CDK4/6-MEK Inhibition in MPNSTs Causes Plasma Cell Infiltration, Sensitization to PD-L1 Blockade, and Tumor Regression-Reference-Cited by-同舟云学术

CDK4/6-MEK Inhibition in MPNSTs Causes Plasma Cell Infiltration, Sensitization to PD-L1 Blockade, and Tumor Regression

Published:2023-07-06 Issue:17 Volume:29 Page:3484-3497
ISSN:1078-0432
Container-title:Clinical Cancer Research
language:en
Short-container-title:

Author:

Kohlmeyer Jordan L.¹²^ORCID,Lingo Joshua J.³⁴^ORCID,Kaemmer Courtney A.²^ORCID,Scherer Amanda⁵^ORCID,Warrier Akshaya³⁶^ORCID,Voigt Ellen³⁴⁶^ORCID,Raygoza Garay Juan A.⁴^ORCID,McGivney Gavin R.³^ORCID,Brockman Qierra R.¹^ORCID,Tang Amy⁷^ORCID,Calizo Ana⁸^ORCID,Pollard Kai⁸^ORCID,Zhang Xiaochun⁹^ORCID,Hirbe Angela C.⁹^ORCID,Pratilas Christine A.⁸^ORCID,Leidinger Mariah¹⁰^ORCID,Breheny Patrick⁴¹¹^ORCID,Chimenti Michael S.¹²^ORCID,Sieren Jessica C.⁴¹³^ORCID,Monga Varun⁴⁵^ORCID,Tanas Munir R.¹³⁴¹⁰^ORCID,Meyerholz David K.¹⁰^ORCID,Darbro Benjamin W.⁴⁶¹⁴^ORCID,Dodd Rebecca D.¹³⁴⁵⁶^ORCID,Quelle Dawn E.¹²³⁴⁶¹⁰^ORCID

Affiliation:

1. 1Molecular Medicine Graduate Program, Carver College of Medicine, University of Iowa, Iowa City, Iowa.

2. 2Department of Neuroscience and Pharmacology, Carver College of Medicine, University of Iowa, Iowa City, Iowa.

3. 3Cancer Biology Graduate Program, University of Iowa, Iowa City, Iowa.

4. 4Holden Comprehensive Cancer Center, University of Iowa, Iowa City, Iowa.

5. 5Department of Internal Medicine, Carver College of Medicine, University of Iowa, Iowa City, Iowa.

6. 6Medical Scientist Training Program, Carver College of Medicine, University of Iowa, Iowa City, Iowa.

7. 7Department of Microbiology and Molecular Cell Biology, Leroy T. Canoles Jr. Cancer Center, Eastern Virginia Medical School, Norfolk, Virginia.

8. 8Department of Oncology, Johns Hopkins University, Sidney Kimmel Comprehensive Cancer Center, Baltimore, Maryland.

9. 9Division of Medical Oncology, Washington University, St. Louis, Missouri.

10. 10Department of Pathology, Carver College of Medicine, University of Iowa, Iowa City, Iowa.

11. 11Department of Biostatistics, College of Public Health, University of Iowa, Iowa City, Iowa.

12. 12Iowa Institute of Human Genetics, Carver College of Medicine, University of Iowa, Iowa City, Iowa.

13. 13Department of Radiation, Carver College of Medicine, University of Iowa, Iowa City, Iowa.

14. 14Department of Pediatrics, Carver College of Medicine, University of Iowa, Iowa City, Iowa.

Abstract

AbstractPurpose:Malignant peripheral nerve sheath tumors (MPNST) are lethal, Ras-driven sarcomas that lack effective therapies. We investigated effects of targeting cyclin-dependent kinases 4 and 6 (CDK4/6), MEK, and/or programmed death-ligand 1 (PD-L1) in preclinical MPNST models.Experimental Design:Patient-matched MPNSTs and precursor lesions were examined by FISH, RNA sequencing, IHC, and Connectivity-Map analyses. Antitumor activity of CDK4/6 and MEK inhibitors was measured in MPNST cell lines, patient-derived xenografts (PDX), and de novo mouse MPNSTs, with the latter used to determine anti–PD-L1 response.Results:Patient tumor analyses identified CDK4/6 and MEK as actionable targets for MPNST therapy. Low-dose combinations of CDK4/6 and MEK inhibitors synergistically reactivated the retinoblastoma (RB1) tumor suppressor, induced cell death, and decreased clonogenic survival of MPNST cells. In immune-deficient mice, dual CDK4/6-MEK inhibition slowed tumor growth in 4 of 5 MPNST PDXs. In immunocompetent mice, combination therapy of de novo MPNSTs caused tumor regression, delayed resistant tumor outgrowth, and improved survival relative to monotherapies. Drug-sensitive tumors that regressed contained plasma cells and increased cytotoxic T cells, whereas drug-resistant tumors adopted an immunosuppressive microenvironment with elevated MHC II-low macrophages and increased tumor cell PD-L1 expression. Excitingly, CDK4/6-MEK inhibition sensitized MPNSTs to anti–PD-L1 immune checkpoint blockade (ICB) with some mice showing complete tumor regression.Conclusions:CDK4/6-MEK inhibition induces a novel plasma cell-associated immune response and extended antitumor activity in MPNSTs, which dramatically enhances anti–PD-L1 therapy. These preclinical findings provide strong rationale for clinical translation of CDK4/6-MEK-ICB targeted therapies in MPNST as they may yield sustained antitumor responses and improved patient outcomes.

Funder

National Cancer Institute

National Institute of Neurological Disorders and Stroke

Children's Tumor Foundation

National Institute of General Medical Sciences

NF1 Research Initiative

Publisher

American Association for Cancer Research (AACR)

Subject

Cancer Research,Oncology

Link

https://aacrjournals.org/clincancerres/article-pdf/doi/10.1158/1078-0432.CCR-23-0749/3345900/ccr-23-0749.pdf