AI Article Synopsis

  • Maintaining healthy nerve connections in fat tissue is essential for metabolic well-being, as obesity, diabetes, and aging can lead to peripheral neuropathy, which hinders nerve regeneration.
  • Researchers tested an adeno-associated virus (AAV) gene therapy to deliver neurotrophic factors like BDNF and NGF directly to fat tissue, showing promise in improving nerve innervation in obese and diabetic mice.
  • NGF was found to be more effective than BDNF for enhancing nerve connections, particularly after prolonged dietary obesity, suggesting that a combination of therapies might provide the best results for treating peripheral neuropathy.

Article Abstract

Maintaining functional adipose innervation is critical for metabolic health. We found that subcutaneous white adipose tissue (scWAT) undergoes peripheral neuropathy (PN) with obesity, diabetes, and aging (reduced small-fiber innervation and nerve/synaptic/growth-cone/vesicle markers, altered nerve activity). Unlike with nerve injuries, peripheral nerves do not regenerate with PN, and therefore new therapies are needed for treatment of this condition affecting 20-30 million Americans. Here, we validated a gene therapy approach using an adipocyte-tropic adeno-associated virus (AAV; serotype Rec2) to deliver neurotrophic factors (brain-derived neurotrophic factor [BDNF] and nerve growth factor [NGF]) directly to scWAT to improve tissue-specific PN as a proof-of-concept approach. AAVRec2-BDNF intra-adipose delivery improved tissue innervation in obese/diabetic mice with PN, but after longer periods of dietary obesity there was reduced efficacy, revealing a key time window for therapies. AAVRec2-NGF also increased scWAT innervation in obese mice and was more effective than BDNF, likely because Rec2 targeted adipocytes, the tissue's endogenous NGF source. AAVRec2-NGF also worked well even after 25 weeks of dietary obesity, unlike BDNF, which likely needs a vector that targets its physiological cellular source (stromal vascular fraction cells). Given the differing effects of AAVs carrying NGF versus BDNF, a combined therapy may be ideal for PN.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11081869PMC
http://dx.doi.org/10.1016/j.ymthe.2024.02.035DOI Listing

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