PI3K/mTOR inhibition induces tumour microenvironment remodelling and sensitises pS6<sup>high</sup> uterine leiomyosarcoma to PD‐1 blockade-Reference-Cited by-同舟云学术

PI3K/mTOR inhibition induces tumour microenvironment remodelling and sensitises pS6^high uterine leiomyosarcoma to PD‐1 blockade

Published:2024-05 Issue:5 Volume:14 Page:
ISSN:2001-1326
Container-title:Clinical and Translational Medicine
language:en
Short-container-title:Clinical & Translational Med

Author:

De Wispelaere Wout¹²³,Annibali Daniela¹⁴^ORCID,Tuyaerts Sandra⁵,Messiaen Julie⁶⁷,Antoranz Asier⁶,Shankar Gautam⁶,Dubroja Nikolina⁶,Herreros‐Pomares Alejandro¹⁸,Baiden‐Amissah Regina E. M.¹,Orban Marie‐Pauline⁹¹⁰,Delfini Marcello⁹¹⁰,Berardi Emanuele¹¹,Van Brussel Thomas²³,Schepers Rogier²³,Philips Gino²³,Boeckx Bram²³,Baietti Maria Francesca¹²,Congedo Luigi¹,HoWangYin Kiave Yune¹³,Bayon Emilie¹³,Van Rompuy Anne‐Sophie¹⁴,Leucci Eleonora¹²,Tabruyn Sebastien P.¹³,Bosisio Francesca⁶,Mazzone Massimiliano⁹¹⁰,Lambrechts Diether²³,Amant Frédéric¹⁴¹⁵^ORCID

Affiliation:

1. Department of Oncology Laboratory of Gynecological Oncology University of Leuven Leuven Belgium

2. Department of Human Genetics Laboratory for Translational Genetics University of Leuven Leuven Belgium

3. Laboratory for Translational Genetics Center for Cancer Biology (CCB) Flemish Institute of Biotechnology (VIB) Leuven Belgium

4. Department of Gynecological Oncology Antoni Van Leeuwenhoek – Netherlands Cancer Institute Amsterdam The Netherlands

5. Department of Medical Oncology Laboratory of Medical and Molecular Oncology (LMMO) Vrije Universiteit Brussel – UZ Brussel Brussels Belgium

6. Department of Imaging and Pathology Translational Cell and Tissue Research University of Leuven Leuven Belgium

7. Department of Pediatrics University Hospitals Leuven Leuven Belgium

8. Department of Biotechnology Universitat Politècnica de Valencia Valencia Spain

9. Laboratory of Tumor Inflammation and Angiogenesis Center for Cancer Biology (CCB) Flemish Institute of Biotechnology (VIB) Leuven Belgium

10. Department of Oncology Laboratory of Tumor Inflammation and Angiogenesis Center for Cancer Biology (CCB) University of Leuven Leuven Belgium

11. Department of Development and Regeneration Laboratory of Tissue Engineering University of Leuven Kortrijk Belgium

12. TRACE, Department of Oncology University of Leuven Leuven Belgium

13. TransCure bioServices Archamps France

14. Department of Pathology University Hospitals Leuven Leuven Belgium

15. Department of Obstetrics and Gynecology University Hospitals Leuven Leuven Belgium

Abstract

AbstractBackgroundUterine leiomyosarcomas (uLMS) are aggressive tumours with poor prognosis and limited treatment options. Although immune checkpoint blockade (ICB) has proven effective in some ‘challenging‐to‐treat’ cancers, clinical trials showed that uLMS do not respond to ICB. Emerging evidence suggests that aberrant PI3K/mTOR signalling can drive resistance to ICB. We therefore explored the relevance of the PI3K/mTOR pathway for ICB treatment in uLMS and explored pharmacological inhibition of this pathway to sensitise these tumours to ICB.MethodsWe performed an integrated multiomics analysis based on TCGA data to explore the correlation between PI3K/mTOR dysregulation and immune infiltration in 101 LMS. We assessed response to PI3K/mTOR inhibitors in immunodeficient and humanized uLMS patient‐derived xenografts (PDXs) by evaluating tumour microenvironment modulation using multiplex immunofluorescence. We explored response to single‐agent and a combination of PI3K/mTOR inhibitors with PD‐1 blockade in humanized uLMS PDXs. We mapped intratumoural dynamics using single‐cell RNA/TCR sequencing of serially collected biopsies.ResultsPI3K/mTOR over‐activation (pS6high) associated with lymphocyte depletion and wound healing immune landscapes in (u)LMS, suggesting it contributes to immune evasion. In contrast, PI3K/mTOR inhibition induced profound tumour microenvironment remodelling in an ICB‐resistant humanized uLMS PDX model, fostering adaptive anti‐tumour immune responses. Indeed, PI3K/mTOR inhibition induced macrophage repolarisation towards an anti‐tumourigenic phenotype and increased antigen presentation on dendritic and tumour cells, but also promoted infiltration of PD‐1+ T cells displaying an exhausted phenotype. When combined with anti‐PD‐1, PI3K/mTOR inhibition led to partial or complete tumour responses, whereas no response to single‐agent anti‐PD‐1 was observed. Combination therapy reinvigorated exhausted T cells and induced clonal hyper‐expansion of a cytotoxic CD8+ T‐cell population supported by a CD4+ Th1 niche.ConclusionsOur findings indicate that aberrant PI3K/mTOR pathway activation contributes to immune escape in uLMS and provides a rationale for combining PI3K/mTOR inhibition with ICB for the treatment of this patient population.

Funder

Kom op tegen Kanker

Stichting Tegen Kanker

Fonds Wetenschappelijk Onderzoek

HORIZON EUROPE Marie Sklodowska-Curie Actions

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/ctm2.1655

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