Identification of disease-related aberrantly spliced transcripts in myeloma and strategies to target these alterations by RNA-based therapeutics

Author:

Ogiya Daisuke,Chyra Zuzana,Verselis Sigitas J.,O’Keefe Morgan,Cobb Jacquelyn,Abiatari Ivane,Talluri Srikanth,Sithara Anjana Anilkumar,Hideshima Teru,Chu Michael P.,Hájek RomanORCID,Dorfman David M.,Pilarski Linda M.,Anderson Kenneth C.ORCID,Adamia SophiaORCID

Abstract

AbstractNovel drug discoveries have shifted the treatment paradigms of most hematological malignancies, including multiple myeloma (MM). However, this plasma cell malignancy remains incurable, and novel therapies are therefore urgently needed. Whole-genome transcriptome analyses in a large cohort of MM patients demonstrated that alterations in pre-mRNA splicing (AS) are frequent in MM. This manuscript describes approaches to identify disease-specific alterations in MM and proposes RNA-based therapeutic strategies to eradicate such alterations. As a “proof of concept”, we examined the causes of aberrant HMMR (Hyaluronan-mediated motility receptor) splicing in MM. We identified clusters of single nucleotide variations (SNVs) in the HMMR transcript where the altered splicing took place. Using bioinformatics tools, we predicted SNVs and splicing factors that potentially contribute to aberrant HMMR splicing. Based on bioinformatic analyses and validation studies, we provided the rationale for RNA-based therapeutic strategies to selectively inhibit altered HMMR splicing in MM. Since splicing is a hallmark of many cancers, strategies described herein for target identification and the design of RNA-based therapeutics that inhibit gene splicing can be applied not only to other genes in MM but also more broadly to other hematological malignancies and solid tumors as well.

Funder

The Paula and Rodger Riney Foundation (K.Anderson) The Adelson Medical Research Foundation

Publisher

Springer Science and Business Media LLC

Subject

Oncology,Hematology

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