Your search keyword '"Ma, Dengke K."' showing total 24 results

1. GPCR signaling regulates severe stress-induced organismic death in Caenorhabditis elegans.

Author

Wang, Changnan, Wang, Changnan, Long, Yong, Wang, Bingying, Zhang, Chao, Ma, Dengke K, Wang, Changnan, Wang, Changnan, Long, Yong, Wang, Bingying, Zhang, Chao, and Ma, Dengke K

Abstract

How an organism dies is a fundamental yet poorly understood question in biology. An organism can die of many causes, including stress-induced phenoptosis, also defined as organismic death that is regulated by its genome-encoded programs. The mechanism of stress-induced phenoptosis is still largely unknown. Here, we show that transient but severe freezing-thaw stress (FTS) in Caenorhabditis elegans induces rapid and robust phenoptosis that is regulated by G-protein coupled receptor (GPCR) signaling. RNAi screens identify the GPCR-encoding fshr-1 in mediating transcriptional responses to FTS. FSHR-1 increases ligand interaction upon FTS and activates a cyclic AMP-PKA cascade leading to a genetic program to promote organismic death under severe stress. FSHR-1/GPCR signaling up-regulates the bZIP-type transcription factor ZIP-10, linking FTS to expression of genes involved in lipid remodeling, proteostasis, and aging. A mathematical model suggests how genes may promote organismic death under severe stress conditions, potentially benefiting growth of the clonal population with individuals less stressed and more reproductively privileged. Our studies reveal the roles of FSHR-1/GPCR-mediated signaling in stress-induced gene expression and phenoptosis in C. elegans, providing empirical new insights into mechanisms of stress-induced phenoptosis with evolutionary implications.

Published

2023

2. Nucleolus localization of SpyCas9 affects its stability and interferes with host protein translation in mammalian cells.

Author

Tan, Renke, Tan, Renke, Du, Wenhao, Liu, Yiyang, Cong, Xiaoji, Bai, Meirong, Jiang, Chenxiao, Li, Zengxia, Tan, Minjia, Ma, Dengke K, Huang, Qiang, Jiang, Wei, Dang, Yongjun, Tan, Renke, Tan, Renke, Du, Wenhao, Liu, Yiyang, Cong, Xiaoji, Bai, Meirong, Jiang, Chenxiao, Li, Zengxia, Tan, Minjia, Ma, Dengke K, Huang, Qiang, Jiang, Wei, and Dang, Yongjun

Abstract

The CRISPR/Cas9 system, originally derived from the prokaryotic adaptive immune system, has been developed as efficient genome editing tools. It enables precise gene manipulation on chromosomal DNA through the specific binding of programmable sgRNA to target DNA, and the Cas9 protein, which has endonuclease activity, will cut a double strand break at specific locus. However, Cas9 is a foreign protein in mammalian cells, and the potential risks associated with its introduction into mammalian cells are not fully understood. In this study, we performed pull-down and mass spectrometry (MS) analysis of Streptococcus pyogenes Cas9 (SpyCas9) interacting proteins in HEK293T cells and showed that the majority of Cas9-associated proteins identified by MS were localized in the nucleolus. Interestingly, we further discovered that the Cas9 protein contains a sequence encoding a nucleolus detention signal (NoDS). Compared with wild-type (WT) Cas9, NoDS-mutated variants of Cas9 (mCas9) are less stable, although their gene editing activity is minimally affected. Overexpression of WT Cas9, but not mCas9, causes general effects on transcription and protein translation in the host cell. Overall, identification of NoDS in Cas9 will improve the understanding of Cas9's biological function in vivo, and the removal of NoDS in Cas9 may enhance its safety for future clinical use.

Published

2022

3. Nucleolus localization of SpyCas9 affects its stability and interferes with host protein translation in mammalian cells.

Author

Tan, Renke, Tan, Renke, Du, Wenhao, Liu, Yiyang, Cong, Xiaoji, Bai, Meirong, Jiang, Chenxiao, Li, Zengxia, Tan, Minjia, Ma, Dengke K, Huang, Qiang, Jiang, Wei, Dang, Yongjun, Tan, Renke, Tan, Renke, Du, Wenhao, Liu, Yiyang, Cong, Xiaoji, Bai, Meirong, Jiang, Chenxiao, Li, Zengxia, Tan, Minjia, Ma, Dengke K, Huang, Qiang, Jiang, Wei, and Dang, Yongjun

