Differences in the Circulating Proteome in Individuals with versus without Sickle Cell Trait

Yanwei Cai; Nora Franceschini; Aditya Surapaneni; Melanie E Garrett; Usman A Tahir; Li Hsu; Marilyn J Telen; Bing Yu; Hua Tang; Yun Li; Simin Liu; Robert E Gerszten; Josef Coresh; JoAnn E Manson; Genevieve L Wojcik; Charles Kooperberg; Paul L Auer; Matthew W Foster; Morgan E Grams; Allison E Ashley-Koch; Laura M Raffield; Alex P Reiner

doi:10.2215/CJN.0000000000000257

Differences in the Circulating Proteome in Individuals with versus without Sickle Cell Trait

Clin J Am Soc Nephrol. 2023 Nov 1;18(11):1416-1425. doi: 10.2215/CJN.0000000000000257. Epub 2023 Aug 3.

Authors

Yanwei Cai¹, Nora Franceschini², Aditya Surapaneni^{3

4}, Melanie E Garrett⁵, Usman A Tahir^{6

7}, Li Hsu¹, Marilyn J Telen^{5

8}, Bing Yu⁹, Hua Tang¹⁰, Yun Li¹¹, Simin Liu¹², Robert E Gerszten^{6

7}, Josef Coresh^{3

4}, JoAnn E Manson¹³, Genevieve L Wojcik³, Charles Kooperberg², Paul L Auer¹⁴, Matthew W Foster¹⁵, Morgan E Grams¹⁶, Allison E Ashley-Koch⁵, Laura M Raffield¹¹, Alex P Reiner^{1

17}

Affiliations

¹ Division of Public Health Sciences, Fred Hutchinson Cancer Center, Seattle, Washington.
² Department of Epidemiology, Gillings School of Global Public Health, University of North Carolina, Chapel Hill, North Carolina.
³ Department of Epidemiology and Welch Center for Prevention, Epidemiology, & Clinical Research, Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland.
⁴ Welch Center for Prevention, Epidemiology, & Clinical Research, Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland.
⁵ Duke Molecular Physiology Institute, Duke University Medical Center, Durham, North Carolina.
⁶ Division of Cardiovascular Medicine, Beth Israel Deaconess Medical Center, Boston, Massachusetts.
⁷ Broad Institute of Harvard University and Massachusetts Institute of Technology, Cambridge, Massachusetts.
⁸ Division of Hematology, Department of Medicine, Duke University Medical Center, Durham, North Carolina.
⁹ School of Public Health, The University of Texas Health Science Center at Houston, Houston, Texas.
¹⁰ Department of Genetics, Stanford University School of Medicine, Stanford, California.
¹¹ Department of Genetics, University of North Carolina, Chapel Hill, North Carolina.
¹² Center for Global Cardiometabolic Health, Departments of Epidemiology, Medicine, and Surgery, Brown University, Providence, Rhode Island.
¹³ Brigham and Women's Hospital, Harvard Medical School, Harvard T.H. Chan School of Public Health, Boston, Massachusetts.
¹⁴ Division of Biostatistics, Institute for Health and Equity, and Cancer Center, Medical College of Wisconsin, Milwaukee, Wisconsin.
¹⁵ Division of Pulmonary, Allergy and Critical Care, Department of Medicine, Duke University Medical Center, Durham, North Carolina.
¹⁶ Division of Precision Medicine, New York University Grossman School of Medicine, New York, New York.
¹⁷ Department of Epidemiology, University of Washington, Seattle, Washington.

PMID: 37533140
PMCID: PMC10637465 (available on 2024-11-01)
DOI: 10.2215/CJN.0000000000000257

Abstract

Background: Sickle cell trait affects approximately 8% of Black individuals in the United States, along with many other individuals with ancestry from malaria-endemic regions worldwide. While traditionally considered a benign condition, recent evidence suggests that sickle cell trait is associated with lower eGFR and higher risk of kidney diseases, including kidney failure. The mechanisms underlying these associations remain poorly understood. We used proteomic profiling to gain insight into the pathobiology of sickle cell trait.

Methods: We measured proteomics ( N =1285 proteins assayed by Olink Explore) using baseline plasma samples from 592 Black participants with sickle cell trait and 1:1 age-matched Black participants without sickle cell trait from the prospective Women's Health Initiative cohort. Age-adjusted linear regression was used to assess the association between protein levels and sickle cell trait.

Results: In age-adjusted models, 35 proteins were significantly associated with sickle cell trait after correction for multiple testing. Several of the sickle cell trait-protein associations were replicated in Black participants from two independent cohorts (Atherosclerosis Risk in Communities study and Jackson Heart Study) assayed using an orthogonal aptamer-based proteomic platform (SomaScan). Many of the validated sickle cell trait-associated proteins are known biomarkers of kidney function or injury ( e.g. , hepatitis A virus cellular receptor 1 [HAVCR1]/kidney injury molecule-1 [KIM-1], uromodulin [UMOD], ephrins), related to red cell physiology or hemolysis (erythropoietin [EPO], heme oxygenase 1 [HMOX1], and α -hemoglobin stabilizing protein) and/or inflammation (fractalkine, C-C motif chemokine ligand 2/monocyte chemoattractant protein-1 [MCP-1], and urokinase plasminogen activator surface receptor [PLAUR]). A protein risk score constructed from the top sickle cell trait-associated biomarkers was associated with incident kidney failure among those with sickle cell trait during Women's Health Initiative follow-up (odds ratio, 1.32; 95% confidence interval, 1.10 to 1.58).

Conclusions: We identified and replicated the association of sickle cell trait with a number of plasma proteins related to hemolysis, kidney injury, and inflammation.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Biomarkers
Female
Hemolysis
Humans
Inflammation
Prospective Studies
Proteome
Proteomics
Renal Insufficiency*
Sickle Cell Trait*
United States

Substances

Proteome
Biomarkers

Abstract

Publication types

MeSH terms

Substances

Grants and funding