A team of researchers at the Medical University of South Carolina (MUSC) report in Frontiers in Immunology that they have identified a type of fat known as a sphingolipid that could predict the severity of heart disease in African American patients with lupus.
The team was led by Samar M. Hammad, Ph.D., associate professor in the MUSC College of Medicine, and the study was funded in part by a pilot project grant from the South Carolina Clinical & Translational Research Institute.
“The most exciting finding of this study is that we may be able to find another way to better diagnose and eventually treat the African American lupus patients who are at increased risk of developing heart disease,” said Hammad.
Systemic lupus erythematosus (SLE), or lupus, is a chronic autoimmune disease that can affect many different organs in the body. Our immune system typically acts like our personal bodyguard. When it senses danger from a virus or infection, it attacks and eliminates the threat. In patients with SLE, the “bodyguard” attacks and damages the person’s own cells, mistaking them as foreign invaders. As a result, patients with SLE can develop complications, such as cardiovascular disease (CVD).
Cholesterol, a type of fat circulating in our blood, is carried on lipid particles called high-density lipoproteins (HDL, the good cholesterol carrier) and low-density lipoprotein (LDL, the bad cholesterol carrier) and typically used to screen for CVD. High levels of LDL cholesterol are commonly used to predict a patient’s risk for developing heart disease because this fat accumulates in the walls of blood vessels.
Despite being at an increased risk of CVD, healthy African Americans have a lipid profile with higher HDL (good) cholesterol and lower triglyceride levels compared with healthy persons of European ancestry. Therefore, the efficacy of the standard screening method for CVD has been called into question for African American patients. Further, approximately 90% of lupus patients are females, and African American women are three times more likely than white women to develop severe symptoms associated with SLE. Thus, the standard screening panels, developed with the white patient in mind, lack efficacy for the African American patient. With the standard method of screening for CVD potentially being unreliable for African American SLE patients, additional biomarkers are needed to improve health outcomes in this group.
Sphingolipids are molecules carried in the blood on lipoproteins. They are important structural components of cells, can act as key signaling molecules and, when disrupted, are associated with several diseases. Recently, serum sphingolipids have been shown to be potential biomarkers for clinical lupus complications.
Notably, the Hammad lab previously found that the sphingolipid profile of healthy African Americans differs from that of healthy whites. They also observed differences in the sphingolipid profiles of African American lupus patients with or without heart disease.
“Treatments for SLE and heart disease are often given as a one-size-fits-all, and they can have major side effects for the patient,” said Hammad.
The purpose of this study was to determine whether sphingolipids are predictive biomarkers for preclinical CVD and CVD severity in African American patients with SLE. At study start (visit 1) and after one year (visit 2), the researchers measured levels of five different sphingolipid classes, with several sphingolipid species in each class, in plasma samples of 51 patients with SLE but without a history of clinical heart disease.
Hammad and her lab established a methodology for profiling sphingolipids in human plasma in 2010 that is now widely used in sphingolipid studies. Using this method, Hammad and her team found that a particular class of sphingolipid in the plasma samples, called lactosylceramide (Lac-Cer), was positively correlated with the change in plaque area over one year. Plaques are clumps of cholesterol found at injury sites of walls of major arteries. Thus, higher levels of Lac-Cer are associated with increased disease activity in African American patients with SLE.
“This finding showed us that the Lac-Cer levels in the circulation could have predictive value for a patient,” explained Hammad. “We could use this as a readout for how a patient is progressing while on medication and get a good indication of his or her heart disease.”
High LDL cholesterol content in the serum is typically used to determine the risk of developing heart disease. The study found no correlation between LDL concentrations and the concentrations of the measured Lac-Cer species, indicating that the traditional biomarker for heart disease was ineffective in predicting disease severity in the African American lupus population.
Ultimately, Hammad believes that studies like these emphasize the need for teamwork between basic scientists and clinicians.
“I’m a basic scientist who has almost 20 years of experience in investigating the role of sphingolipids in health and disease,” said Hammad. “This study was possible, thanks to the organized and well thought out collection and banking of patient samples from the clinical side, led by Dr. Jim Oates, division director of Rheumatology and Immunology.”
Future objectives of the team will include determining whether their findings can be applied to the general population.
“Using sphingolipids as a tool to complement other diagnostic modalities will be important because SLE is often hard to diagnose,” said Hammad. “I think sphingolipids can play a major role in the diagnosis, prognosis and treatment of lupus.”
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About MUSC
Founded in 1824 in Charleston, MUSC is home to the oldest medical school in the South as well as the state’s only integrated academic health sciences center, with a unique charge to serve the state through education, research and patient care. Each year, MUSC educates and trains more than 3,000 students and nearly 800 residents in six colleges: Dental Medicine, Graduate Studies, Health Professions, Medicine, Nursing and Pharmacy. MUSC brought in more than $271 million in biomedical research funds in fiscal year 2020, continuing to lead the state in obtaining National Institutes of Health funding, with more than $129.9 million. For information on academic programs, visit musc.edu.
As the clinical health system of the Medical University of South Carolina, MUSC Health is dedicated to delivering the highest quality patient care available while training generations of competent, compassionate health care providers to serve the people of South Carolina and beyond. Comprising some 1,600 beds, more than 100 outreach sites, the MUSC College of Medicine, the physicians' practice plan and nearly 275 telehealth locations, MUSC Health owns and operates eight hospitals situated in Charleston, Chester, Florence, Lancaster and Marion counties. In 2020, for the sixth consecutive year, U.S. News & World Report named MUSC Health the No. 1 hospital in South Carolina. To learn more about clinical patient services, visit muschealth.org.
MUSC and its affiliates have collective annual budgets of $3.2 billion. The more than 17,000 MUSC team members include world-class faculty, physicians, specialty providers and scientists who deliver groundbreaking education, research, technology and patient care.
About the SCTR Institute
The South Carolina Clinical & Translational Research (SCTR) Institute is the catalyst for changing the culture of biomedical research, facilitating the sharing of resources and expertise and streamlining research-related processes to bring about large-scale change in clinical and translational research efforts in South Carolina. Our vision is to improve health outcomes and quality of life for the population through discoveries translated into evidence-based practice. To learn more, visit https://research.musc.edu/resources/sctr.
Journal
Frontiers in Immunology
Method of Research
Observational study
Subject of Research
People
Article Title
Plasma Sphingolipid Profile Associated With Subclinical Atherosclerosis and Clinical Disease Markers of Systemic Lupus Erythematosus: Potential Predictive Value
Article Publication Date
21-Jul-2021
COI Statement
The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.