Abstract

The CRISPR/Cas9 system, originally derived from the prokaryotic adaptive immune system, has been developed as efficient genome editing tools. It enables precise gene manipulation on chromosomal DNA through the specific binding of programmable sgRNA to target DNA, and the Cas9 protein, which has endonuclease activity, will cut a double strand break at specific locus. However, Cas9 is a foreign protein in mammalian cells, and the potential risks associated with its introduction into mammalian cells are not fully understood. In this study, we performed pull-down and mass spectrometry (MS) analysis of Streptococcus pyogenes Cas9 (SpyCas9) interacting proteins in HEK293T cells and showed that the majority of Cas9-associated proteins identified by MS were localized in the nucleolus. Interestingly, we further discovered that the Cas9 protein contains a sequence encoding a nucleolus detention signal (NoDS). Compared with wild-type (WT) Cas9, NoDS-mutated variants of Cas9 (mCas9) are less stable, although their gene editing activity is minimally affected. Overexpression of WT Cas9, but not mCas9, causes general effects on transcription and protein translation in the host cell. Overall, identification of NoDS in Cas9 will improve the understanding of Cas9's biological function in vivo, and the removal of NoDS in Cas9 may enhance its safety for future clinical use.

Published

2022

4. A conserved megaprotein-based molecular bridge critical for lipid trafficking and cold resilience.

Author

Wang, Changnan, Wang, Changnan, Wang, Bingying, Pandey, Taruna, Long, Yong, Zhang, Jianxiu, Oh, Fiona, Sima, Jessica, Guo, Ruyin, Liu, Yun, Zhang, Chao, Mukherjee, Shaeri, Bassik, Michael, Lin, Weichun, Deng, Huichao, Vale, Goncalo, McDonald, Jeffrey G, Shen, Kang, Ma, Dengke K, Wang, Changnan, Wang, Changnan, Wang, Bingying, Pandey, Taruna, Long, Yong, Zhang, Jianxiu, Oh, Fiona, Sima, Jessica, Guo, Ruyin, Liu, Yun, Zhang, Chao, Mukherjee, Shaeri, Bassik, Michael, Lin, Weichun, Deng, Huichao, Vale, Goncalo, McDonald, Jeffrey G, Shen, Kang, and Ma, Dengke K

Abstract

Cells adapt to cold by increasing levels of unsaturated phospholipids and membrane fluidity through conserved homeostatic mechanisms. Here we report an exceptionally large and evolutionarily conserved protein LPD-3 in C. elegans that mediates lipid trafficking to confer cold resilience. We identify lpd-3 mutants in a mutagenesis screen for genetic suppressors of the lipid desaturase FAT-7. LPD-3 bridges the endoplasmic reticulum (ER) and plasma membranes (PM), forming a structurally predicted hydrophobic tunnel for lipid trafficking. lpd-3 mutants exhibit abnormal phospholipid distribution, diminished FAT-7 abundance, organismic vulnerability to cold, and are rescued by Lecithin comprising unsaturated phospholipids. Deficient lpd-3 homologues in Zebrafish and mammalian cells cause defects similar to those observed in C. elegans. As mutations in BLTP1, the human orthologue of lpd-3, cause Alkuraya-Kucinskas syndrome, LPD-3 family proteins may serve as evolutionarily conserved highway bridges critical for ER-associated non-vesicular lipid trafficking and resilience to cold stress in eukaryotic cells.

Published

2022

5. The conserved transmembrane protein TMEM-39 coordinates with COPII to promote collagen secretion and regulate ER stress response.

Author

Zhang, Zhe, Zhang, Zhe, Luo, Shuo, Barbosa, Guilherme Oliveira, Bai, Meirong, Kornberg, Thomas B, Ma, Dengke K, Zhang, Zhe, Zhang, Zhe, Luo, Shuo, Barbosa, Guilherme Oliveira, Bai, Meirong, Kornberg, Thomas B, and Ma, Dengke K

Abstract

Dysregulation of collagen production and secretion contributes to aging and tissue fibrosis of major organs. How procollagen proteins in the endoplasmic reticulum (ER) route as specialized cargos for secretion remains to be fully elucidated. Here, we report that TMEM39, an ER-localized transmembrane protein, regulates production and secretory cargo trafficking of procollagen. We identify the C. elegans ortholog TMEM-39 from an unbiased RNAi screen and show that deficiency of tmem-39 leads to striking defects in cuticle collagen production and constitutively high ER stress response. RNAi knockdown of the tmem-39 ortholog in Drosophila causes similar defects in collagen secretion from fat body cells. The cytosolic domain of human TMEM39A binds to Sec23A, a vesicle coat protein that drives collagen secretion and vesicular trafficking. TMEM-39 regulation of collagen secretion is independent of ER stress response and autophagy. We propose that the roles of TMEM-39 in collagen secretion and ER homeostasis are likely evolutionarily conserved.

Published

2021

6. The C. elegans homolog of human panic-disorder risk gene TMEM132D orchestrates neuronal morphogenesis through the WAVE-regulatory complex.

