News Release

SP-101 is a novel AAV gene therapy for cystic fibrosis

Peer-Reviewed Publication

Mary Ann Liebert, Inc./Genetic Engineering News

Human Gene Therapy

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The first peer-reviewed journal in the field of human gene therapy, providing all-inclusive coverage of the research, methods, and clinical developments that are driving today's explosion of gene therapy advances.

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Credit: Mary Ann Liebert, Inc.

Scientists from Spirovant Sciences describe SP-101, a novel adeno-associated virus (AAV) gene therapy for the treatment of cystic fibrosis (CF) in the peer-reviewed journal Human Gene Therapy. They also showed that after single dose inhaled delivery of SP-101, SP-101 vector genomes were detected throughout the respiratory tract of CF ferrets. Click here to read the articles now.

Cystic fibrosis is a genetic disease caused by mutations in the cystic fibrosis transmembrane conductance regulator (CFTR) gene. Katherine Excoffon, and coauthors from Spirovant Sciences, describe SP-101, an AAV gene therapy vector that has been optimized for efficient human airway cell transduction, and that contains a functional and regulated shortened human CFTR minigene (hCFTRΔR).

The investigators showed that hCFTRΔR mRNA expression was highest in ferrets that also received single does inhaled doxorubicin, an AAV transduction augmenter.

“SP-101 mediated hCFTRΔR mRNA expression was clearly apparent in all SP-101 dose groups 2-weeks and 13-weeks post-dose,” stated the investigators.

In in vitro studies, “functional correction of CF human airway epithelia increased with increasing multiplicity of infection and doxorubicin concentration and correlated with increasing cell-associated vector genomes and hCFTRΔR mRNA expression.”

“A number of efforts to use AAV for CF gene therapy have fallen short on efficiency and duration of gene transfer ,” says Editor in Chief Terence R. Flotte, MD, Celia and Isaac Haidak Professor of Medical Education and Dean, Provost, and Executive Deputy Chancellor, University of Massachusetts Medical School. “The vector described by Excoffon and colleagues combines a number of improvements in an attempt to overcome these obstacles and fulfill the unmet needs of CF patients for whom effective CFTR modulators are not available.”

About the Journal
Human Gene Therapy, 
the Official Journal of the European Society of Gene and Cell Therapy and eight other international gene therapy societies, was the first peer-reviewed journal in the field and provides all-inclusive access to the critical pillars of human gene therapy: research, methods, and clinical applications. The Journal is led by Editor-in-Chief Terence R. Flotte, MD, Celia and Isaac Haidak Professor of Medical Education and Dean, Provost, and Executive Deputy Chancellor, University of Massachusetts Medical School, and an esteemed international editorial board. Human Gene Therapy is available in print and online. Complete tables of contents and a sample issue are available on the Human Gene Therapy website.

About the Publisher
Mary Ann Liebert, Inc. is a global media company dedicated to creating, curating, and delivering impactful peer-reviewed research and authoritative content services to advance the fields of biotechnology and the life sciences, specialized clinical medicine, and public health and policy. For complete information, please visit the Mary Ann Liebert, Inc. website.


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