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Crotamiton derivative JM03 extends lifespan and improves oxidative and hypertonic stress resistance in Caenorhabditis elegans via inhibiting OSM-9.

Keting BaoWenwen LiuZhouzhi SongJiali FengZhifan MaoLingyuan BaoTianyue SunZelan HuJian Li
Published in: eLife (2022)
While screening our in-house 1072 marketed drugs for their ability to extend the lifespan using Caenorhabditis elegans ( C. elegans ) as an animal model, crotamiton ( N -ethyl-o-crotonotoluidide) showed anti-aging activity and was selected for further structural optimization. After replacing the ortho-methyl of crotamiton with ortho-fluoro, crotamiton derivative JM03 was obtained and showed better activity in terms of lifespan-extension and stress resistance than crotamiton. It was further explored that JM03 extended the lifespan of C. elegans through osmotic avoidance abnormal-9 (OSM-9). Besides, JM03 improves the ability of nematode to resist oxidative stress and hypertonic stress through OSM-9, but not osm-9/capsaicin receptor related-2 (OCR-2). Then the inhibition of OSM-9 by JM03 reduces the aggregation of Q35 in C. elegans via upregulating the genes associated with proteostasis. SKN-1 signaling was also found to be activated after JM03 treatment, which might contribute to proteostasis, stress resistance and lifespan extension. In summary, this study explored a new small molecule derived from crotamiton, which has efficient anti-oxidative, anti-hypertonic, and anti-aging effects, and could further lead to promising application prospects.
Keyphrases
  • small molecule
  • oxidative stress
  • stress induced
  • computed tomography
  • dna damage
  • heat stress
  • drug induced
  • endoplasmic reticulum stress
  • combination therapy
  • induced apoptosis
  • water soluble
  • heat shock protein