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Generation of an efficiently secreted, cell penetrating NF-?B inhibitor

journal contribution
posted on 2023-06-09, 15:55 authored by Apostolos Koutsokeras, Nirupam Purkayastha, Anne Rigby, Maria C Subang, Michelle Sclanders, Sandrine Vessillier, Lisa MullenLisa Mullen, Yuti Chernajovsky, David Gould
Gene therapy is a powerful approach to treat disease locally. However, if the therapeutic target is intracellular, the therapeutic will be effective only in the cells where the therapeutic gene is delivered. We have engineered a fusion protein containing an intracellular inhibitor of the transcription factor NF-?B pathway that can be effectively secreted from producing cells. This fusion protein is cleaved extracellularly by metalloproteinases allowing release of a protein transduction domain (PTD) linked to the NF-?B inhibitor for translocation into neighboring cells. We show that engineered molecules can be efficiently secreted (>80%); are cleaved with matrix metalloprotease-1; inhibit NF-?B driven transcription in a biological assay with a human reporter cell line; and display significant inhibition in mouse paw inflammation models when delivered by lentivirus or secreting cells. No inhibition of NF-?B transcription or therapeutic effect was seen using molecules devoid of the PTD and NF-?B inhibitory domains. By creating a fusion protein with an endogenous secretion partner, we demonstrate a novel approach to efficiently secrete PTD-containing protein domains, overcoming previous limitations, and allowing for potent paracrine effects.

History

Publication status

  • Published

File Version

  • Published version

Journal

FASEB Journal

ISSN

0892-6638

Publisher

Federation of American Society of Experimental Biology

Issue

1

Volume

28

Page range

373-381

Department affiliated with

  • Clinical and Experimental Medicine Publications

Full text available

  • No

Peer reviewed?

  • Yes

Legacy Posted Date

2018-11-16

First Compliant Deposit (FCD) Date

2018-11-16

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