SBME Research Seminar - Dr. Hannah Carter
Immune Checkpoint Blockade (ICB) has revolutionized cancer treatment, however mechanisms determining patient response remain poorly understood. We used machine learning to predict ICB response from germline and somatic biomarkers and studied feature usage by the learned model to uncover putative mechanisms driving superior outcomes. Patients with higher T follicular helper infiltrates were robust to defects in the class-I Major Histocompatibility Complex (MHC-I). Further investigation uncovered different ICB responses in MHC-I versus MHC-II neoantigen reliant tumors across patients. Despite similar response rates, MHC-II reliant responses were associated with significantly longer durable clinical benefit (Discovery: Median OS=63.6 vs. 34.5 months P=0.0074; Validation: Median OS=37.5 vs. 33.1 months, P=0.040). Characteristics of the tumor immune microenvironment reflected MHC neoantigen reliance, and analysis of immune checkpoints revealed LAG3 as a potential target in MHC-II but not MHC-I reliant responses. This study highlights the value of interpretable machine learning models in elucidating the biological basis of therapy responses.
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BMEG 598: March 21st Session
March 21, 2024 @ 11:00 am - 12:00 pm PDT
BMEG 598: March 21st Session
Through the BMEG 598: Biomedical Engineering Seminar, Biomedical Engineering graduate students will be exposed to innovative and cutting-edge research happening both on the UBC campus with their colleagues and around the world. This is session is part of a series of sessions during which students will present their research. The students presenting and the title of their presentation can be found below.
Students Presenting:
• Emily Bliven “A multimodal investigation into mechanically preventing hip fracture with a femoral augmentation“
• Nico Werschler “Engineering human vascular organoids“
Location:
DMCBH 101 LT