Advertisement

Welcome to the new AJNR, Updated Hall of Fame, and more. Read the full announcements.

AJNR is seeking candidates for the position of Associate Section Editor, AJNR Case Collection. Read the full announcement.

 

Research ArticleINTERVENTIONAL

Preprocedural C-Reactive Protein Levels Predict Stroke and Death in Patients Undergoing Carotid Stenting

K. Gröschel, U. Ernemann, J. Larsen, M. Knauth, F. Schmidt, J. Artschwager and A. Kastrup
American Journal of Neuroradiology October 2007, 28 (9) 1743-1746; DOI: https://doi.org/10.3174/ajnr.A0650

Abstract

BACKGROUND AND PURPOSE: Elevated baseline levels of C-reactive protein (CRP) are associated with an adverse outcome during coronary stent placement. The aim of this study was to evaluate whether preprocedural CRP levels also are predictive of stroke and death in patients undergoing carotid stent placement (CAS).

MATERIALS AND METHODS: We reviewed data prospectively collected from 130 patients (97 men, 33 women; mean age, 68.5 ± 10.1 years; range, 43–89 years) who underwent CAS for symptomatic carotid stenosis and from whom preprocedural CRP values had been obtained. A CRP value of >5 mg/L was considered to be elevated. The frequency of stroke and death within 30 days was compared between patients with and without elevated baseline CRP levels using χ2 and multivariate logistic regression analysis.

RESULTS: Baseline CRP values were normal in 94 (72.3%) patients but were elevated in 36 (27.7%) patients. The demographic and clinical characteristics were similar in both treatment groups. The 30-day stroke and death rate was significantly higher in patients with elevated CRP values (8/36; 22.2%) than in those without (3/94; 3.2%; P < .01). After adjusting for demographic characteristics, degree of carotid stenosis, and use of cerebral protection devices and/or statin therapy, an elevated CRP value before CAS remained a significant and independent predictor of stroke and death within 30 days after CAS (odds ratio, 7.7; 95% confidence interval: 1.8–32.8, P = .006).

CONCLUSIONS: Baseline CRP is a powerful predictor of outcome in patients undergoing CAS, which underscores the role of inflammation in the pathogenesis of embolic complications during this procedure.

During the past decade, increasing evidence has indicated that inflammation plays an important role in the initiation and progression of atherosclerotic disease involving both coronary and carotid arteries.1, 2 C-reactive protein (CRP), serum amyloid A protein, and fibrinogen are acute phase reactants that are synthesized in response to proinflammatory cytokines. Among these, CRP is the most common systemic marker of inflammation. In patients with substantial carotid artery narrowing, elevated CRP levels have been observed in those with recent cerebral ischemic symptoms,3 indicating that inflammation not only is part of the atherosclerotic process but also may indicate the clinical course. In support of this notion, serum CRP concentrations have recently been shown to be a marker for unstable carotid plaque.4 Because of the high risk of recurrent stroke in patients with a recently symptomatic carotid stenosis, several landmark studies have been performed to unequivocally demonstrate that carotid endarterectomy (CEA) effectively reduces this risk.5, 6 Along with CEA, carotid angioplasty and stent placement (CAS) is increasingly being used as a therapeutic alternative. Although several recent randomized trials and large, single-center studies have indicated that CAS can be performed with acceptable periprocedural complication rates,710 distal embolization of plaque fragments to the brain is one of the major limitations of this method and is probably associated with the plaque stability. Although a number of recent studies have demonstrated an association between baseline CRP values and adverse outcome during coronary stent placement,1114 little is known about the utility of this inflammatory marker for prediction of ischemic events in patients treated with CAS. Therefore, we sought to investigate whether elevated preprocedural CRP levels are associated with an increased risk of stroke or death within 30 days in patients undergoing CAS for symptomatic carotid stenosis.

Materials and Methods

Study Population

Prospectively collected data were reviewed for all patients with high-grade symptomatic carotid stenosis (≥70% assessed with sonography according to European Carotid Surgery Trial [ECST] criteria6); patients were treated with CAS at 2 university hospitals (Tübingen and Göttingen) between January 2000 and December 2005. A carotid stenosis was considered symptomatic if the patient had experienced an ipsilateral ocular or cerebral (permanent or transient) ischemic event within the past 6 months. All patients were informed of the investigative nature of CAS and gave their written consent. The Institutional Ethics Review Board of both universities approved the CAS protocol. The outcomes of patients treated at the university hospital of Tübingen and various subgroup analyses have been published previously.9, 15, 16

Carotid Stent Protocol

All patients were treated with carotid angioplasty with stent placement according to a standardized protocol recently described in detail.9 At first, all CAS procedures had been performed without cerebral protection devices. When cerebral protection devices became available, the choice of which type of device to use, if any, depended on the personal preference of the interventional neuroradiologist performing the procedure. At least 3 days before the procedure, patients received orally administered aspirin (100 mg daily) and clopidogrel (75 mg daily). Clopidogrel was continued for a 6-week period, and aspirin was given indefinitely. To document patency of the stent, all patients routinely received a sonography at the follow-up visit 1–2 days after CAS.

Data Collection and Clinical Evaluation

A stroke neurologist obtained the medical history of and performed neurologic examination on each patient before CAS. Additional neurologic examinations were performed the day after CAS and at day 30. The following cerebrovascular risk factors were recorded using history or direct measurements: hypertension (blood pressure ≥140/90 mmHg, based on the established World Health Organization criteria and measured on repeated occasions), diabetes mellitus (HbA1c >6.5%, fasting blood glucose >120 mg/dL, or presence of antidiabetic drugs), hyperlipidemia (fasting serum cholesterol levels >220 mg/dL or presence of lipid-lowering drugs), smoking (current or within the previous year), previous transient ischemic attacks and strokes, coronary artery disease (angina, myocardial infarction, percutaneous transluminal angioplasty, or surgery), and the presence of contralateral carotid disease (assessed with sonography). To exclude a current pulmonary or urinary tract infection, all patients received chest radiographs and a urinary analysis.

