Influence of the Human Lipidome on Epicardial Fat Volume in Mexican American Individuals

Ana Cristina Leandro; Laura F. Michael; Marcio Almeida; Mikko Kuokkanen; Kevin Huynh; Corey Giles; Thy Duong; Vincent P. Diego; Ravindranath Duggirala; Geoffrey D. Clarke; John Blangero; Peter J. Meikle; Joanne E. Curran

doi:10.3389/fcvm.2022.889985

Influence of the Human Lipidome on Epicardial Fat Volume in Mexican American Individuals

Ana Cristina Leandro, Laura F. Michael, Marcio Almeida, Mikko Kuokkanen, Kevin Huynh, Corey Giles, Thy Duong, Vincent P. Diego, Ravindranath Duggirala, Geoffrey D. Clarke, John Blangero, Peter J. Meikle, Joanne E. Curran

Research output: Contribution to journal › Article › Research › peer-review

7 Citations (Scopus)

Abstract

Introduction: Cardiovascular disease (CVD) is the leading cause of mortality worldwide and is the leading cause of death in the US. Lipid dysregulation is a well-known precursor to metabolic diseases, including CVD. There is a growing body of literature that suggests MRI-derived epicardial fat volume, or epicardial adipose tissue (EAT) volume, is linked to the development of coronary artery disease. Interestingly, epicardial fat is also actively involved in lipid and energy homeostasis, with epicardial adipose tissue having a greater capacity for release and uptake of free fatty acids. However, there is a scarcity of knowledge on the influence of plasma lipids on EAT volume. Aim: The focus of this study is on the identification of novel lipidomic species associated with CMRI-derived measures of epicardial fat in Mexican American individuals. Methods: We performed lipidomic profiling on 200 Mexican American individuals. High-throughput mass spectrometry enabled rapid capture of precise lipidomic profiles, providing measures of 799 unique species from circulating plasma samples. Because of our extended pedigree design, we utilized a standard quantitative genetic linear mixed model analysis to determine whether lipids were correlated with EAT by formally testing for association between each lipid species and the CMRI epicardial fat phenotype. Results: After correction for multiple testing using the FDR approach, we identified 135 lipid species showing significant association with epicardial fat. Of those, 131 lipid species were positively correlated with EAT, where increased circulating lipid levels were correlated with increased epicardial fat. Interestingly, the top 10 lipid species associated with an increased epicardial fat volume were from the deoxyceramide (Cer(m)) and triacylglycerol (TG) families. Deoxyceramides are atypical and neurotoxic sphingolipids. Triacylglycerols are an abundant lipid class and comprise the bulk of storage fat in tissues. Pathologically elevated TG and Cer(m) levels are related to CVD risk and, in our study, to EAT volume. Conclusion: Our results indicate that specific lipid abnormalities such as enriched saturated triacylglycerols and the presence of toxic ceramides Cer(m) in plasma of our individuals could precede CVD with increased EAT volume.

Original language	English
Article number	889985
Number of pages	15
Journal	Frontiers in Cardiovascular Medicine
Volume	9
DOIs	https://doi.org/10.3389/fcvm.2022.889985
Publication status	Published - 6 Jun 2022
Externally published	Yes

Keywords

cardiovascular disease
CMRI
epicardial fat volume
lipidomic profiles
Mexican Americans

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3389/fcvm.2022.889985Licence: CC BY

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Leandro, A. C., Michael, L. F., Almeida, M., Kuokkanen, M., Huynh, K., Giles, C., Duong, T., Diego, V. P., Duggirala, R., Clarke, G. D., Blangero, J., Meikle, P. J., & Curran, J. E. (2022). Influence of the Human Lipidome on Epicardial Fat Volume in Mexican American Individuals. Frontiers in Cardiovascular Medicine, 9, Article 889985. https://doi.org/10.3389/fcvm.2022.889985

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title = "Influence of the Human Lipidome on Epicardial Fat Volume in Mexican American Individuals",