Author

Wang, Xin, Wang, Xin, Jiang, Wei, Luo, Shuo, Yang, Xiaoyu, Wang, Changnan, Wang, Bingying, Dang, Yongjun, Shen, Yin, Ma, Dengke K, Wang, Xin, Wang, Xin, Jiang, Wei, Luo, Shuo, Yang, Xiaoyu, Wang, Changnan, Wang, Bingying, Dang, Yongjun, Shen, Yin, and Ma, Dengke K

Abstract

TMEM132D is a human gene identified with multiple risk alleles for panic disorders, anxiety and major depressive disorders. Defining a conserved family of transmembrane proteins, TMEM132D and its homologs are still of unknown molecular functions. By generating loss-of-function mutants of the sole TMEM132 ortholog in C. elegans, we identify abnormal morphologic phenotypes in the dopaminergic PDE neurons. Using a yeast two-hybrid screen, we find that NAP1 directly interacts with the cytoplasmic domain of human TMEM132D, and mutations in C. elegans tmem-132 that disrupt interaction with NAP1 cause similar morphologic defects in the PDE neurons. NAP1 is a component of the WAVE regulatory complex (WRC) that controls F-actin cytoskeletal dynamics. Decreasing activity of WRC rescues the PDE defects in tmem-132 mutants, whereas gain-of-function of TMEM132D in mammalian cells inhibits WRC, leading to decreased abundance of select WRC components, impaired actin nucleation and cell motility. We propose that metazoan TMEM132 family proteins play evolutionarily conserved roles in regulating NAP1 protein homologs to restrict inappropriate WRC activity, cytoskeletal and morphologic changes in the cell.

Published

2021

7. The C. elegans homolog of human panic-disorder risk gene TMEM132D orchestrates neuronal morphogenesis through the WAVE-regulatory complex.

Author

Wang, Xin, Wang, Xin, Jiang, Wei, Luo, Shuo, Yang, Xiaoyu, Wang, Changnan, Wang, Bingying, Dang, Yongjun, Shen, Yin, Ma, Dengke K, Wang, Xin, Wang, Xin, Jiang, Wei, Luo, Shuo, Yang, Xiaoyu, Wang, Changnan, Wang, Bingying, Dang, Yongjun, Shen, Yin, and Ma, Dengke K

Abstract

TMEM132D is a human gene identified with multiple risk alleles for panic disorders, anxiety and major depressive disorders. Defining a conserved family of transmembrane proteins, TMEM132D and its homologs are still of unknown molecular functions. By generating loss-of-function mutants of the sole TMEM132 ortholog in C. elegans, we identify abnormal morphologic phenotypes in the dopaminergic PDE neurons. Using a yeast two-hybrid screen, we find that NAP1 directly interacts with the cytoplasmic domain of human TMEM132D, and mutations in C. elegans tmem-132 that disrupt interaction with NAP1 cause similar morphologic defects in the PDE neurons. NAP1 is a component of the WAVE regulatory complex (WRC) that controls F-actin cytoskeletal dynamics. Decreasing activity of WRC rescues the PDE defects in tmem-132 mutants, whereas gain-of-function of TMEM132D in mammalian cells inhibits WRC, leading to decreased abundance of select WRC components, impaired actin nucleation and cell motility. We propose that metazoan TMEM132 family proteins play evolutionarily conserved roles in regulating NAP1 protein homologs to restrict inappropriate WRC activity, cytoskeletal and morphologic changes in the cell.

Published

2021

8. The conserved transmembrane protein TMEM-39 coordinates with COPII to promote collagen secretion and regulate ER stress response.

Author

Zhang, Zhe, Chisholm, Andrew D1, Zhang, Zhe, Luo, Shuo, Barbosa, Guilherme Oliveira, Bai, Meirong, Kornberg, Thomas B, Ma, Dengke K, Zhang, Zhe, Chisholm, Andrew D1, Zhang, Zhe, Luo, Shuo, Barbosa, Guilherme Oliveira, Bai, Meirong, Kornberg, Thomas B, and Ma, Dengke K

Abstract

Dysregulation of collagen production and secretion contributes to aging and tissue fibrosis of major organs. How procollagen proteins in the endoplasmic reticulum (ER) route as specialized cargos for secretion remains to be fully elucidated. Here, we report that TMEM39, an ER-localized transmembrane protein, regulates production and secretory cargo trafficking of procollagen. We identify the C. elegans ortholog TMEM-39 from an unbiased RNAi screen and show that deficiency of tmem-39 leads to striking defects in cuticle collagen production and constitutively high ER stress response. RNAi knockdown of the tmem-39 ortholog in Drosophila causes similar defects in collagen secretion from fat body cells. The cytosolic domain of human TMEM39A binds to Sec23A, a vesicle coat protein that drives collagen secretion and vesicular trafficking. TMEM-39 regulation of collagen secretion is independent of ER stress response and autophagy. We propose that the roles of TMEM-39 in collagen secretion and ER homeostasis are likely evolutionarily conserved.

