Systemic delivery of factor IX messenger RNA for protein replacement therapy

Author:

Ramaswamy Suvasini,Tonnu Nina,Tachikawa Kiyoshi,Limphong Pattraranee,Vega Jerel B.,Karmali Priya P.,Chivukula Pad,Verma Inder M.

Abstract

Safe and efficient delivery of messenger RNAs for protein replacement therapies offers great promise but remains challenging. In this report, we demonstrate systemic, in vivo, nonviral mRNA delivery through lipid nanoparticles (LNPs) to treat a Factor IX (FIX)-deficient mouse model of hemophilia B. Delivery of human FIX (hFIX) mRNA encapsulated in our LUNAR LNPs results in a rapid pulse of FIX protein (within 4–6 h) that remains stable for up to 4–6 d and is therapeutically effective, like the recombinant human factor IX protein (rhFIX) that is the current standard of care. Extensive cytokine and liver enzyme profiling showed that repeated administration of the mRNA–LUNAR complex does not cause any adverse innate or adaptive immune responses in immune-competent, hemophilic mice. The levels of hFIX protein that were produced also remained consistent during repeated administrations. These results suggest that delivery of long mRNAs is a viable therapeutic alternative for many clotting disorders and for other hepatic diseases where recombinant proteins may be unaffordable or unsuitable.

Funder

HHS | NIH | National Cancer Institute

Leona M. and Harry B. Helmsley Charitable Trust

California Institute for Regenerative Medicine

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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