Volume 13, Issue 6 (November & December 2022)                   BCN 2022, 13(6): 807-814 | Back to browse issues page


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Safari A, Fadakar N, Borhani-Haghighi A. The Association Between Inflammatory Biomarkers and Vitamin D Level With the Evolution and Severity of Stroke. BCN 2022; 13 (6) :807-814
URL: http://bcn.iums.ac.ir/article-1-1577-en.html
1- Stem Cells Technology Research Center, Shiraz University of Medical Sciences, Shiraz, Iran.
2- Clinical Neurology Research Center, Shiraz University of Medical Sciences, Shiraz, Iran.
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1. Introduction
Stroke is among the most common causes of mortality and morbidity globally (Borhani-Haghighi et al., 2013); however, our armamentarium for its treatment is limited (Shahtaheri, et al., 2012). Numerous pieces of evidence have revealed the crucial role of inflammation in the pathogenesis of acute ischemic stroke. Hence, inflammatory biomarkers might predict the functional outcome of the stroke (Safari, et al., 2016).
C-reactive protein (CRP) or Pentraxin1(Ptx1), is made by liver cells in response to interleukin-1 (IL-1), IL-6, and tumor necrotic factor-alpha (TNF-α). High-sensitivity CRP (hsCRP) picks up even low CRP (Mohebbi et al., 2012).
Serum amyloid A (SAA) is also an acute-phase reactant that increases within hours after an inflammatory reaction starts. Some studies have suggested the superiority of SAA over erythrocyte sedimentation rate (ESR) and CRP in quantifying inflammatory reactions (Cunnane et al., 2000).
Osteopontin (OPN) is a secreted extracellular phosphoprotein, which plays a pivotal role in the normal mineralization of bone as well as up-regulating calcified plaques of the vessels. In addition, OPN has immunomodulatory activities via chemotaxis, cell attachment, cytokine production, and anti-apoptosis mechanism (Wang & Denhardt, 2008).
Low 25-hydroxyvitamin D (25-OH vitamin D) levels have been reported to be associated with obesity, diabetes mellitus (DM), dyslipidemia, and hypertension, which are the major risk factors in ischemic stroke (Muscogiuri et al., 2017).
Even though there is increasing evidence regarding the association between vitamin D deficiency and an increased risk of stroke “evolution” (Zhou et al., 2018), the association between vitamin D level and the severity of the stroke and its inflammatory aspects is still unclear. The severity of stroke is assessed by both clinical measures, such as the National Institutes of Health Stroke Scale (NIHSS), and radiologic measures, like the Alberta Stroke Program Early CT Score (ASPECTS), the two available criteria for assessing stroke severity.
There are a few studies that have investigated the association between NIHSS as a stroke severity measure and vitamin D level at the time of admission (Daubail et al., 2013; Park et al., 2015; Tu, Zhao, Xu, & Chen, 2014; Wang, Ji, Tong, & Zhang, 2014; Wei & Kuang, 2018; Zhang, Wang, Zhong, Liao, & Lu, 2018). However, to the best of our knowledge, no study has investigated the association between radiological severity scales, such as ASPECTS, and vitamin D levels. In addition, the acute phase reactants were not analyzed in the aforementioned studies.
We compared serum 25-OH vitamin D (vitamin D), hsCRP, SAA, and osteopontin levels between patients with middle cerebral artery (MCA) infarction and age- gender-matched normal individuals. We also investigated the association between stroke severity according to the NIHSS and the ASPECTS, vitamin D levels, and inflammatory biomarkers. We hypothesized that vitamin D deficiency might induce a larger infarct area according to ASPECTS through modulation of immunologic factors, such as hsCRP, SAA, and osteopontin. 

2. Materials and Methods
This is a prospective cross-sectional study conducted in Namazi hospital, a high-volume center for stroke in southwestern Iran, affiliated with the Shiraz University of Medical Sciences from June 2017 to March 2018. 

Inclusion criteria
Patients with first-ever acute ischemic stroke in the middle cerebral artery (MCA) territory within seven days before recruitment were enrolled. According to the Recognition of Stroke in the Emergency Room (ROSIER) scale (Nor et al., 2005), ischemic stroke was defined as an acute focal neurological deficit, presented for at least 24 hours, and confirmed by a brain CT or an MRI. Other inclusion criteria were the age of more than 18 years and providing written informed consent.

