; Sergey I. Nikolaev; Stefan Michiels; Gérôme Jules-Clement; Ken André Olaussen; Fabrice André; Jean Yves Scoazec; Fabrice Barlesi; Santiago Ponce; Jean Charles Soria; Benjamin Besse; Yohann Loriot; Luc Friboulet

doi:10.1186/s12943-024-02134-4

Deciphering resistance mechanisms in cancer: final report of MATCH-R study with a focus on molecular drivers and PDX development

Damien Vasseur, Ludovic Bigot, Kristi Beshiri, Juan Flórez-Arango, Francesco Facchinetti, Antoine Hollebecque, Lambros Tselikas, Mihaela Aldea, Felix Blanc-Durand, Anas Gazzah, David Planchard, Ludovic Lacroix, Noémie Pata-Merci, Catline Nobre, Alice Da Silva, Claudio Nicotra, Maud Ngo-Camus, Floriane Braye, Sergey I. Nikolaev, Stefan MichielsGérôme Jules-Clement, Ken André Olaussen, Fabrice André, Jean Yves Scoazec, Fabrice Barlesi, Santiago Ponce, Jean Charles Soria, Benjamin Besse, Yohann Loriot, Luc Friboulet

Résultats de recherche: Contribution à un journal › Article › Revue par des pairs

Résumé

Background: Understanding the resistance mechanisms of tumor is crucial for advancing cancer therapies. The prospective MATCH-R trial (NCT02517892), led by Gustave Roussy, aimed to characterize resistance mechanisms to cancer treatments through molecular analysis of fresh tumor biopsies. This report presents the genomic data analysis of the MATCH-R study conducted from 2015 to 2022 and focuses on targeted therapies. Methods: The study included resistant metastatic patients (pts) who accepted an image-guided tumor biopsy. After evaluation of tumor content (TC) in frozen tissue biopsies, targeted NGS (10 < TC < 30%) or Whole Exome Sequencing and RNA sequencing (TC > 30%) were performed before and/or after the anticancer therapy. Patient-derived xenografts (PDX) were established by implanting tumor fragments into NOD scid gamma mice and amplified up to five passages. Results: A total of 1,120 biopsies were collected from 857 pts with the most frequent tumor types being lung (38.8%), digestive (16.3%) and prostate (14.1%) cancer. Molecular targetable driver were identified in 30.9% (n = 265/857) of the patients, with EGFR (41.5%), FGFR2/3 (15.5%), ALK (11.7%), BRAF (6.8%), and KRAS (5.7%) being the most common altered genes. Furthermore, 66.0% (n = 175/265) had a biopsy at progression on targeted therapy. Among resistant cases, 41.1% (n = 72/175) had no identified molecular mechanism, 32.0% (n = 56/175) showed on-target resistance, and 25.1% (n = 44/175) exhibited a by-pass resistance mechanism. Molecular profiling of the 44 patients with by-pass resistance identified 51 variants, with KRAS (13.7%), PIK3CA (11.8%), PTEN (11.8%), NF2 (7.8%), AKT1 (5.9%), and NF1 (5.9%) being the most altered genes. Treatment was tailored for 45% of the patients with a resistance mechanism identified leading to an 11 months median extension of clinical benefit. A total of 341 biopsies were implanted in mice, successfully establishing 136 PDX models achieving a 39.9% success rate. PDX models are available for EGFR (n = 31), FGFR2/3 (n = 26), KRAS (n = 18), ALK (n = 16), BRAF (n = 6) and NTRK (n = 2) driven cancers. These models closely recapitulate the biology of the original tumors in term of molecular alterations and pharmacological status, and served as valuable models to validate overcoming treatment strategies. Conclusion: The MATCH-R study highlights the feasibility of on purpose image guided tumor biopsies and PDX establishment to characterize resistance mechanisms and guide personalized therapies to improve outcomes in pre-treated metastatic patients. Graphical Abstract: (Figure presented.)

langue originale	Anglais
Numéro d'article	221
journal	Molecular Cancer
Volume	23
Numéro de publication	1
Les DOIs	https://doi.org/10.1186/s12943-024-02134-4
état	Publié - 1 déc. 2024

