Plasma proteomic and autoantibody profiles reveal the proteomic characteristics involved in longevity families in Bama, China

Ye, Shengliang; Ma, Li; Zhang, Rong; Liu, Fengjuan; Jiang, Peng; Xu, Jun; Cao, Haijun; Du, Xi; Lin, Fen; Cheng, Lu; Zhou, Xuefeng; Shi, Zhihui; Liu, Yeheng; Huang, Yaojin; Wang, Zongkui; Li, Changqing

doi:10.1186/s12014-019-9242-4

Cited by 9 publications

(10 citation statements)

References 62 publications

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“…Inclusion criteria for a manuscript included healthy individuals, proteomics results published on or after 2010, publications/authors provided list of significant/all proteins. Thirty three manuscripts met the inclusion criteria, including 12 that covered human plasma (Enroth et al, 2015; Lehallier et al, 2019; Lind et al, 2019; Menni et al, 2015; Ngo et al, 2016; Orwoll et al, 2018; Santos‐Lozano et al, 2020; Sun et al, 2018; Tanaka et al, 2018; Wang, Zhu, et al, 2019; Wang, Zhang, et al, 2019; Ye et al, 2019), 9 from 14 different matrices in humans (Baird et al, 2012; Bakun et al, 2014; Bell‐Temin et al, 2019; Gueugneau et al, 2014; Heinze et al, 2018; Hennrich et al, 2018; Ubaida‐Mohien et al, 2019; Waldera‐Lupa et al, 2014; Wang, Wang, et al, 2018), and 12 publications covering 21 different species/matrices (Amin et al, 2020; Angelidis et al, 2019; Braun et al, 2016; Cutler et al, 2017; Drulis‐Fajdasz et al, 2018; Gebert et al, 2020; Heinze et al, 2018; Kelley et al, 2018; Meng et al, 2020; Stauch et al, 2015; Wang, Zhu, et al, 2019; Yu et al, 2020). The age range of participants included in these studies spanned from 14 to 103 years, and measures were carried out using multiple platforms including but not limited to liquid chromatography–mass spectrometry (LC‐MS)‐based proteomics, multiplexed proteomic assay using modified aptamers (SOMAscan) and Proximity Extension Assay (PEA, O‐Link) (Gold et al, 2010; Lundberg et al, 2011).…”

Section: Methodsmentioning

confidence: 99%

Proteomics in aging research: A roadmap to clinical, translational research

et al. 2021

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The identification of plasma proteins that systematically change with age and, independent of chronological age, predict accelerated decline of health is an expanding area of research. Circulating proteins are ideal translational “omics” since they are final effectors of physiological pathways and because physicians are accustomed to use information of plasma proteins as biomarkers for diagnosis, prognosis, and tracking the effectiveness of treatments. Recent technological advancements, including mass spectrometry (MS)‐based proteomics, multiplexed proteomic assay using modified aptamers (SOMAscan), and Proximity Extension Assay (PEA, O‐Link), have allowed for the assessment of thousands of proteins in plasma or other biological matrices, which are potentially translatable into new clinical biomarkers and provide new clues about the mechanisms by which aging is associated with health deterioration and functional decline. We carried out a detailed literature search for proteomic studies performed in different matrices (plasma, serum, urine, saliva, tissues) and species using multiple platforms. Herein, we identified 232 proteins that were age‐associated across studies. Enrichment analysis of the 232 age‐associated proteins revealed metabolic pathways previously connected with biological aging both in animal models and in humans, most remarkably insulin‐like growth factor (IGF) signaling, mitogen‐activated protein kinases (MAPK), hypoxia‐inducible factor 1 (HIF1), cytokine signaling, Forkhead Box O (FOXO) metabolic pathways, folate metabolism, advance glycation end products (AGE), and receptor AGE (RAGE) metabolic pathway. Information on these age‐relevant proteins, likely expanded and validated in longitudinal studies and examined in mechanistic studies, will be essential for patient stratification and the development of new treatments aimed at improving health expectancy.

