Lysophosphatidylserine: A Signaling Lipid with Implications in Human Diseases

Chakraborty, Arnab; Kamat, Siddhesh S.

doi:10.1021/acs.chemrev.3c00701

Cited by 3 publications

(10 citation statements)

References 419 publications

(964 reference statements)

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“…Specifically, in the central nervous system, lyso-PS controls the activation of microglial cells, and in turn neuroinflammation, particularly in the cerebellum. On the other hand, in the immune system, this signaling lysophospholipid regulates histamine release from mast cell degranulation, pro-inflammatory responses from macrophages, and the maturation of T cells, to list a few processes 1, 2 . While it is now evident that lyso-PS is ubiquitously present 1 , little remains known on how it is enzymatically produced and metabolized, or what are its physiological functions in other (peripheral) mammalian tissues.…”

Section: Discussionmentioning

confidence: 99%

“…Our studies partly corroborate these findings, and show that ABHD6 functions as a lyso-PS-specific lysophospholipase in the liver and kidney in mice, and selectively controls levels of lyso-PS lipids, but not other lysophospholipids, in these tissues under normal physiological conditions (not in high-fat diet paradigms) ( Figure 3 , Supplementary Figure 2 ). Given its recent links to systemic (glucose) metabolism 1 , it will be interesting to see how dysregulated lyso-PS signaling in the liver might contribute towards metabolic conditions such as hepatic steatosis or systemic insulin resistance (modulated by ABHD6 activity), and crosstalk with other lipid pathways involved in such human diseases.…”

Section: Discussionmentioning

confidence: 99%

“…Given its amphiphilic (hydrophilic and lipophilic) chemical nature, lyso-PS acts as a very potent hormone-like signaling molecule 11 . Hence, the physiological concentrations of lyso-PS are tightly regulated by dedicated enzymes in all mammalian tissues 1, 2 . For example, lyso-PS is biosynthesized from phosphatidylserine (PS) precursors by the action of PS-specific phospholipases.…”

Section: Introductionmentioning

confidence: 99%

“…The glycerolysophospholipid lysophosphatidylserine (lyso-PS) is fast emerging as an important signaling lipid, which is central to the functioning of many important biological processes in mammals, including humans 1,2 . Given its indispensable role in physiology, over the past two decades, the biochemical activities and mechanisms associated with lyso-PS metabolism and signaling have been extensively investigated, mostly in the context of the mammalian central nervous and immune system 1,2 . This study bias stems from numerous genetic mapping of human subjects (patients) or population-level genome-wide association studies, which causally link the dysregulation in lyso-PS metabolism or signaling to an array of hereditary neurological and autoimmune diseases in humans 1,[3][4][5][6][7][8][9][10] .…”

Section: Introductionmentioning

confidence: 99%

“…Given its indispensable role in physiology, over the past two decades, the biochemical activities and mechanisms associated with lyso-PS metabolism and signaling have been extensively investigated, mostly in the context of the mammalian central nervous and immune system 1,2 . This study bias stems from numerous genetic mapping of human subjects (patients) or population-level genome-wide association studies, which causally link the dysregulation in lyso-PS metabolism or signaling to an array of hereditary neurological and autoimmune diseases in humans 1,[3][4][5][6][7][8][9][10] . Despite this, it is now apparent from several recent reports that lyso-PS is quite abundant in almost all mammalian tissues 1 , and yet, very little remains known of its physiological role or metabolism beyond the human nervous and immune systems.…”

Section: Introductionmentioning

confidence: 99%

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Identification of ABHD6 as a regulator of lysophosphatidylserines in the mammalian liver and kidneys

