Impaired DNAJB2 Response to Heat Shock in Fibroblasts from a Neuropathy Patient with DNAJB2/HSJ1 Mutation: Cystamine as a Potential Therapeutic Intervention
Raj Kumar Pradhan, Nikolas G. Kinney, Brigid K. Jensen, Hristelina Ilieva

TL;DR
A DNAJB2 mutation in a neuropathy patient impairs the protein's response to heat stress, and cystamine may help restore its function.
Contribution
This is the first study to investigate the heterozygous DNAJB2 c.823+6C>T mutation in neuropathy and test cystamine as a potential treatment.
Findings
The DNAJB2 mutation leads to reduced baseline levels and impaired upregulation in response to heat shock.
Cystamine treatment increased DNAJB2 levels in both control and patient fibroblasts.
The mutation may contribute to the pathogenesis of sensory–motor polyneuropathy.
Abstract
Background and Objectives: Neuropathy is a debilitating disorder characterized by peripheral nerve dysfunction and damage to sensory, motor, and autonomic neurons and their axons. While homozygous mutations in DNAJB2/HSJ1 have been linked to early-onset neuropathy, a heterozygous DNAJB2 c.823+6C>T was discovered in an adult patient with severe sensory–motor polyneuropathy. This mutation is predicted to affect both isoforms of the protein. DNAJB2 (HSP40), a key member of the heat shock protein family, plays a critical role in cellular protection and stress, including response to heat shock. DNAJB2 traffics unfolded proteins to another heat shock protein, HSP70, and activates its ATPase activity to result in a correctly folded protein(s). In this study, we aimed to investigate the effects of the heterozygous DNAJB2 c.823+6C>T mutation on the stress response of DNAJB2 in fibroblasts…
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Taxonomy
TopicsHeat shock proteins research · Genetic Neurodegenerative Diseases · Exercise and Physiological Responses