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10.1186/s12943-024-02134-4

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Vasseur, D., Bigot, L., Beshiri, K., Flórez-Arango, J., Facchinetti, F., Hollebecque, A., Tselikas, L., Aldea, M., Blanc-Durand, F., Gazzah, A., Planchard, D., Lacroix, L., Pata-Merci, N., Nobre, C., Da Silva, A., Nicotra, C., Ngo-Camus, M., Braye, F., Nikolaev, S. I., ... Friboulet, L. (2024). Deciphering resistance mechanisms in cancer: final report of MATCH-R study with a focus on molecular drivers and PDX development. Molecular Cancer, 23(1), Article 221. https://doi.org/10.1186/s12943-024-02134-4

@article{a1237d5c8992469595cb5628fce6be0c,

title = "Deciphering resistance mechanisms in cancer: final report of MATCH-R study with a focus on molecular drivers and PDX development",

abstract = "Background: Understanding the resistance mechanisms of tumor is crucial for advancing cancer therapies. The prospective MATCH-R trial (NCT02517892), led by Gustave Roussy, aimed to characterize resistance mechanisms to cancer treatments through molecular analysis of fresh tumor biopsies. This report presents the genomic data analysis of the MATCH-R study conducted from 2015 to 2022 and focuses on targeted therapies. Methods: The study included resistant metastatic patients (pts) who accepted an image-guided tumor biopsy. After evaluation of tumor content (TC) in frozen tissue biopsies, targeted NGS (10 < TC < 30%) or Whole Exome Sequencing and RNA sequencing (TC > 30%) were performed before and/or after the anticancer therapy. Patient-derived xenografts (PDX) were established by implanting tumor fragments into NOD scid gamma mice and amplified up to five passages. Results: A total of 1,120 biopsies were collected from 857 pts with the most frequent tumor types being lung (38.8%), digestive (16.3%) and prostate (14.1%) cancer. Molecular targetable driver were identified in 30.9% (n = 265/857) of the patients, with EGFR (41.5%), FGFR2/3 (15.5%), ALK (11.7%), BRAF (6.8%), and KRAS (5.7%) being the most common altered genes. Furthermore, 66.0% (n = 175/265) had a biopsy at progression on targeted therapy. Among resistant cases, 41.1% (n = 72/175) had no identified molecular mechanism, 32.0% (n = 56/175) showed on-target resistance, and 25.1% (n = 44/175) exhibited a by-pass resistance mechanism. Molecular profiling of the 44 patients with by-pass resistance identified 51 variants, with KRAS (13.7%), PIK3CA (11.8%), PTEN (11.8%), NF2 (7.8%), AKT1 (5.9%), and NF1 (5.9%) being the most altered genes. Treatment was tailored for 45% of the patients with a resistance mechanism identified leading to an 11 months median extension of clinical benefit. A total of 341 biopsies were implanted in mice, successfully establishing 136 PDX models achieving a 39.9% success rate. PDX models are available for EGFR (n = 31), FGFR2/3 (n = 26), KRAS (n = 18), ALK (n = 16), BRAF (n = 6) and NTRK (n = 2) driven cancers. These models closely recapitulate the biology of the original tumors in term of molecular alterations and pharmacological status, and served as valuable models to validate overcoming treatment strategies. Conclusion: The MATCH-R study highlights the feasibility of on purpose image guided tumor biopsies and PDX establishment to characterize resistance mechanisms and guide personalized therapies to improve outcomes in pre-treated metastatic patients. Graphical Abstract: (Figure presented.)",

keywords = "Biopsy, Cancer, Metastatic, PDX, Resistance, Targeted therapy",

author = "Damien Vasseur and Ludovic Bigot and Kristi Beshiri and Juan Fl{\'o}rez-Arango and Francesco Facchinetti and Antoine Hollebecque and Lambros Tselikas and Mihaela Aldea and Felix Blanc-Durand and Anas Gazzah and David Planchard and Ludovic Lacroix and No{\'e}mie Pata-Merci and Catline Nobre and {Da Silva}, Alice and Claudio Nicotra and Maud Ngo-Camus and Floriane Braye and Nikolaev, {Sergey I.} and Stefan Michiels and G{\'e}r{\^o}me Jules-Clement and Olaussen, {Ken Andr{\'e}} and Fabrice Andr{\'e} and Scoazec, {Jean Yves} and Fabrice Barlesi and Santiago Ponce and Soria, {Jean Charles} and Benjamin Besse and Yohann Loriot and Luc Friboulet",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2024",