The exclusion criteria
Patients with primary intracranial hemorrhage were excluded. Patients with recurrent ischemic stroke and ischemic stroke that lasted more than seven days were also not included. 
Patients with lacunar stroke [Causative Classification System for Ischemic Stroke (CSS type III)] (Ay et al., 2005) were also excluded.
Patients with cervico-cephalic arterial dissection, vasculitides, cerebral venous sinus thrombosis, hypoperfusion syndromes, iatrogenic stroke, vasospasm after subarachnoid hemorrhage, meningitis, hematologic causes of stroke, Moyamoya disease, and reversible vasoconstriction syndrome were also excluded.
Conditions that could affect vitamin D, hsCRP, SAA, and osteopontin levels, such as atrial fibrillation (Cheng, et al., 2012; Thompson, et al., 2015), fever or any other sign of infection, any previously proven neoplastic (Garland et al., 2006; Moshkovskii, 2012), rheumatologic or inflammatory diseases (Hwang et al., 2016), renal failure (Dieter et al., 2016; Tonelli, et al., 2005), acute or chronic liver failure (Maury, Teppo, & Salaspuro, 1983), respiratory failure (Bozinovski et al., 2008), recent surgery (Habib, et al., 2009), thyroid (Reza,et al., 2013), and parathyroid diseases (Maser, et al., 2018), Alzheimer’s disease (Chung et al., 2000), Parkinson’s disease and any history of osteoporosis (Abdu-Allah, et al., 2015) or its related risk factors were also excluded. Patients with excessive alcohol intake were not recruited as well (Hillborn, 1998).
Patients who received vitamin D or calcium supplements, anticoagulants, glucocorticoids, other anti-inflammatory drugs, calcitonin, parathyroid hormone, and osteoporosis-related medications were also excluded.

Control group
The control group included age-and-gender-matched individuals with neither any history of ischemic stroke/ transient ischemic attack (TIA) nor any of the above-mentioned exclusion criteria.

Sample size and variables
The sample size was calculated based on α=0.05, β=0.80, and the effect size of 0.6 by G Power Software. Body mass index (BMI) was measured in the case and control groups. Major cerebrovascular risk factors, including current or previous cigarette smoking habits, hypertension, diabetes mellitus (DM), dyslipidemia, and a history of ischemic heart disease (IHD), were investigated for all participants. 

Laboratory investigations
Ten cc blood was obtained from patients 2-7 days after the stroke, and from the controls. The sera were banked at -80°C and then defrosted. Calcium, phosphor, alkaline phosphatase (ALP), fasting blood sugar (FBS), blood urea nitrogen (BUN), and creatinine (Cr) were measured by standard techniques. 25-OH vitamin D was quantified by the enzyme-linked immunosorbent assay (ELISA) method. The details were mentioned in our previous publication (Safari et al., 2019)

Study ethics
The study was approved by the ethics committee of Shiraz University of Medical Sciences (No#1396-S104). Written informed consent was taken from both patients and controls. If the patients were confused or unconscious, consent was taken from their next of kin.

Statistical analysis
Statistical analyses were conducted using SPSS version 20. For variables with a normal distribution, the results were presented with a mean and 95% confidence interval (CI). The Chi-square test and independent t-test were used to test the differences. The logistic regression model was utilized to determine the effects of hypertension, DM, smoking, IHD, serum levels of hsCRP, SAA, osteopontin, and vitamin D on stroke evolution. Pearson correlation coefficient was used to find the association between stroke severity scales (NIHSS and ASPECT) and serum concentration of biomarkers (hsCRP, SAA, osteopontin, and vitamin D). The significance level of 0.05 was deemed appropriate.

3. Results
Eighty-nine patients with acute ischemic stroke were initially recruited. After applying all the inclusion and exclusion criteria, 46 patients with the first-ever attack of MCA infarction were selected. The 46 age-and-gender-matched healthy subjects were recruited as the control population. Table 1 shows demographic variables, stroke risk factors, calcium, vitamin D level, hsCRP, SAA, and osteopontin levels.

On evaluating the risk factors and serum biomarkers with stroke evolution, univariate analysis revealed the association of DM, hypertension, smoking, and the history of IHD, in addition to higher SAA, higher hsCRP, and lower vitamin D levels with the evolution of stroke (Table 2). 

