@article{af1338e444a84c5399853b2534538420,
title = "Microtubule regulators act in the nervous system to modulate fat metabolism and longevity through DAF-16 in C. elegans",
abstract = "Microtubule (MT) regulation is involved in both neuronal function and the maintenance of neuronal structure, and MT dysregulation appears to be a general downstream indicator and effector of age-related neurodegeneration. But the role of MTs in natural aging is largely unknown. Here, we demonstrate a role of MT regulators in regulating longevity. We find that loss of EFA-6, a modulator of MT dynamics, can delay both neuronal aging and extend the lifespan of C. elegans. Through the use of genetic mutants affecting other MT-regulating genes in C. elegans, we find that loss of MT stabilizing genes (including ptrn-1 and ptl-1) shortens lifespan, while loss of MT destabilizing gene hdac-6 extends lifespan. Via the use of tissue-specific transgenes, we further show that these MT regulators can act in the nervous system to modulate lifespan. Through RNA-seq analyses, we found that genes involved in lipid metabolism were differentially expressed in MT regulator mutants, and via the use of Nile Red and Oil Red O staining, we show that the MT regulator mutants have altered fat storage. We further find that the increased fat storage and extended lifespan of the long-lived MT regulator mutants are dependent on the DAF-16/FOXO transcription factor. Our results suggest that neuronal MT status might affect organismal aging through DAF-16-regulated changes in fat metabolism, and therefore, MT-based therapies might represent a novel intervention to promote healthy aging.",
keywords = "daf-16, efa-6, fat metabolism, longevity, microtubules, neuronal aging",
author = "Aiping Xu and Zhao Zhang and Ko, {Su Hyuk} and Fisher, {Alfred L.} and Zhijie Liu and Lizhen Chen",
note = "Funding Information: We thank Dr. Hongning Wang for assistance in the thrashing assay, Dr. Pamela Larsen and Dr. Karl Rodriguez for discussion of our work and for providing RNAi clones. This work was supported by funds from the San Antonio Nathan Shock Center (NIA grant 3P30 AG013319-23S2) to LC, CPRIT RR160017 to ZL, V Foundation V2016-017 to ZL, Voelcker Fund Young Investigator award to ZL, Susan G. Komen CCR award CCR17483391 to ZL, NCI 1U54CA217297-01/PRJ001 to ZL, funds from the South Texas VA Healthcare System to ALF, NIA grant AG044768 to ALF, NIEHS grant ES017761 to ALF, and NINDS NS102782 to ALF, NIA grant AG013319 to ALF. RNA-seq data were generated in the Genome Sequencing Facility which is supported by NIH-NCI P30 CA054174 (Cancer Center at UT Health San Antonio), NIH Shared Instrument grant 1S10OD021805-01 (S10 grant), and CPRIT Core Facility Award (RP160732). Funding Information: and for providing RNAi clones. This work was supported by funds from the San Antonio Nathan Shock Center (NIA grant 3P30 AG013319‐23S2) to LC, CPRIT RR160017 to ZL, V Foundation V2016‐017 to ZL, Voelcker Fund Young Investigator award to ZL, Susan G. Komen CCR award CCR17483391 to ZL, NCI 1U54CA217297‐01/PRJ001 to ZL, funds from the South Texas VA Healthcare System to ALF, NIA grant AG044768 to ALF, NIEHS grant ES017761 to ALF, and NINDS NS102782 to ALF, NIA grant AG013319 to ALF. RNA‐seq data were generated in the Genome Sequencing Facility which is supported by NIH‐NCI P30 CA054174 (Cancer Center at UT Health San Antonio), NIH Shared Instrument grant 1S10OD021805‐01 (S10 grant), and CPRIT Core Facility Award (RP160732). Publisher Copyright: {\textcopyright} 2019 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.",
year = "2019",
month = apr,
doi = "10.1111/acel.12884",
language = "English (US)",
volume = "18",
journal = "Aging Cell",
issn = "1474-9718",
publisher = "Wiley-Blackwell",
number = "2",
}