Adult-restricted gene knock-down reveals candidates that affect locomotive healthspan in C. elegans

被引:0
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作者
Areta Jushaj
Matthew Churgin
Miguel De La Torre
Amanda Kieswetter
Brecht Driesschaert
Ineke Dhondt
Bart P. Braeckman
Christopher Fang-Yen
Liesbet Temmerman
机构
[1] KU Leuven,Animal Physiology and Neurobiology, Department of Biology
[2] University of Pennsylvania,Department of Bioengineering
[3] Ghent University,Laboratory of Aging Physiology and Molecular Evolution, Department of Biology
来源
Biogerontology | 2023年 / 24卷
关键词
Aging; Healthspan; F26A3.4; Locomotion; WorMotel;
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中图分类号
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摘要
Understanding how we can age healthily is a challenge at the heart of biogerontological interest. Whereas myriad genes are known to affect the lifespan of model organisms, effects of such interventions on healthspan—the period of life where an animal is considered healthy, rather than merely alive—are less clear. To understand relationships between life- and healthspan, in recent years several platforms were developed with the purpose of assessing both readouts simultaneously. We here relied on one such platform, the WorMotel, to study effects of adulthood-restricted knock-down of 130 Caenorhabditis elegans genes on the locomotive health of the animals along their lifespans. We found that knock-down of six genes affected healthspan while lifespan remained unchanged. For two of these, F26A3.4 and chn-1, knock-down resulted in an improvement of healthspan. In follow-up experiments we showed that knockdown of F26A3.4 indeed improves locomotive health and muscle structure at old age.
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页码:225 / 233
页数:8
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