abstract = "Introduction: Cardiovascular disease (CVD) is the leading cause of mortality worldwide and is the leading cause of death in the US. Lipid dysregulation is a well-known precursor to metabolic diseases, including CVD. There is a growing body of literature that suggests MRI-derived epicardial fat volume, or epicardial adipose tissue (EAT) volume, is linked to the development of coronary artery disease. Interestingly, epicardial fat is also actively involved in lipid and energy homeostasis, with epicardial adipose tissue having a greater capacity for release and uptake of free fatty acids. However, there is a scarcity of knowledge on the influence of plasma lipids on EAT volume. Aim: The focus of this study is on the identification of novel lipidomic species associated with CMRI-derived measures of epicardial fat in Mexican American individuals. Methods: We performed lipidomic profiling on 200 Mexican American individuals. High-throughput mass spectrometry enabled rapid capture of precise lipidomic profiles, providing measures of 799 unique species from circulating plasma samples. Because of our extended pedigree design, we utilized a standard quantitative genetic linear mixed model analysis to determine whether lipids were correlated with EAT by formally testing for association between each lipid species and the CMRI epicardial fat phenotype. Results: After correction for multiple testing using the FDR approach, we identified 135 lipid species showing significant association with epicardial fat. Of those, 131 lipid species were positively correlated with EAT, where increased circulating lipid levels were correlated with increased epicardial fat. Interestingly, the top 10 lipid species associated with an increased epicardial fat volume were from the deoxyceramide (Cer(m)) and triacylglycerol (TG) families. Deoxyceramides are atypical and neurotoxic sphingolipids. Triacylglycerols are an abundant lipid class and comprise the bulk of storage fat in tissues. Pathologically elevated TG and Cer(m) levels are related to CVD risk and, in our study, to EAT volume. Conclusion: Our results indicate that specific lipid abnormalities such as enriched saturated triacylglycerols and the presence of toxic ceramides Cer(m) in plasma of our individuals could precede CVD with increased EAT volume.",

keywords = "cardiovascular disease, CMRI, epicardial fat volume, lipidomic profiles, Mexican Americans",

author = "Leandro, {Ana Cristina} and Michael, {Laura F.} and Marcio Almeida and Mikko Kuokkanen and Kevin Huynh and Corey Giles and Thy Duong and Diego, {Vincent P.} and Ravindranath Duggirala and Clarke, {Geoffrey D.} and John Blangero and Meikle, {Peter J.} and Curran, {Joanne E.}",

note = "Funding Information: This work was supported in part by National Institutes of Health (NIH) grants P01 HL045522 (SAFHS data collection), R01 HL140681 (lipid profiling), R37 MH059490 (analytical methods and software used), R01 EB015611 (analytical methods and software used), Eli Lilly and Company (cardiac imaging) and a grant from the Valley Baptist Legacy Foundation for Project THRIVE (biorepository). This work was conducted in part in facilities constructed under the support of NIH grant C06 RR020547. PM was supported by a L3 Investigator grant from the National Health and Medical Research Council of Australia (2009965). KH was supported by a National Health and Medical Research Council of Australia investigator grant (1197190). The funders were not involved in the study design, collection, analysis, interpretation of data, the writing of this article or the decision to submit it for publication. Funding Information: The authors thank and acknowledge the participants of the San Antonio Family Heart Study for their continued involvement in our research programs. We thank Katherine Truax, Marcelo Leandro, and Johnathon Waggoner from the Department of Human Genetics and South Texas Diabetes and Obesity Institute, UTRGV for laboratory assistance and Scott Mc Ahren from Eli Lilly for assistance with study quality control. Publisher Copyright: Copyright {\textcopyright} 2022 Leandro, Michael, Almeida, Kuokkanen, Huynh, Giles, Duong, Diego, Duggirala, Clarke, Blangero, Meikle and Curran.",

year = "2022",

month = jun,

day = "6",

doi = "10.3389/fcvm.2022.889985",

language = "English",

volume = "9",

journal = "Frontiers in Cardiovascular Medicine",

issn = "2297-055X",

publisher = "Frontiers Media SA",

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TY - JOUR

T1 - Influence of the Human Lipidome on Epicardial Fat Volume in Mexican American Individuals

AU - Leandro, Ana Cristina

AU - Michael, Laura F.

AU - Almeida, Marcio

AU - Kuokkanen, Mikko

AU - Huynh, Kevin

AU - Giles, Corey

AU - Duong, Thy

AU - Diego, Vincent P.

AU - Duggirala, Ravindranath

AU - Clarke, Geoffrey D.

AU - Blangero, John

AU - Meikle, Peter J.

AU - Curran, Joanne E.

N1 - Funding Information: This work was supported in part by National Institutes of Health (NIH) grants P01 HL045522 (SAFHS data collection), R01 HL140681 (lipid profiling), R37 MH059490 (analytical methods and software used), R01 EB015611 (analytical methods and software used), Eli Lilly and Company (cardiac imaging) and a grant from the Valley Baptist Legacy Foundation for Project THRIVE (biorepository). This work was conducted in part in facilities constructed under the support of NIH grant C06 RR020547. PM was supported by a L3 Investigator grant from the National Health and Medical Research Council of Australia (2009965). KH was supported by a National Health and Medical Research Council of Australia investigator grant (1197190). The funders were not involved in the study design, collection, analysis, interpretation of data, the writing of this article or the decision to submit it for publication. Funding Information: The authors thank and acknowledge the participants of the San Antonio Family Heart Study for their continued involvement in our research programs. We thank Katherine Truax, Marcelo Leandro, and Johnathon Waggoner from the Department of Human Genetics and South Texas Diabetes and Obesity Institute, UTRGV for laboratory assistance and Scott Mc Ahren from Eli Lilly for assistance with study quality control. Publisher Copyright: Copyright © 2022 Leandro, Michael, Almeida, Kuokkanen, Huynh, Giles, Duong, Diego, Duggirala, Clarke, Blangero, Meikle and Curran.

