Margaret Donnelly
mwdonnelly.bsky.social
Margaret Donnelly
@mwdonnelly.bsky.social
Retried technology marketer and entrepreneur. Dachshund lover. Artist and jewelry maker. Living with MTNBC since 2021.
Reposted by Margaret Donnelly
Anthony S. Fauci, whose high-profile role in helping lead the nation’s coronavirus response made him the target of threats, has been stripped of his government security protection.

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wapo.st
January 24, 2025 at 8:00 PM
Reposted by Margaret Donnelly
Neoantigen DNA vaccines are safe, feasible, and induce neoantigen-specific immune responses in triple-negative breast cancer patients

A clinical trial to prevent recurrence of tumors promising results for patients with triple-negative breast cancer.

genomemedicine.biome...
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Neoantigen DNA vaccines are safe, feasible, and induce neoantigen-specific immune responses in triple-negative breast cancer patients - Genome Medicine
Background Neoantigen vaccines can induce or enhance highly specific antitumor immune responses with minimal risk of autoimmunity. We have developed a neoantigen DNA vaccine platform capable of efficiently presenting both HLA class I and II epitopes and performed a phase 1 clinical trial in triple-negative breast cancer patients with persistent disease on surgical pathology following neoadjuvant chemotherapy, a patient population at high risk of disease recurrence. Methods Expressed somatic mutations were identified by tumor/normal exome sequencing and tumor RNA sequencing. The pVACtools software suite of neoantigen prediction algorithms was used to identify and prioritize cancer neoantigens and facilitate vaccine design for manufacture in an academic GMP facility. Neoantigen DNA vaccines were administered via electroporation in the adjuvant setting (i.e., following surgical removal of the primary tumor and completion of standard of care therapy). Vaccines were monitored for safety and immune responses via ELISpot, intracellular cytokine production via flow cytometry, and TCR sequencing. Results Eighteen subjects received three doses of a neoantigen DNA vaccine encoding on average 11 neoantigens per patient (range 4–20). The vaccinations were well tolerated with relatively few adverse events. Neoantigen-specific T cell responses were induced in 14/18 patients as measured by ELISpot and flow cytometry. At a median follow-up of 36 months, recurrence-free survival was 87.5% (95% CI: 72.7–100%) in the cohort of vaccinated patients. Conclusion Our study demonstrates neoantigen DNA vaccines are safe, feasible, and capable of inducing neoantigen-specific immune responses. Clinical trial registration number NCT02348320.
genomemedicine.biomedcentral.com
November 28, 2024 at 11:11 AM
Kicking the tires at BlueSky. I quit using Twitter/X some time ago. Not sure how bsky will fit with my social media consumption. Still like Facebook for close connections, but dislike it due to the heavy advertising. Hoping to find good content here.
December 1, 2024 at 8:10 PM