A surgical window of opportunity trial evaluating the effect of the PCSK9 inhibitor evolocumab on tumoral MHC-I expression and CD8+ infiltration in glioma.

Many cancers evade immunosurveillance by downregulating surface major histocompatibility class (MHC)-I. Proprotein convertase subtilisin/kexin type 9 (PCSK9) promotes MHC-I degradation and is elevated in glioma. Evolocumab is a clinically approved PCSK9 inhibitor which restores MHC-I expression in pre-clinical cancer models. However, monoclonal antibodies have limited blood brain/tumor barrier penetrance (BBB/BTB). We conducted a window-of-opportunity trial, evaluating evolocumab's BBB/BTB penetrance and biological effect (PesKE; NCT04937413). Patients with newly diagnosed or recurrent glioma undergoing a clinically indicated biopsy or resection were enrolled (n = 32, M: 16, F: 16; control average age: 51.85, evolocumab: 53). Intervention participants (n = 6) received a single subcutaneous evolocumab dose pre-procedure, of which 4 provided research tissue. No significant adverse events were observed. Evolocumab was detected in all analyzed intervention tissue, with an average tumor: blood ratio of 0.0222 (SD ± 0.0190), akin to other monoclonals. Evolocumab quantitation was 4.44× greater in contrast-enhancing (mean 0.0068 fmol/mcg (SD ± 0.001)) vs non-contrast enhancing cases (mean 0.0015 fmol/mcg (SD ± 0.0004)). Proteomic analysis found positive trends between evolocumab and MHC-I subtypes (HLA-A-C, E-G), with a significant positive correlation with HLA-H (R2 = 0.9584, p = 0.021*). Tumor tissue with higher evolocumab titers demonstrated increased surface MHC-I and CD8+ T cell infiltration. Increased CD8+ TNF, FASLG and GZMA transcription was observed in high titer tissue compared to low titer tissue and untreated controls. Pre-resection evolocumab is well tolerated but exhibits BBB/BTB penetrance akin to other monoclonal antibodies. Increased tumoral evolocumab/PCSK9i may enhance tumoral MHC-I/effector CD8+ infiltration. Future work will explore combining evolocumab with BBB/BTB opening therapies like low-intensity focused ultrasound.

Duke Scholars

Author Mustafa Khasraw Neurosurgery

Author David Michael Ashley Neurosurgery

Author Evan Calabrese Radiology, Neuroradiology

Author Anoop Patel Neurosurgery

Author Allan Howard Friedman Neurosurgery

Author Henry Seth Friedman Neurosurgery, Neuro-Oncology

Author Simon Gray Gregory Neurosurgery, Neuro-Oncology

Author Margaret Johnson Neurosurgery

Author James Emmett Herndon II Biostatistics & Bioinformatics, Division of Biostatistics

Author Chuan-Yuan Li Dermatology

Author John Howard Sampson Neurosurgery

Author Stephen Thomas Keir Neurosurgery, Neuro-Oncology

Author Matthew Wolf Foster Medicine, Pulmonary, Allergy, and Critical Care Medicine

Author Gerald Arthur Grant Neurosurgery

Author Annick Desjardins Neurosurgery, Neuro-Oncology

Author Roger Edwin McLendon Pathology

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