Chemical chaperones protect epidermolysis bullosa simplex keratinocytes from heat stress-induced keratin aggregation: involvement of heat shock proteins and MAP kinases.

[epidermolysis bullosa simplex]

Epidermolysis bullosa simplex (EBS ) is a blistering skin disease caused by mutations in keratin genes (KRT 5 or KRT 14 ), with no existing therapies . Aggregates of misfolded mutant keratins are seen in cultured keratinocytes from severe EBS patients . In other protein-folding disorders , involvement of molecular chaperones and the ubiquitin-proteasome system may modify disease severity . In this study , the effects of heat stress on keratin aggregation in immortalized cells from two patients with EBS (KRT 5 ) and a healthy control were examined with and without addition of various test compounds . Heat-induced (43 â€‰Â°C , 30 â€‰minutes ) aggregates were observed in all cell lines , the amount of which correlated with the donor phenotype . In EBS cells pre-exposed to proteasome inhibitor , MG 132 , and p 38 -mitogen-activated protein kinase (MAPK ) inhibitor , SB 203580 , the proportion of aggregate-positive cells increased , suggesting a role of proteasomes and phosphorylation in removing mutated keratin . In contrast , aggregates were reduced by pretreatment with two chemical chaperones , trimethylamine N-oxide (TMAO ) and 4 -phenylbutyrate (4 -PBA ). TMAO also modulated stress-induced p 38 /c-jun N-terminal kinase (JNK ) activation and expression of heat shock protein (HSPA 1 A ), the latter of which colocalized with phosphorylated keratin 5 in EBS cells . Taken together , our findings suggest therapeutic targets for EBS and other keratinopathies .

Diseases
Validation

Diseases presenting "misfolded mutant keratins" symptom

epidermolysis bullosa simplex

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