lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in Neurospora crassa

Using an automated cell counting technique developed previously (Case et al., Ecology and Evolution 2014; 4: 3494), we explore the lifespan effects of lac‐1, a ceramide synthase gene paralogous to lag‐1 in Neurospora crassa in conjunction with the band bd (ras‐1) gene. We find that the replicative l...

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Autores principales: Brunson, John K., Griffith, James, Bowles, Daneisha, Case, Mary E., Arnold, Jonathan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2016
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5167027/
https://www.ncbi.nlm.nih.gov/pubmed/28031787
http://dx.doi.org/10.1002/ece3.2554
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author Brunson, John K.
Griffith, James
Bowles, Daneisha
Case, Mary E.
Arnold, Jonathan
author_facet Brunson, John K.
Griffith, James
Bowles, Daneisha
Case, Mary E.
Arnold, Jonathan
author_sort Brunson, John K.
collection PubMed
description Using an automated cell counting technique developed previously (Case et al., Ecology and Evolution 2014; 4: 3494), we explore the lifespan effects of lac‐1, a ceramide synthase gene paralogous to lag‐1 in Neurospora crassa in conjunction with the band bd (ras‐1) gene. We find that the replicative lifespan of a lac‐1 (KO) bd double mutants is short, about one race tube cycle, and this double mutant lacks a strong ~21‐hr clock cycle as shown by race tube and fluorometer analysis of fluorescent strains including lac‐1 (KO). This short replicative lifespan phenotype is contrasted with a very long estimated chronological lifespan for lac‐1 (KO) bd double mutants from 247 to 462 days based on our regression analyses on log viability, and for the single mutant lac‐1 (KO), 161 days. Both of these estimated lifespans are much higher than that of previously studied WT and bd single mutant strains. In a lac‐1 rescue and induction experiment, the expression of lac‐1 (+) as driven by a quinic acid‐dependent promoter actually decreases the median chronological lifespan of cells down to only 7 days, much lower than the 34‐day median lifespan found in control bd conidia also grown on quinic acid media, which we interpret as an effect of balancing selection acting on ceramide levels based on previous findings from the literature. Prior work has shown phytoceramides can act as a signal for apoptosis in stressed N. crassa cells. To test this hypothesis of balancing selection on phytoceramide levels, we examine the viability of WT, lag‐1 (KO) bd, and lac‐1 (KO) bd strains following the dual stresses of heat and glycolysis inhibition, along with phytoceramide treatments of different dosages. We find that the phytoceramide dosage–response curve is altered in the lag‐1 (KO) bd mutant, but not in the lac‐1 (KO) bd mutant. We conclude that phytoceramide production is responsible for the previously reported longevity effects in the lag‐1 (KO) bd mutant, but a different ceramide may be responsible for the longevity effect observed in the lac‐1 (KO) bd mutant.
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spelling pubmed-51670272016-12-28 lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in Neurospora crassa Brunson, John K. Griffith, James Bowles, Daneisha Case, Mary E. Arnold, Jonathan Ecol Evol Original Research Using an automated cell counting technique developed previously (Case et al., Ecology and Evolution 2014; 4: 3494), we explore the lifespan effects of lac‐1, a ceramide synthase gene paralogous to lag‐1 in Neurospora crassa in conjunction with the band bd (ras‐1) gene. We find that the replicative lifespan of a lac‐1 (KO) bd double mutants is short, about one race tube cycle, and this double mutant lacks a strong ~21‐hr clock cycle as shown by race tube and fluorometer analysis of fluorescent strains including lac‐1 (KO). This short replicative lifespan phenotype is contrasted with a very long estimated chronological lifespan for lac‐1 (KO) bd double mutants from 247 to 462 days based on our regression analyses on log viability, and for the single mutant lac‐1 (KO), 161 days. Both of these estimated lifespans are much higher than that of previously studied WT and bd single mutant strains. In a lac‐1 rescue and induction experiment, the expression of lac‐1 (+) as driven by a quinic acid‐dependent promoter actually decreases the median chronological lifespan of cells down to only 7 days, much lower than the 34‐day median lifespan found in control bd conidia also grown on quinic acid media, which we interpret as an effect of balancing selection acting on ceramide levels based on previous findings from the literature. Prior work has shown phytoceramides can act as a signal for apoptosis in stressed N. crassa cells. To test this hypothesis of balancing selection on phytoceramide levels, we examine the viability of WT, lag‐1 (KO) bd, and lac‐1 (KO) bd strains following the dual stresses of heat and glycolysis inhibition, along with phytoceramide treatments of different dosages. We find that the phytoceramide dosage–response curve is altered in the lag‐1 (KO) bd mutant, but not in the lac‐1 (KO) bd mutant. We conclude that phytoceramide production is responsible for the previously reported longevity effects in the lag‐1 (KO) bd mutant, but a different ceramide may be responsible for the longevity effect observed in the lac‐1 (KO) bd mutant. John Wiley and Sons Inc. 2016-10-24 /pmc/articles/PMC5167027/ /pubmed/28031787 http://dx.doi.org/10.1002/ece3.2554 Text en © 2016 The Authors. Ecology and Evolution published by John Wiley & Sons Ltd. This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Research
Brunson, John K.
Griffith, James
Bowles, Daneisha
Case, Mary E.
Arnold, Jonathan
lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in Neurospora crassa
title lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in Neurospora crassa
title_full lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in Neurospora crassa
title_fullStr lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in Neurospora crassa
title_full_unstemmed lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in Neurospora crassa
title_short lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in Neurospora crassa
title_sort lac‐1 and lag‐1 with ras‐1 affect aging and the biological clock in neurospora crassa
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5167027/
https://www.ncbi.nlm.nih.gov/pubmed/28031787
http://dx.doi.org/10.1002/ece3.2554
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