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CDK4/6-MEK Inhibition in MPNSTs Causes Plasma Cell Infiltration, Sensitization to PD-L1 Blockade, and Tumor Regression.
Kohlmeyer, Jordan L; Lingo, Joshua J; Kaemmer, Courtney A; Scherer, Amanda; Warrier, Akshaya; Voigt, Ellen; Raygoza Garay, Juan A; McGivney, Gavin R; Brockman, Qierra R; Tang, Amy; Calizo, Ana; Pollard, Kai; Zhang, Xiaochun; Hirbe, Angela C; Pratilas, Christine A; Leidinger, Mariah; Breheny, Patrick; Chimenti, Michael S; Sieren, Jessica C; Monga, Varun; Tanas, Munir R; Meyerholz, David K; Darbro, Benjamin W; Dodd, Rebecca D; Quelle, Dawn E.
Affiliation
  • Kohlmeyer JL; Molecular Medicine Graduate Program, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Lingo JJ; Department of Neuroscience and Pharmacology, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Kaemmer CA; Cancer Biology Graduate Program, University of Iowa, Iowa City, Iowa.
  • Scherer A; Holden Comprehensive Cancer Center, University of Iowa, Iowa City, Iowa.
  • Warrier A; Department of Neuroscience and Pharmacology, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Voigt E; Department of Internal Medicine, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Raygoza Garay JA; Cancer Biology Graduate Program, University of Iowa, Iowa City, Iowa.
  • McGivney GR; Medical Scientist Training Program, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Brockman QR; Cancer Biology Graduate Program, University of Iowa, Iowa City, Iowa.
  • Tang A; Holden Comprehensive Cancer Center, University of Iowa, Iowa City, Iowa.
  • Calizo A; Medical Scientist Training Program, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Pollard K; Holden Comprehensive Cancer Center, University of Iowa, Iowa City, Iowa.
  • Zhang X; Cancer Biology Graduate Program, University of Iowa, Iowa City, Iowa.
  • Hirbe AC; Molecular Medicine Graduate Program, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Pratilas CA; Department of Microbiology and Molecular Cell Biology, Leroy T. Canoles Jr. Cancer Center, Eastern Virginia Medical School, Norfolk, Virginia.
  • Leidinger M; Department of Oncology, Johns Hopkins University, Sidney Kimmel Comprehensive Cancer Center, Baltimore, Maryland.
  • Breheny P; Department of Oncology, Johns Hopkins University, Sidney Kimmel Comprehensive Cancer Center, Baltimore, Maryland.
  • Chimenti MS; Division of Medical Oncology, Washington University, St. Louis, Missouri.
  • Sieren JC; Division of Medical Oncology, Washington University, St. Louis, Missouri.
  • Monga V; Department of Oncology, Johns Hopkins University, Sidney Kimmel Comprehensive Cancer Center, Baltimore, Maryland.
  • Tanas MR; Department of Pathology, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Meyerholz DK; Holden Comprehensive Cancer Center, University of Iowa, Iowa City, Iowa.
  • Darbro BW; Department of Biostatistics, College of Public Health, University of Iowa, Iowa City, Iowa.
  • Dodd RD; Iowa Institute of Human Genetics, Carver College of Medicine, University of Iowa, Iowa City, Iowa.
  • Quelle DE; Holden Comprehensive Cancer Center, University of Iowa, Iowa City, Iowa.
Clin Cancer Res ; 29(17): 3484-3497, 2023 09 01.
Article in En | MEDLINE | ID: mdl-37410426
PURPOSE: 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.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Neurofibrosarcoma Type of study: Etiology_studies / Prognostic_studies Limits: Animals / Humans Language: En Journal: Clin Cancer Res Journal subject: NEOPLASIAS Year: 2023 Type: Article
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Neurofibrosarcoma Type of study: Etiology_studies / Prognostic_studies Limits: Animals / Humans Language: En Journal: Clin Cancer Res Journal subject: NEOPLASIAS Year: 2023 Type: Article