Published

2021

9. The conserved autoimmune-disease risk gene TMEM39A regulates lysosome dynamics.

Author

Luo, Shuo, Luo, Shuo, Wang, Xin, Bai, Meirong, Jiang, Wei, Zhang, Zhe, Chen, Yifan, Ma, Dengke K, Luo, Shuo, Luo, Shuo, Wang, Xin, Bai, Meirong, Jiang, Wei, Zhang, Zhe, Chen, Yifan, and Ma, Dengke K

Abstract

TMEM39A encodes an evolutionarily conserved transmembrane protein and carries single-nucleotide polymorphisms associated with increased risk of major human autoimmune diseases, including multiple sclerosis. The exact cellular function of TMEM39A remains not well understood. Here, we report that TMEM-39, the sole Caenorhabditis elegans (C. elegans) ortholog of TMEM39A, regulates lysosome distribution and accumulation. Elimination of tmem-39 leads to lysosome tubularization and reduced lysosome mobility, as well as accumulation of the lysosome-associated membrane protein LMP-1. In mammalian cells, loss of TMEM39A leads to redistribution of lysosomes from the perinuclear region to cell periphery. Mechanistically, TMEM39A interacts with the dynein intermediate light chain DYNC1I2 to maintain proper lysosome distribution. Deficiency of tmem-39 or the DYNC1I2 homolog in C. elegans impairs mTOR signaling and activates the downstream TFEB-like transcription factor HLH-30. We propose evolutionarily conserved roles of TMEM39 family proteins in regulating lysosome distribution and lysosome-associated signaling, dysfunction of which in humans may underlie aspects of autoimmune diseases.

Published

2021

10. Neuronal GDPGP1 and glycogen metabolism: friend or foe?

Author

Singhal, Neel S, Singhal, Neel S, Lee, Evan M, Ma, Dengke K, Singhal, Neel S, Singhal, Neel S, Lee, Evan M, and Ma, Dengke K

Abstract

The adult brain consumes glucose for energy needs and stores glucose as glycogen mainly in astrocytes. Schulz et al. (2020. J. Cell Biol.https://doi.org/10.1083/jcb.201807127) identify the stress-regulated metabolic enzyme GDPGP1 that promotes neuronal survival likely through glycogen reserves in mouse and C. elegans neurons.

Published

2020

11. Cytoprotection by a naturally occurring variant of ATP5G1 in Arctic ground squirrel neural progenitor cells.

Author

Singhal, Neel S, Singhal, Neel S, Bai, Meirong, Lee, Evan M, Luo, Shuo, Cook, Kayleigh R, Ma, Dengke K, Singhal, Neel S, Singhal, Neel S, Bai, Meirong, Lee, Evan M, Luo, Shuo, Cook, Kayleigh R, and Ma, Dengke K

Abstract

Many organisms in nature have evolved mechanisms to tolerate severe hypoxia or ischemia, including the hibernation-capable Arctic ground squirrel (AGS). Although hypoxic or ischemia tolerance in AGS involves physiological adaptations, little is known about the critical cellular mechanisms underlying intrinsic AGS cell resilience to metabolic stress. Through cell survival-based cDNA expression screens in neural progenitor cells, we identify a genetic variant of AGS Atp5g1 that confers cell resilience to metabolic stress. Atp5g1 encodes a subunit of the mitochondrial ATP synthase. Ectopic expression in mouse cells and CRISPR/Cas9 base editing of endogenous AGS loci revealed causal roles of one AGS-specific amino acid substitution in mediating cytoprotection by AGS ATP5G1. AGS ATP5G1 promotes metabolic stress resilience by modulating mitochondrial morphological change and metabolic functions. Our results identify a naturally occurring variant of ATP5G1 from a mammalian hibernator that critically contributes to intrinsic cytoprotection against metabolic stress.

Published

2020

12. Broadly conserved roles of TMEM131 family proteins in intracellular collagen assembly and secretory cargo trafficking.

Author

Zhang, Zhe, Zhang, Zhe, Bai, Meirong, Barbosa, Guilherme Oliveira, Chen, Andrew, Wei, Yuehua, Luo, Shuo, Wang, Xin, Wang, Bingying, Tsukui, Tatsuya, Li, Hao, Sheppard, Dean, Kornberg, Thomas B, Ma, Dengke K, Zhang, Zhe, Zhang, Zhe, Bai, Meirong, Barbosa, Guilherme Oliveira, Chen, Andrew, Wei, Yuehua, Luo, Shuo, Wang, Xin, Wang, Bingying, Tsukui, Tatsuya, Li, Hao, Sheppard, Dean, Kornberg, Thomas B, and Ma, Dengke K

Abstract

Collagen is the most abundant protein in animals. Its dysregulation contributes to aging and many human disorders, including pathological tissue fibrosis in major organs. How premature collagen proteins in the endoplasmic reticulum (ER) assemble and route for secretion remains molecularly undefined. From an RNA interference screen, we identified an uncharacterized Caenorhabditis elegans gene tmem-131, deficiency of which impairs collagen production and activates ER stress response. We find that amino termini of human TMEM131 contain bacterial PapD chaperone-like domains, which recruit premature collagen monomers for proper assembly and secretion. Carboxy termini of TMEM131 interact with TRAPPC8, a component of the TRAPP tethering complex, to drive collagen cargo trafficking from ER to the Golgi. We provide evidence that previously undescribed roles of TMEM131 in collagen recruitment and secretion are evolutionarily conserved in C. elegans, Drosophila, and humans.