In stroke patients, significant reverse associations between vitamin D and SAA levels (R= -0.241, P=0.025), and vitamin D and hsCRP levels (R= -0.267, P=0.011) were detected. However, there was no significant association between vitamin D and serum osteopontin levels (R=0.051, P=0.642).
In stroke patients, the mean and 95% CI of admission NIHSS score were 12.97 and 10.65-15.35, respectively. In addition, the mean and 95% CI of their ASPECT score were 6.24 and 5.57-6.83, respectively. 
There was a significant reverse association between NIHSS score and vitamin D level (R= -0.306, P=0.043). Meanwhile, a significant association between NIHSS score and hsCRP (R=0.482, P=0.001), as well as SAA levels (R=0.315, P=0.04) were found. However, the reverse association between NIHSS score and osteopontin level was not significant (R= -0.091, P=0.56). 
When stroke severity was evaluated according to ASPECT, there was a significant reverse association between ASPECT score and hsCRP and SAA levels (R= -0.401, P=0.007 and R= -0.361, P=0.017). However, no significant association between ASPECT score and vitamin D and osteopontin levels (R=0.221 and - 0.071, P=0.149 and 0.651) was seen.

4. Discussion
The current study showed the association of hypertension, DM, smoking, history of ischemic heart disease, higher SAA, higher hsCRP, and lower vitamin D levels with stroke evolution in a case-controlled study. Meanwhile, in stroke patients, its severity was associated with higher SAA, higher hsCRP, and lower vitamin D according to the clinical scale (higher admission NIHSS). According to the ASPECT score, higher SAA and hsCRP, but not lower vitamin D levels, were associated with more infarct areas. NIHSS and ASPECT scores were not significantly associated with osteopontin levels.
Our results are consistent with previous studies, which showed the association between vitamin D deficiency and stroke evolution (Zhang et al., 2017). The anti-calcific protective effect of vitamin D in the process of atherogenesis might prevent the evolution of atherothrombotic ischemic stroke (Mozos & Marginean, 2015).
Meanwhile, vitamin D deficiency was associated with higher NIHSS in all (Afshari, Amani, Soltani, Haghighizadeh, & Afsharmanesh, 2015; Daubail et al., 2013; Park et al., 2015; Tu et al., 2014; Wang et al., 2014), as well as subgroups of acute ischemic stroke patients (Zhou et al., 2018). The anti-inflammatory effect of vitamin D might play a role in stroke severity. There are both animal and human studies supporting this hypothesis. Balden et al. showed larger infarct volumes and more severe behavioral disturbances in rats fed with a vitamin D-deficient diet compared to controls. They hypothesized the activation of inflammatory markers and suppression of inherent neuroprotective agents, such as Insulin-growth factor-1. Interestingly, vitamin D injection in the acute stage did not improve infarct volume or behavioral disturbance (Balden, Selvamani, & Sohrabji, 2012). Wang et al. stated that serum vitamin D levels were adversely associated with serum levels of IL‐6 and hsCRP in stroke patients (Wang, et al., 2018) . 
As far as we know, few studies have studied the link between ASPECT score with vitamin D levels, hsCRP, SAA, and osteopontin. The current study failed to show the association between ASPECT score and vitamin D or osteopontin levels. However, it revealed a significant association between lower ASPECT scores (i.e. larger infarct areas) and higher levels of hsCRP and SAA.
The fundamental limitation of the current study was the small sample size. We deleted all the confounding factors affecting vitamin D, hsCRP, SAA, and osteopontin levels to increase the reliability of the results. Finding a pure group of MCA infarction with the exclusion of all confounding factors was the primary obstacle. 
In conclusion, the present study showed vitamin D’s speculative role in both the evolution and severity of stroke. The protective effects of vitamin D might be due to its immune-modulatory activities. More extensive studies are warranted to investigate the benefits of vitamin D supplementation in preventing and treating stroke patients.

Ethical Considerations
Compliance with ethical guidelines

The study was approved by the ethics committee of Shiraz University of Medical Sciences (No.: #1396-S104). Written informed consent was taken from both patients and controls. If the patients were confused or unconscious, consent was taken from their next of kin.

Funding
This study is in partial fulfillment of the thesis project for the specialty of neurology degree by Dr. Nima Fadakar. This study is financially supported by the Office of Vice Chancellor for Research of Shiraz University of Medical Sciences (Grant No.: #13990). 

Authors' contributions
All authors equally contributed to preparing this article.

Conflict of interest
The authors declare no conflict of interest.

Acknowledgments
We thank Heydari and Neydavoodi for statistical analysis; Zafarmnad for data collection; and H. Argasi at the Research Consultation Center (RCC) of Shiraz University of Medical Sciences for literal editing.


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Type of Study: Original | Subject: Clinical Neuroscience
Received: 2019/08/6 | Accepted: 2020/02/10 | Published: 2022/11/1

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