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Section: Methodsmentioning

confidence: 99%

Proteomics in aging research: A roadmap to clinical, translational research

et al. 2021

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“…164,187 Specifically, the plasma proteomic and autoantibody profiles of offspring of long-lived families and age-related controls were compared. 187 TMT labeling enabled the quantification of over 500 proteins, out of which 12 proteins were differentially expressed between the two groups (proteins with increased levels: LPA, DEFA3, immunoglobulin, BLVRB, and PDIA3; proteins with reduced levels: TPM, GBA, DSG2, SRC, CHGA, ITGB3, and TAGLN2). In a second study, 175 proteins were identified to be differentially abundant between the groups, and a panel of five proteins (MMP2, CCL5, PF4, IGFBP2, and C9) may serve as biomarkers to predict healthy aging and longevity.…”

Section: ■ Agingmentioning

confidence: 99%

“…The Bama Yao Autonomous County in China is one of the well-known longevity regions. Multiple genome and population studies have been carried out in the past, and recently, proteomics studies have been pursued. , Specifically, the plasma proteomic and autoantibody profiles of offspring of long-lived families and age-related controls were compared . TMT labeling enabled the quantification of over 500 proteins, out of which 12 proteins were differentially expressed between the two groups (proteins with increased levels: LPA, DEFA3, immunoglobulin, BLVRB, and PDIA3; proteins with reduced levels: TPM, GBA, DSG2, SRC, CHGA, ITGB3, and TAGLN2).…”

Section: Agingmentioning

confidence: 99%

Advances and Utility of the Human Plasma Proteome

et al. 2021

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The study of proteins circulating in blood offers tremendous opportunities to diagnose, stratify, or possibly prevent diseases. With recent technological advances and the urgent need to understand the effects of COVID-19, the proteomic analysis of blood-derived serum and plasma has become even more important for studying human biology and pathophysiology. Here we provide views and perspectives about technological developments and possible clinical applications that use mass-spectrometry(MS)- or affinity-based methods. We discuss examples where plasma proteomics contributed valuable insights into SARS-CoV-2 infections, aging, and hemostasis and the opportunities offered by combining proteomics with genetic data. As a contribution to the Human Proteome Organization (HUPO) Human Plasma Proteome Project (HPPP), we present the Human Plasma PeptideAtlas build 2021-07 that comprises 4395 canonical and 1482 additional nonredundant human proteins detected in 240 MS-based experiments. In addition, we report the new Human Extracellular Vesicle PeptideAtlas 2021-06, which comprises five studies and 2757 canonical proteins detected in extracellular vesicles circulating in blood, of which 74% (2047) are in common with the plasma PeptideAtlas. Our overview summarizes the recent advances, impactful applications, and ongoing challenges for translating plasma proteomics into utility for precision medicine.

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“…In our previous studies [ 6 , 10 ], we found some differentially expressed proteins (DEPs) between Bama longevous family group and normal controls from non-longevous region of China. Some of these DEPs such as PGK1, ENO1, LDHA, LDHB, PKM, and GAPDH, were glycolysis/gluconeogenesis-related proteins.…”

Section: Introductionmentioning

confidence: 99%

Proteomics profiles of blood glucose-related proteins involved in a Chinese longevity cohort

Zhang

Liu

et al. 2022

Clin Proteom

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Background High blood glucose level is one of the main characteristics of diabetes mellitus. Based on previous studies, it is speculated longevity families may have certain advantages in blood glucose regulation. However, limited information on these items has been reported. The purpose of this study was to profile differences of plasma proteomics between longevity subjects (with normal fructosamine (FUN) level) and non-longevity area participants (with exceeding standard FUN level). Methods In this study, a TMT-based proteomics analysis was used to profile differences of plasma proteomics between longevity subjects (with normal FUN level) and non-longevity area participants (with exceeding standard FUN level). Results were validated by Luminex detection. Results A total of 155 differentially expressed proteins (DEPs) were identified between these two groups. The DEPs related to blood glucose regulation were mainly involved in glycolysis/gluconeogenesis, pyruvate metabolism and propanoate metabolism, and most of the DEPs were contained in carbohydrate metabolism, PI3K-Akt pathway, glucagon signaling pathway and inflammatory response. Validation by Luminex detection confirmed that CD163 was down-regulated, and SPARC, PARK 7 and IGFBP-1 were up-regulated in longevity participants. Conclusions This study not only highlighted carbohydrate metabolism, PI3K-Akt pathway, glucagon signaling pathway and inflammatory response may play important roles in blood glucose regulation, but also indicated that YWHAZ, YWHAB, YWHAG, YWHAE, CALM3, CRP, SAA2, PARK 7, IGFBP1 and VNN1 may serve as potential biomarkers for predicting abnormal blood glucose levels.

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Plasma proteomic and autoantibody profiles reveal the proteomic characteristics involved in longevity families in Bama, China

Cited by 9 publications

References 62 publications

Proteomics in aging research: A roadmap to clinical, translational research

Proteomics in aging research: A roadmap to clinical, translational research

Advances and Utility of the Human Plasma Proteome

Proteomics profiles of blood glucose-related proteins involved in a Chinese longevity cohort

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