Published

2020

13. Neuronal GDPGP1 and glycogen metabolism: friend or foe?

Author

Singhal, Neel S, Singhal, Neel S, Lee, Evan M, Ma, Dengke K, Singhal, Neel S, Singhal, Neel S, Lee, Evan M, and Ma, Dengke K

Abstract

The adult brain consumes glucose for energy needs and stores glucose as glycogen mainly in astrocytes. Schulz et al. (2020. J. Cell Biol.https://doi.org/10.1083/jcb.201807127) identify the stress-regulated metabolic enzyme GDPGP1 that promotes neuronal survival likely through glycogen reserves in mouse and C. elegans neurons.

Published

2020

14. Broadly conserved roles of TMEM131 family proteins in intracellular collagen assembly and secretory cargo trafficking.

Author

Zhang, Zhe, Zhang, Zhe, Bai, Meirong, Barbosa, Guilherme Oliveira, Chen, Andrew, Wei, Yuehua, Luo, Shuo, Wang, Xin, Wang, Bingying, Tsukui, Tatsuya, Li, Hao, Sheppard, Dean, Kornberg, Thomas B, Ma, Dengke K, Zhang, Zhe, Zhang, Zhe, Bai, Meirong, Barbosa, Guilherme Oliveira, Chen, Andrew, Wei, Yuehua, Luo, Shuo, Wang, Xin, Wang, Bingying, Tsukui, Tatsuya, Li, Hao, Sheppard, Dean, Kornberg, Thomas B, and Ma, Dengke K

Abstract

Collagen is the most abundant protein in animals. Its dysregulation contributes to aging and many human disorders, including pathological tissue fibrosis in major organs. How premature collagen proteins in the endoplasmic reticulum (ER) assemble and route for secretion remains molecularly undefined. From an RNA interference screen, we identified an uncharacterized Caenorhabditis elegans gene tmem-131, deficiency of which impairs collagen production and activates ER stress response. We find that amino termini of human TMEM131 contain bacterial PapD chaperone-like domains, which recruit premature collagen monomers for proper assembly and secretion. Carboxy termini of TMEM131 interact with TRAPPC8, a component of the TRAPP tethering complex, to drive collagen cargo trafficking from ER to the Golgi. We provide evidence that previously undescribed roles of TMEM131 in collagen recruitment and secretion are evolutionarily conserved in C. elegans, Drosophila, and humans.

Published

2020

15. Cytoprotection by a naturally occurring variant of ATP5G1 in Arctic ground squirrel neural progenitor cells.

Author

Singhal, Neel S, Singhal, Neel S, Bai, Meirong, Lee, Evan M, Luo, Shuo, Cook, Kayleigh R, Ma, Dengke K, Singhal, Neel S, Singhal, Neel S, Bai, Meirong, Lee, Evan M, Luo, Shuo, Cook, Kayleigh R, and Ma, Dengke K

Abstract

Many organisms in nature have evolved mechanisms to tolerate severe hypoxia or ischemia, including the hibernation-capable Arctic ground squirrel (AGS). Although hypoxic or ischemia tolerance in AGS involves physiological adaptations, little is known about the critical cellular mechanisms underlying intrinsic AGS cell resilience to metabolic stress. Through cell survival-based cDNA expression screens in neural progenitor cells, we identify a genetic variant of AGS Atp5g1 that confers cell resilience to metabolic stress. Atp5g1 encodes a subunit of the mitochondrial ATP synthase. Ectopic expression in mouse cells and CRISPR/Cas9 base editing of endogenous AGS loci revealed causal roles of one AGS-specific amino acid substitution in mediating cytoprotection by AGS ATP5G1. AGS ATP5G1 promotes metabolic stress resilience by modulating mitochondrial morphological change and metabolic functions. Our results identify a naturally occurring variant of ATP5G1 from a mammalian hibernator that critically contributes to intrinsic cytoprotection against metabolic stress.