PY - 2022/6/6

Y1 - 2022/6/6

N2 - Introduction: Cardiovascular disease (CVD) is the leading cause of mortality worldwide and is the leading cause of death in the US. Lipid dysregulation is a well-known precursor to metabolic diseases, including CVD. There is a growing body of literature that suggests MRI-derived epicardial fat volume, or epicardial adipose tissue (EAT) volume, is linked to the development of coronary artery disease. Interestingly, epicardial fat is also actively involved in lipid and energy homeostasis, with epicardial adipose tissue having a greater capacity for release and uptake of free fatty acids. However, there is a scarcity of knowledge on the influence of plasma lipids on EAT volume. Aim: The focus of this study is on the identification of novel lipidomic species associated with CMRI-derived measures of epicardial fat in Mexican American individuals. Methods: We performed lipidomic profiling on 200 Mexican American individuals. High-throughput mass spectrometry enabled rapid capture of precise lipidomic profiles, providing measures of 799 unique species from circulating plasma samples. Because of our extended pedigree design, we utilized a standard quantitative genetic linear mixed model analysis to determine whether lipids were correlated with EAT by formally testing for association between each lipid species and the CMRI epicardial fat phenotype. Results: After correction for multiple testing using the FDR approach, we identified 135 lipid species showing significant association with epicardial fat. Of those, 131 lipid species were positively correlated with EAT, where increased circulating lipid levels were correlated with increased epicardial fat. Interestingly, the top 10 lipid species associated with an increased epicardial fat volume were from the deoxyceramide (Cer(m)) and triacylglycerol (TG) families. Deoxyceramides are atypical and neurotoxic sphingolipids. Triacylglycerols are an abundant lipid class and comprise the bulk of storage fat in tissues. Pathologically elevated TG and Cer(m) levels are related to CVD risk and, in our study, to EAT volume. Conclusion: Our results indicate that specific lipid abnormalities such as enriched saturated triacylglycerols and the presence of toxic ceramides Cer(m) in plasma of our individuals could precede CVD with increased EAT volume.

AB - Introduction: Cardiovascular disease (CVD) is the leading cause of mortality worldwide and is the leading cause of death in the US. Lipid dysregulation is a well-known precursor to metabolic diseases, including CVD. There is a growing body of literature that suggests MRI-derived epicardial fat volume, or epicardial adipose tissue (EAT) volume, is linked to the development of coronary artery disease. Interestingly, epicardial fat is also actively involved in lipid and energy homeostasis, with epicardial adipose tissue having a greater capacity for release and uptake of free fatty acids. However, there is a scarcity of knowledge on the influence of plasma lipids on EAT volume. Aim: The focus of this study is on the identification of novel lipidomic species associated with CMRI-derived measures of epicardial fat in Mexican American individuals. Methods: We performed lipidomic profiling on 200 Mexican American individuals. High-throughput mass spectrometry enabled rapid capture of precise lipidomic profiles, providing measures of 799 unique species from circulating plasma samples. Because of our extended pedigree design, we utilized a standard quantitative genetic linear mixed model analysis to determine whether lipids were correlated with EAT by formally testing for association between each lipid species and the CMRI epicardial fat phenotype. Results: After correction for multiple testing using the FDR approach, we identified 135 lipid species showing significant association with epicardial fat. Of those, 131 lipid species were positively correlated with EAT, where increased circulating lipid levels were correlated with increased epicardial fat. Interestingly, the top 10 lipid species associated with an increased epicardial fat volume were from the deoxyceramide (Cer(m)) and triacylglycerol (TG) families. Deoxyceramides are atypical and neurotoxic sphingolipids. Triacylglycerols are an abundant lipid class and comprise the bulk of storage fat in tissues. Pathologically elevated TG and Cer(m) levels are related to CVD risk and, in our study, to EAT volume. Conclusion: Our results indicate that specific lipid abnormalities such as enriched saturated triacylglycerols and the presence of toxic ceramides Cer(m) in plasma of our individuals could precede CVD with increased EAT volume.

KW - cardiovascular disease

KW - CMRI

KW - epicardial fat volume

KW - lipidomic profiles

KW - Mexican Americans

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U2 - 10.3389/fcvm.2022.889985

DO - 10.3389/fcvm.2022.889985

M3 - Article

C2 - 35734277

AN - SCOPUS:85138697516

SN - 2297-055X

VL - 9

JO - Frontiers in Cardiovascular Medicine

JF - Frontiers in Cardiovascular Medicine

M1 - 889985

ER -

Influence of the Human Lipidome on Epicardial Fat Volume in Mexican American Individuals

Abstract

Keywords

UN SDGs

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