Human cytomegalovirus-IgM seropositivity is not associated with atherogenic alterations of lipid profiles and inflammatory status in ischemic stroke patients: a preliminary study

Background: Past exposure to human cytomegalovirus has been suggested to participate in the pathogenetic events associated with atherosclerotic lesion establishment and progression. However, whether ongoing human cytomegalovirus infection is related to plaque instability, and subsequent acute cerebr...

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Published in:Neurological research (New York) 2011-06, Vol.33 (5), p.473-481
Main Authors: Liu, Lei, Tuo, Hou-Zhen, Wang, Rui-Jin, Yi, Li, Wang, Jia-Wei, Wang, De-Xin
Format: Article
Language:English
Subjects:
Acute ischemic stroke
Adult
Aged
Aged, 80 and over
Antibodies, Viral - biosynthesis
Brain Ischemia - epidemiology
Brain Ischemia - pathology
Brain Ischemia - virology
Cohort Studies
Comorbidity
Cytomegalovirus
Cytomegalovirus Infections - blood
Cytomegalovirus Infections - epidemiology
Cytomegalovirus Infections - pathology
Female
High-sensitivity C-reactive protein
Human cytomegalovirus
Human cytomegalovirus-IgM
Humans
Hyperlipidemias - epidemiology
Hyperlipidemias - pathology
Hyperlipidemias - virology
Immunoglobulin M - blood
Inflammation - immunology
Inflammation - pathology
Inflammation - virology
Intracranial Arteriosclerosis - epidemiology
Intracranial Arteriosclerosis - pathology
Intracranial Arteriosclerosis - virology
Male
Metabolic disorders
Middle Aged
Pilot Projects
Plaque instability
Stroke - epidemiology
Stroke - pathology
Stroke - virology
Vasculitis, Central Nervous System - epidemiology
Vasculitis, Central Nervous System - pathology
Vasculitis, Central Nervous System - virology
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Summary:Background: Past exposure to human cytomegalovirus has been suggested to participate in the pathogenetic events associated with atherosclerotic lesion establishment and progression. However, whether ongoing human cytomegalovirus infection is related to plaque instability, and subsequent acute cerebral ischemia, is relatively unknown. The purpose of this study was to evaluate the potential relationships between active human cytomegalovirus infection and ischemic stroke, especially in regard to metabolism and inflammation. Methods: Ninety-nine acute ischemic stroke patients, associated with large artery atherosclerosis, were divided into two groups based on the presence or absence of human cytomegalovirus immunoglobulin M (IgM) (human cytomegalovirus-IgM-positive/human cytomegalovirus-IgM-negative = 33:66). Baseline clinical characteristics, inflammatory factors, and biochemical assessments were compared in both groups. Then, all patients and human cytomegalovirus-IgM-positive patients were divided into quartiles according to their high-sensitivity C-reactive protein levels, respectively, and risk factors were compared. Finally, correlations between inflammatory factors (high-sensitivity C-reactive protein and white blood cell count) and other atherosclerosis risk factors in both human cytomegalovirus-IgM-positive and -negative subjects were evaluated. Results: An association between human cytomegalovirus-IgM seropositivity and atherogenic modification of metabolism and inflammatory status were not found in this study. Both age and white blood cell count increased across quartiles of high-sensitivity C-reactive protein in all subjects (P = 0·001), while age and low-density lipoprotein cholesterol increased across quartiles of high-sensitivity C-reactive protein in the human cytomegalovirus-IgM-positive group (P = 0·02 and 0·007, respectively). Multivariate linear regression analysis showed that high-sensitivity C-reactive protein was associated with age in human cytomegalovirus-IgM-positive group (P = 0·002), while no other factor was associated with white blood cell count in these subjects. Conclusion: Our study provided no evidence for the direct implication of active systemic human cytomegalovirus infection, represented by human cytomegalovirus-IgM positivity, in the pathogenesis of acute ischemic strokes, particularly those involving plaque instability and metabolic disorders.
ISSN:0161-6412
1743-1328
DOI:10.1179/016164111X13007856084007