Published

2020

16. Resilience to Injury: A New Approach to Neuroprotection?

Author

Singhal, Neel S, Singhal, Neel S, Sun, Chung-Huan, Lee, Evan M, Ma, Dengke K, Singhal, Neel S, Singhal, Neel S, Sun, Chung-Huan, Lee, Evan M, and Ma, Dengke K

Abstract

Despite thousands of neuroprotectants demonstrating promise in preclinical trials, a neuroprotective therapeutic has yet to be approved for the treatment of acute brain injuries such as stroke or traumatic brain injury. Developing a more detailed understanding of models and populations demonstrating "neurological resilience" in spite of brain injury can give us important insights into new translational therapies. Resilience is the process of active adaptation to a stressor. In the context of neuroprotection, models of preconditioning and unique animal models of extreme physiology (such as hibernating species) reliably demonstrate resilience in the laboratory setting. In the clinical setting, resilience is observed in young patients and can be found in those with specific genetic polymorphisms. These important examples of resilience can help transform and extend the current neuroprotective framework from simply countering the injurious cascade into one that anticipates, monitors, and optimizes patients' physiological responses from the time of injury throughout the process of recovery. This review summarizes the underpinnings of key adaptations common to models of resilience and how this understanding can be applied to new neuroprotective approaches.

Published

2020

17. MDT-15/MED15 permits longevity at low temperature via enhancing lipidostasis and proteostasis.

Author

Lee, Dongyeop, Campisi, Judith1, Lee, Dongyeop, An, Seon Woo A, Jung, Yoonji, Yamaoka, Yasuyo, Ryu, Youngjae, Goh, Grace Ying Shyen, Beigi, Arshia, Yang, Jae-Seong, Jung, Gyoo Yeol, Ma, Dengke K, Ha, Chang Man, Taubert, Stefan, Lee, Youngsook, Lee, Seung-Jae V, Lee, Dongyeop, Campisi, Judith1, Lee, Dongyeop, An, Seon Woo A, Jung, Yoonji, Yamaoka, Yasuyo, Ryu, Youngjae, Goh, Grace Ying Shyen, Beigi, Arshia, Yang, Jae-Seong, Jung, Gyoo Yeol, Ma, Dengke K, Ha, Chang Man, Taubert, Stefan, Lee, Youngsook, and Lee, Seung-Jae V

Abstract

Low temperatures delay aging and promote longevity in many organisms. However, the metabolic and homeostatic aspects of low-temperature-induced longevity remain poorly understood. Here, we show that lipid homeostasis regulated by Caenorhabditis elegans Mediator 15 (MDT-15 or MED15), a transcriptional coregulator, is essential for low-temperature-induced longevity and proteostasis. We find that inhibition of mdt-15 prevents animals from living long at low temperatures. We show that MDT-15 up-regulates fat-7, a fatty acid desaturase that converts saturated fatty acids (SFAs) to unsaturated fatty acids (UFAs), at low temperatures. We then demonstrate that maintaining a high UFA/SFA ratio is essential for proteostasis at low temperatures. We show that dietary supplementation with a monounsaturated fatty acid, oleic acid (OA), substantially mitigates the short life span and proteotoxicity in mdt-15(-) animals at low temperatures. Thus, lipidostasis regulated by MDT-15 appears to be a limiting factor for proteostasis and longevity at low temperatures. Our findings highlight the crucial roles of lipid regulation in maintaining normal organismal physiology under different environmental conditions.

Published

2019

18. A genetic program mediates cold-warming response and promotes stress-induced phenoptosis in C. elegans.

Author

Jiang, Wei, Jiang, Wei, Wei, Yuehua, Long, Yong, Owen, Arthur, Wang, Bingying, Wu, Xuebing, Luo, Shuo, Dang, Yongjun, Ma, Dengke K, Jiang, Wei, Jiang, Wei, Wei, Yuehua, Long, Yong, Owen, Arthur, Wang, Bingying, Wu, Xuebing, Luo, Shuo, Dang, Yongjun, and Ma, Dengke K

Abstract

How multicellular organisms respond to and are impacted by severe hypothermic stress is largely unknown. From C. elegans screens for mutants abnormally responding to cold-warming stimuli, we identify a molecular genetic pathway comprising ISY-1, a conserved uncharacterized protein, and ZIP-10, a bZIP-type transcription factor. ISY-1 gatekeeps the ZIP-10 transcriptional program by regulating the microRNA mir-60. Downstream of ISY-1 and mir-60, zip-10 levels rapidly and specifically increase upon transient cold-warming exposure. Prolonged zip-10 up-regulation induces several protease-encoding genes and promotes stress-induced organismic death, or phenoptosis, of C. elegans. zip-10 deficiency confers enhanced resistance to prolonged cold-warming stress, more prominently in adults than larvae. We conclude that the ZIP-10 genetic program mediates cold-warming response and may have evolved to promote wild-population kin selection under resource-limiting and thermal stress conditions.

