Akila S Venkataramany scite author profile

T cells redirected to cancer cells either via a chimeric antigen receptor (CAR-T) or a bispecific molecule have been breakthrough technologies; however, CAR-T cells require individualized manufacturing and bispecifics generally require continuous infusions. We created an off-the-shelf, single-dose solution for achieving prolonged systemic serum levels of protein immunotherapeutics via adeno-associated virus (AAV) gene transfer. We demonstrate proof of principle in a CD19 + lymphoma xenograft model using a single intravenous dose of AAV expressing a secreted version of blinatumomab, which could serve as a universal alternative for CD19 CAR-T cell therapy. In addition, we created an inducible version using an exon skipping strategy and achieved repeated, on-demand expression up to at least 36 weeks after AAV injection. Our system could be considered for short-term and/or repeated expression of other transgenes of interest for noncancer applications.

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Heat increases full-length SMN splicing: promise for splice-augmenting therapies for SMA

Dominguez

Cunningham

Venkataramany

et al. 2022

Hum Genet

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Akila S Venkataramany

Alternative RNA splicing defects in pediatric cancers: new insights in tumorigenesis and potential therapeutic vulnerabilities

Leveraging gene therapy to achieve long-term continuous or controllable expression of biotherapeutics

Heat increases full-length SMN splicing: promise for splice-augmenting therapies for SMA

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