month = dec,

day = "1",

doi = "10.1186/s12943-024-02134-4",

language = "English",

volume = "23",

journal = "Molecular Cancer",

issn = "1476-4598",

number = "1",

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Vasseur, D, Bigot, L, Beshiri, K, Flórez-Arango, J, Facchinetti, F, Hollebecque, A, Tselikas, L, Aldea, M, Blanc-Durand, F, Gazzah, A, Planchard, D, Lacroix, L, Pata-Merci, N, Nobre, C, Da Silva, A, Nicotra, C, Ngo-Camus, M, Braye, F, Nikolaev, SI, Michiels, S, Jules-Clement, G, Olaussen, KA, André, F, Scoazec, JY, Barlesi, F, Ponce, S, Soria, JC, Besse, B, Loriot, Y & Friboulet, L 2024, 'Deciphering resistance mechanisms in cancer: final report of MATCH-R study with a focus on molecular drivers and PDX development', Molecular Cancer, VOL. 23, Numéro 1, 221. https://doi.org/10.1186/s12943-024-02134-4

TY - JOUR

T1 - Deciphering resistance mechanisms in cancer

T2 - final report of MATCH-R study with a focus on molecular drivers and PDX development

AU - Vasseur, Damien

AU - Bigot, Ludovic

AU - Beshiri, Kristi

AU - Flórez-Arango, Juan

AU - Facchinetti, Francesco

AU - Hollebecque, Antoine

AU - Tselikas, Lambros

AU - Aldea, Mihaela

AU - Blanc-Durand, Felix

AU - Gazzah, Anas

AU - Planchard, David

AU - Lacroix, Ludovic

AU - Pata-Merci, Noémie

AU - Nobre, Catline

AU - Da Silva, Alice

AU - Nicotra, Claudio

AU - Ngo-Camus, Maud

AU - Braye, Floriane

AU - Nikolaev, Sergey I.

AU - Michiels, Stefan

AU - Jules-Clement, Gérôme

AU - Olaussen, Ken André

AU - André, Fabrice

AU - Scoazec, Jean Yves

AU - Barlesi, Fabrice

AU - Ponce, Santiago

AU - Soria, Jean Charles

AU - Besse, Benjamin

AU - Loriot, Yohann

AU - Friboulet, Luc

PY - 2024/12/1

Y1 - 2024/12/1

N2 - Background: Understanding the resistance mechanisms of tumor is crucial for advancing cancer therapies. The prospective MATCH-R trial (NCT02517892), led by Gustave Roussy, aimed to characterize resistance mechanisms to cancer treatments through molecular analysis of fresh tumor biopsies. This report presents the genomic data analysis of the MATCH-R study conducted from 2015 to 2022 and focuses on targeted therapies. Methods: The study included resistant metastatic patients (pts) who accepted an image-guided tumor biopsy. After evaluation of tumor content (TC) in frozen tissue biopsies, targeted NGS (10 < TC < 30%) or Whole Exome Sequencing and RNA sequencing (TC > 30%) were performed before and/or after the anticancer therapy. Patient-derived xenografts (PDX) were established by implanting tumor fragments into NOD scid gamma mice and amplified up to five passages. Results: A total of 1,120 biopsies were collected from 857 pts with the most frequent tumor types being lung (38.8%), digestive (16.3%) and prostate (14.1%) cancer. Molecular targetable driver were identified in 30.9% (n = 265/857) of the patients, with EGFR (41.5%), FGFR2/3 (15.5%), ALK (11.7%), BRAF (6.8%), and KRAS (5.7%) being the most common altered genes. Furthermore, 66.0% (n = 175/265) had a biopsy at progression on targeted therapy. Among resistant cases, 41.1% (n = 72/175) had no identified molecular mechanism, 32.0% (n = 56/175) showed on-target resistance, and 25.1% (n = 44/175) exhibited a by-pass resistance mechanism. Molecular profiling of the 44 patients with by-pass resistance identified 51 variants, with KRAS (13.7%), PIK3CA (11.8%), PTEN (11.8%), NF2 (7.8%), AKT1 (5.9%), and NF1 (5.9%) being the most altered genes. Treatment was tailored for 45% of the patients with a resistance mechanism identified leading to an 11 months median extension of clinical benefit. A total of 341 biopsies were implanted in mice, successfully establishing 136 PDX models achieving a 39.9% success rate. PDX models are available for EGFR (n = 31), FGFR2/3 (n = 26), KRAS (n = 18), ALK (n = 16), BRAF (n = 6) and NTRK (n = 2) driven cancers. These models closely recapitulate the biology of the original tumors in term of molecular alterations and pharmacological status, and served as valuable models to validate overcoming treatment strategies. Conclusion: The MATCH-R study highlights the feasibility of on purpose image guided tumor biopsies and PDX establishment to characterize resistance mechanisms and guide personalized therapies to improve outcomes in pre-treated metastatic patients. Graphical Abstract: (Figure presented.)