Published

2018

19. Conserved roles of C. elegans and human MANFs in sulfatide binding and cytoprotection.

Author

Bai, Meirong, Bai, Meirong, Vozdek, Roman, Hnízda, Aleš, Jiang, Chenxiao, Wang, Bingying, Kuchar, Ladislav, Li, Tiejun, Zhang, Yuefan, Wood, Chase, Feng, Liang, Dang, Yongjun, Ma, Dengke K, Bai, Meirong, Bai, Meirong, Vozdek, Roman, Hnízda, Aleš, Jiang, Chenxiao, Wang, Bingying, Kuchar, Ladislav, Li, Tiejun, Zhang, Yuefan, Wood, Chase, Feng, Liang, Dang, Yongjun, and Ma, Dengke K

Abstract

Mesencephalic astrocyte-derived neurotrophic factor (MANF) is an endoplasmic reticulum (ER) protein that can be secreted and protects dopamine neurons and cardiomyocytes from ER stress and apoptosis. The mechanism of action of extracellular MANF has long been elusive. From a genetic screen for mutants with abnormal ER stress response, we identified the gene Y54G2A.23 as the evolutionarily conserved C. elegans MANF orthologue. We find that MANF binds to the lipid sulfatide, also known as 3-O-sulfogalactosylceramide present in serum and outer-cell membrane leaflets, directly in isolated forms and in reconstituted lipid micelles. Sulfatide binding promotes cellular MANF uptake and cytoprotection from hypoxia-induced cell death. Heightened ER stress responses of MANF-null C. elegans mutants and mammalian cells are alleviated by human MANF in a sulfatide-dependent manner. Our results demonstrate conserved roles of MANF in sulfatide binding and ER stress response, supporting sulfatide as a long-sought lipid mediator of MANF's cytoprotection.

Published

2018

20. WDR-23 and SKN-1/Nrf2 Coordinate with the BLI-3 Dual Oxidase in Response to Iodide-Triggered Oxidative Stress.

Author

Xu, Zhaofa, Xu, Zhaofa, Hu, Yiman, Deng, Yajun, Chen, Yutao, Hua, Hanqi, Huang, Siyu, Nie, Qian, Pan, Qian, Ma, Dengke K, Ma, Long, Xu, Zhaofa, Xu, Zhaofa, Hu, Yiman, Deng, Yajun, Chen, Yutao, Hua, Hanqi, Huang, Siyu, Nie, Qian, Pan, Qian, Ma, Dengke K, and Ma, Long

Abstract

Animals utilize conserved mechanisms to regulate oxidative stress. The C. elegans SKN-1 protein is homologous to the vertebrate Nrf (NF-E2-related factor) family of cap 'n' collar (CnC) transcription factors and functions as a core regulator of xenobiotic and oxidative stress responses. The WD40 repeat-containing protein WDR-23 is a key negative regulator of SKN-1 activity. We previously found that the oxidative stress induced by excess iodide can be relieved by loss of function in the BLI-3/TSP-15/DOXA-1 dual oxidase complex. To further understand the molecular mechanism of this process, we screened for new mutants that can survive in excess iodide and identified gain-of-function mutations in skn-1 and loss-of-function mutations in wdr-23 The SKN-1C isoform functions in the hypodermis to affect animal's response to excess iodide, while the SKN-1A isoform appears to play a minor role. wdr-23(lf) can interact with bli-3 mutations in a manner different from skn-1(gf) Transcriptome studies suggest that excess iodide causes developmental arrest largely independent of changes in gene expression, and wdr-23(lf) could affect the expression of a subset of genes by a mechanism different from SKN-1 activation. We propose that WDR-23 and SKN-1 coordinate with the BLI-3/TSP-15/DOXA-1 dual oxidase complex in response to iodide-triggered oxidative stress.

Published

2018

21. Conserved roles of C. elegans and human MANFs in sulfatide binding and cytoprotection.

Author

Bai, Meirong, Bai, Meirong, Vozdek, Roman, Hnízda, Aleš, Jiang, Chenxiao, Wang, Bingying, Kuchar, Ladislav, Li, Tiejun, Zhang, Yuefan, Wood, Chase, Feng, Liang, Dang, Yongjun, Ma, Dengke K, Bai, Meirong, Bai, Meirong, Vozdek, Roman, Hnízda, Aleš, Jiang, Chenxiao, Wang, Bingying, Kuchar, Ladislav, Li, Tiejun, Zhang, Yuefan, Wood, Chase, Feng, Liang, Dang, Yongjun, and Ma, Dengke K

Abstract

Mesencephalic astrocyte-derived neurotrophic factor (MANF) is an endoplasmic reticulum (ER) protein that can be secreted and protects dopamine neurons and cardiomyocytes from ER stress and apoptosis. The mechanism of action of extracellular MANF has long been elusive. From a genetic screen for mutants with abnormal ER stress response, we identified the gene Y54G2A.23 as the evolutionarily conserved C. elegans MANF orthologue. We find that MANF binds to the lipid sulfatide, also known as 3-O-sulfogalactosylceramide present in serum and outer-cell membrane leaflets, directly in isolated forms and in reconstituted lipid micelles. Sulfatide binding promotes cellular MANF uptake and cytoprotection from hypoxia-induced cell death. Heightened ER stress responses of MANF-null C. elegans mutants and mammalian cells are alleviated by human MANF in a sulfatide-dependent manner. Our results demonstrate conserved roles of MANF in sulfatide binding and ER stress response, supporting sulfatide as a long-sought lipid mediator of MANF's cytoprotection.