Chakraborty,

Punnamraju,

Sajeevan

et al. 2024

Preprint

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SUMMARYLysophosphatidylserine (lyso-PS) is a potent hormone-like signaling lysophospholipid, which regulates many facets of mammalian biology and dysregulation in its metabolism is associated with several human neurological and autoimmune diseases. Despite the physiological importance and causal relation with human pathophysiology, little is known about the metabolism of lyso-PS in tissues other than the nervous and immune systems. To address this problem, here, we attempted to identify one (or more) lipase(s) capable of degrading lyso-PS in different mammalian tissues. We found that the membrane proteomic fraction of most mammalian tissues possess lyso-PS lipase activity, yet interestingly, the only bona fide lyso-PS lipase ABHD12 displays this enzymatic activity and has control over lyso-PS metabolism only in the mammalian brain. Using anin vitroinhibitor screen against membrane proteomic fractions of different tissues, we find that another lipase from the metabolic serine hydrolase family, ABHD6, is a putative lyso-PS lipase in the mouse liver and kidney. Finally, using pharmacological tools, we validate the lyso-PS lipase activity of ABHD6in vivo, and functionally designate this enzyme as a major lyso-PS lipase in primary hepatocytes, and the mammalian liver and kidneys.HIGHLIGHTSLyso-PS lipase enzymatic activity is present in the membrane proteomic fraction of most mammalian tissuesAnin vitroinhibitor screen identifies ABHD6 as a putative lyso-PS lipase in the liver and kidneyABHD6 functions as a lyso-PS lipase in primary hepatocytesABHD6 also performs lyso-PS lipase activityin vivoand regulates lyso-PS levels in the liver and kidney

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Identification of ABHD6 as a regulator of lysophosphatidylserines in the mammalian liver and kidneys

Chakraborty,

Punnamraju,

Sajeevan

et al. 2024

Preprint

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Benzo[a]pyrene exposure induces anxiety-like behaviors in the mice through brain metabolic alterations

Li,

Xie,

Xiao

et al. 2024

Science of The Total Environment

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Integrated Transcriptomic Analyses of Liver and Mammary Gland Tissues Reveals the Regulatory Mechanism Underlying Dairy Goats at Late Lactation When Feeding Rumen-Protected Lysine

Dai,

Han,

Sun

et al. 2024

IJMS

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Although low-protein diets can improve the nitrogen utilization efficiency and alleviate economic pressures in ruminants, they may also negatively impact dairy performance. Rumen-protected lysine (RPL) supplementation can improve the health status and growth performance of ruminants without compromising nitrogen utilization efficiency and feed intake. In this study, a total of thirty-three multiparous dairy goats in the late-lactation period were randomly divided into three groups that were separately fed the control diet (namely the protein-adequacy group), the low-protein diet (namely the protein-deficient group), and the RPL-supplemented protein-deficient diet (namely RPL-supplementation group) for five weeks. Here, we investigated the molecular mechanisms regarding how low-protein diets with RPL supplementation compromise lactation phenotypes in dairy goats through cross-tissue transcriptomic analyses. Dietary protein deficiency caused an imbalance in amino acid (AA) intake, disrupted hepatic function, and impaired milk synthesis. Transcriptomic analyses further showed that RPL supplementation exhibited some beneficial effects, like mitigating abnormal lipid and energy metabolism in the liver, elevating hepatic resistance to oxidative stress, improving the mammary absorption of AAs, as well as activating mammary lipid and protein anabolism primarily through peroxisome proliferator-activated receptor (PPAR) and janus kinase-signal transducer (JAK)—signal transducer and activator of transcription (STAT) signaling, respectively. RPL supplementation of a low-protein diet contributes to maintaining late lactation in dairy goats primarily through mitigating hepatic energy disturbances and activating both lipid and protein metabolism in the mammary glands. Since RPL supplementation initiated a series of comprised events on mammary protein and lipid metabolism as well as the hepatic function and energy generation in dairy goats under protein deficiency during late lactation, these findings thus provide some insights into how RPL supplementation helps maintain milk production and health in dairy mammals especially at late lactation.

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Lysophosphatidylserine: A Signaling Lipid with Implications in Human Diseases

Cited by 3 publications

References 419 publications

Identification of ABHD6 as a regulator of lysophosphatidylserines in the mammalian liver and kidneys

Identification of ABHD6 as a regulator of lysophosphatidylserines in the mammalian liver and kidneys

Benzo[a]pyrene exposure induces anxiety-like behaviors in the mice through brain metabolic alterations

Integrated Transcriptomic Analyses of Liver and Mammary Gland Tissues Reveals the Regulatory Mechanism Underlying Dairy Goats at Late Lactation When Feeding Rumen-Protected Lysine

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