AB - Background: Understanding the resistance mechanisms of tumor is crucial for advancing cancer therapies. The prospective MATCH-R trial (NCT02517892), led by Gustave Roussy, aimed to characterize resistance mechanisms to cancer treatments through molecular analysis of fresh tumor biopsies. This report presents the genomic data analysis of the MATCH-R study conducted from 2015 to 2022 and focuses on targeted therapies. Methods: The study included resistant metastatic patients (pts) who accepted an image-guided tumor biopsy. After evaluation of tumor content (TC) in frozen tissue biopsies, targeted NGS (10 < TC < 30%) or Whole Exome Sequencing and RNA sequencing (TC > 30%) were performed before and/or after the anticancer therapy. Patient-derived xenografts (PDX) were established by implanting tumor fragments into NOD scid gamma mice and amplified up to five passages. Results: A total of 1,120 biopsies were collected from 857 pts with the most frequent tumor types being lung (38.8%), digestive (16.3%) and prostate (14.1%) cancer. Molecular targetable driver were identified in 30.9% (n = 265/857) of the patients, with EGFR (41.5%), FGFR2/3 (15.5%), ALK (11.7%), BRAF (6.8%), and KRAS (5.7%) being the most common altered genes. Furthermore, 66.0% (n = 175/265) had a biopsy at progression on targeted therapy. Among resistant cases, 41.1% (n = 72/175) had no identified molecular mechanism, 32.0% (n = 56/175) showed on-target resistance, and 25.1% (n = 44/175) exhibited a by-pass resistance mechanism. Molecular profiling of the 44 patients with by-pass resistance identified 51 variants, with KRAS (13.7%), PIK3CA (11.8%), PTEN (11.8%), NF2 (7.8%), AKT1 (5.9%), and NF1 (5.9%) being the most altered genes. Treatment was tailored for 45% of the patients with a resistance mechanism identified leading to an 11 months median extension of clinical benefit. A total of 341 biopsies were implanted in mice, successfully establishing 136 PDX models achieving a 39.9% success rate. PDX models are available for EGFR (n = 31), FGFR2/3 (n = 26), KRAS (n = 18), ALK (n = 16), BRAF (n = 6) and NTRK (n = 2) driven cancers. These models closely recapitulate the biology of the original tumors in term of molecular alterations and pharmacological status, and served as valuable models to validate overcoming treatment strategies. Conclusion: The MATCH-R study highlights the feasibility of on purpose image guided tumor biopsies and PDX establishment to characterize resistance mechanisms and guide personalized therapies to improve outcomes in pre-treated metastatic patients. Graphical Abstract: (Figure presented.)

KW - Biopsy

KW - Cancer

KW - Metastatic

KW - PDX

KW - Resistance

KW - Targeted therapy

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DO - 10.1186/s12943-024-02134-4

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AN - SCOPUS:85205605475

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JO - Molecular Cancer

JF - Molecular Cancer

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M1 - 221

ER -