Published

2018

22. A genetic program mediates cold-warming response and promotes stress-induced phenoptosis in C. elegans.

Author

Jiang, Wei, Jiang, Wei, Wei, Yuehua, Long, Yong, Owen, Arthur, Wang, Bingying, Wu, Xuebing, Luo, Shuo, Dang, Yongjun, Ma, Dengke K, Jiang, Wei, Jiang, Wei, Wei, Yuehua, Long, Yong, Owen, Arthur, Wang, Bingying, Wu, Xuebing, Luo, Shuo, Dang, Yongjun, and Ma, Dengke K

Abstract

How multicellular organisms respond to and are impacted by severe hypothermic stress is largely unknown. From C. elegans screens for mutants abnormally responding to cold-warming stimuli, we identify a molecular genetic pathway comprising ISY-1, a conserved uncharacterized protein, and ZIP-10, a bZIP-type transcription factor. ISY-1 gatekeeps the ZIP-10 transcriptional program by regulating the microRNA mir-60. Downstream of ISY-1 and mir-60, zip-10 levels rapidly and specifically increase upon transient cold-warming exposure. Prolonged zip-10 up-regulation induces several protease-encoding genes and promotes stress-induced organismic death, or phenoptosis, of C. elegans. zip-10 deficiency confers enhanced resistance to prolonged cold-warming stress, more prominently in adults than larvae. We conclude that the ZIP-10 genetic program mediates cold-warming response and may have evolved to promote wild-population kin selection under resource-limiting and thermal stress conditions.

Published

2018

23. Acyl-CoA Dehydrogenase Drives Heat Adaptation by Sequestering Fatty Acids.

Author

Ma, Dengke K, Ma, Dengke K, Li, Zhijie, Lu, Alice Y, Sun, Fang, Chen, Sidi, Rothe, Michael, Menzel, Ralph, Sun, Fei, Horvitz, H Robert, Ma, Dengke K, Ma, Dengke K, Li, Zhijie, Lu, Alice Y, Sun, Fang, Chen, Sidi, Rothe, Michael, Menzel, Ralph, Sun, Fei, and Horvitz, H Robert

Abstract

Cells adapt to temperature shifts by adjusting levels of lipid desaturation and membrane fluidity. This fundamental process occurs in nearly all forms of life, but its mechanism in eukaryotes is unknown. We discovered that the evolutionarily conserved Caenorhabditis elegans gene acdh-11 (acyl-CoA dehydrogenase [ACDH]) facilitates heat adaptation by regulating the lipid desaturase FAT-7. Human ACDH deficiency causes the most common inherited disorders of fatty acid oxidation, with syndromes that are exacerbated by hyperthermia. Heat upregulates acdh-11 expression to decrease fat-7 expression. We solved the high-resolution crystal structure of ACDH-11 and established the molecular basis of its selective and high-affinity binding to C11/C12-chain fatty acids. ACDH-11 sequesters C11/C12-chain fatty acids and prevents these fatty acids from activating nuclear hormone receptors and driving fat-7 expression. Thus, the ACDH-11 pathway drives heat adaptation by linking temperature shifts to regulation of lipid desaturase levels and membrane fluidity via an unprecedented mode of fatty acid signaling.

Published

2015

24. Cytochrome P450 drives a HIF-regulated behavioral response to reoxygenation by C. elegans.

Author

Ma, Dengke K, Ma, Dengke K, Rothe, Michael, Zheng, Shu, Bhatla, Nikhil, Pender, Corinne L, Menzel, Ralph, Horvitz, H Robert, Ma, Dengke K, Ma, Dengke K, Rothe, Michael, Zheng, Shu, Bhatla, Nikhil, Pender, Corinne L, Menzel, Ralph, and Horvitz, H Robert

Abstract

Oxygen deprivation followed by reoxygenation causes pathological responses in many disorders, including ischemic stroke, heart attacks, and reperfusion injury. Key aspects of ischemia-reperfusion can be modeled by a Caenorhabditis elegans behavior, the O2-ON response, which is suppressed by hypoxic preconditioning or inactivation of the O2-sensing HIF (hypoxia-inducible factor) hydroxylase EGL-9. From a genetic screen, we found that the cytochrome P450 oxygenase CYP-13A12 acts in response to the EGL-9-HIF-1 pathway to facilitate the O2-ON response. CYP-13A12 promotes oxidation of polyunsaturated fatty acids into eicosanoids, signaling molecules that can strongly affect inflammatory pain and ischemia-reperfusion injury responses in mammals. We propose that roles of the EGL-9-HIF-1 pathway and cytochrome P450 in controlling responses to reoxygenation after anoxia are evolutionarily conserved.

Published

2013