Guillaume Andrieu PhD and Jordan Shafran report research on new mechanisms to develop immunotherapy for triple negative breast cancer
The research team of Andrieu and Shafran, directed by Gerald Denis PhD, in the BU-BMC Cancer Center, has just reported that “BET bromodomain targeting suppresses the PD-1/PD-L1 pathway in triple-negative breast cancer and elicits anti-tumor immune response”, which appeared today in Cell Reports ‘Sneak Peek’ https://papers.ssrn.com/sol3/papers.cfm?abstract_id=3260754
The mechanisms that control the expression of immune inhibitory molecules in diverse cancer types, such as PD-L1, and host immune receptors such as PD-1 on T cells in the tumor microenvironment, are being investigated urgently. New tools to inhibit these checkpoints show great promise to unleash anti-tumor immunity, and results of recent cancer clinical trials are encouraging. Immunotherapy as an exciting and evolving field was recognized on October 1, 2018, with the award of the Nobel Prize in Medicine to Honjo and Allison. On the other hand, clinical cases in which immune therapy approaches fail are poorly understood, and failure is common enough for certain cancer types to have caused widespread frustration in clinical trials. Given the limited therapeutic options available to patients with triple negative breast cancer, new modalities are urgently needed, and promising results from new immunotherapy clinical trials could quickly reshape the treatment of this subtype of breast cancer.
Here, Andrieu, Shafran and Denis show that inhibition of the BET bromodomain protein family can reduce PD-L1 expression in cellular models of triple negative breast cancer. It is also highly innovative and significant that they show these same pathways control PD-1 expression in human primary T cells, which holds out the possibility that multiple relevant cells in the tumor microenvironment could be targeted by these approaches. They are continuing this research, with support from the National Cancer Institute with a new grant, called “BET bromodomain proteins and the immunometabolism of triple negative breast cancer” (R01 CA222170).
Tashia Prince-Lacombe Named APP Chief of Solid Oncology
We are excited to announce the appointment of Tashia Prince-Lacombe, MSN, NP, as the new Chief Advanced Practice Provider for the Solid Oncology team at Boston Medical Center.
Tashia is an Assistant Professor at Boston University Chobanian & Avedisian School of Medicine, dual-certified Nurse Practitioner in Adult-Gerontology and Psychiatric Mental Health, with more than 15 years of nursing experience, including over a decade as an Advanced Practice Provider. Since joining BMC’s Hematology & Oncology Service in 2020, she has played a critical leadership role in enhancing APP operations—improving scheduling, onboarding, mentorship, education and clinical workflows.
A Doctor of Nursing Practice candidate with a focus on leadership and health systems improvement, Tashia is a proven collaborator who has worked closely with physicians, nursing leadership, and operational teams to align staffing models with institutional goals, improve APP engagement, and drive clinical efficiency. Her national recognition includes a 2022 NCODA presentation highlighting her work on advancing APP collaboration in GU oncology.
In addition to her clinical leadership, Tashia is a dedicated educator and mentor, and she supports the development of undergraduate and graduate nursing students through active mentorship and clinical teaching.
Tashia’s early leadership experience in emergency medicine and psychiatry further solidified her strengths in high-acuity care, crisis management, and team development. Her passion for building high-performing, collaborative APP teams has made her a respected and trusted leader committed to delivering patient-centered, high-quality care.
Please join us in congratulating Tashia on this well-deserved appointment and in supporting her as she steps into this important leadership role.