C-Reactive Protein Measurements

In both hospitals, peripheral blood samples were assayed within 24 hours before CAS with a routine test for CRP (Rolf Greiner BioChemica, Germany or Advia 1650 Chemistry System; Bayer Diagnostics, Germany). Both tests used an immunoprecipitation technique of serum CRP with photometric analysis. The elevated preprocedural CRP level was defined as >5 mg/L, the upper normal reference value in both laboratories.

Definitions of Clinical Outcome Measures

The clinical outcome measures were minor or major stroke or death within 30 days and were defined as follows17:

  • Minor Stroke. Any new neurologic deficit (either ocular or cerebral) that persisted for more than 24 hours and that either resolved completely within 30 days or increased the National Institutes of Health stroke scale score by ≤3 points.

  • Major Stroke. Any new neurologic deficit that persisted after 30 days or increased the National Institutes of Health stroke scale score by >3 points.

Statistical Analysis

Continuous values were expressed as mean ± SD and nominal variables as counts and percentages. For comparisons of categorical data, 2-tailed χ2 statistics with Yates correction and univariate Fisher exact test were used. The Fisher exact test was used when the predicted contingency table cell values were less than 5. Analyses of continuous variables between the cohorts were performed with an unpaired Student t test. A multiple logistic regression analysis was applied to assess the independent effect of preprocedural CRP values on postinterventional complication rates, whereas adjustment was performed for the potentially confounding effects of other baseline variables. Baseline variables were considered for inclusion in this analysis if they were imbalanced between both treatment groups, which were indicated by a P value of less than .2. Moreover, variables that were likely to influence the incidence of cardiovascular events (eg, the degree of carotid stenosis, the use of cerebral protection devices during CAS, the type of the stent, or the year in which the intervention was performed) were entered into this analysis. Interaction was assessed using additive and multiplicative interaction terms. Results of the logistic regression model are presented as odds ratio (OR) and 95% confidence interval (CI). A P value of less than .05 was considered to indicate a statistically significant difference. All statistical analyses were performed with SPSS (version 13; SPSS, Chicago, Ill).

Results

From January 2000 to December 2005, a total of 278 consecutive patients with a symptomatic carotid stenosis had been treated with CAS at both institutions. Of these patients, preprocedural CRP values had been obtained in 130 patients (97 men and 33 women; mean age, 68.5 ± 10.1 years; age range, 43–89 years) who comprised the study population for this analysis. The remaining 148 patients were excluded; of these, 18 patients either had confounding disease states (eg, such as inflammatory, neoplastic, or infectious diseases) or factors leading to elevated CRP levels (eg, treatment with steroids, immunosuppressive drugs, or nonsteroidal anti-inflammatory drugs, except for low-dose aspirin or clopidogrel), and 130 patients did not have CRP values. With respect to the baseline characteristics, there were no significant differences between the population of patients with available CRP values and those without (Table 1).

View this table:
Table 1:

Baseline characteristics of patients with and without available CRP values

Thirty-six (27.7%) patients had elevated CRP values before CAS. The demographic and clinical characteristics of patients with normal preprocedural CRP values and those with elevated CRP values before CAS were similar; however, there were more male patients in the group with elevated CRP values than in the group with normal CRP levels (Table 2). Hypertension and hyperlipidemia were the most frequent vascular risk factors in both groups, followed by cigarette smoking, diabetes mellitus, and coronary artery disease.

View this table:
Table 2:

Patient characteristics according to preprocedural CRP levels*

CAS was successful in all patients, and patency of the reconstructed artery was documented with a sonography follow-up study in each patient. Table 3 summarizes the postprocedural complication rates within 30 days. For the entire study population, the minor stroke rate was 7 of 130 (5.38%), the major stroke rate was 2 of 130 (1.54%), and the death rate was 2 of 130 (1.54%). All strokes were ipsilateral to the treated artery and occurred either during or within 24 hours after CAS.

View this table:
Table 3:

Periprocedural complications within 30 days after CAS according to preprocedural CRP levels

The incidence of stroke and death within 30 days was significantly different (P < .01) between patients with elevated preprocedural CRP values (22.2%) and those with normal CRP values (3.2%) (Table 3). In a multivariate logistic regression model, after adjusting for all the significant univariate predictors and for statin therapy, baseline CRP (OR, 7.7; 95% CI, 1.8–32.8, P = .006) and age >80 years (OR, 8.8; 95% CI, 1.7–44.9, P = .009) remained significant independent predictors of stroke and death after CAS.

Discussion

In this study, we analyzed the relationship between baseline CRP levels and cardiovascular complications after CAS in patients with a symptomatic carotid stenosis. Our results suggest that elevated preprocedural CRP levels are associated with an increased risk of stroke and death after CAS in these patients. To the best of our knowledge, a similar finding has not been reported before. Whereas several recent clinical studies have revealed an association between the extent of myocardial injury during percutaneous coronary interventions and baseline CRP values,1114 our study supports the notion preprocedural levels of acute-phase reactants also are clinically relevant predictors of outcome during carotid interventions. The relationship between elevated baseline CRP and ischemic complications during and after CAS was independent of other possible confounders, including concomitant statin therapy, which has been shown to reduce CRP levels.18

Because all ischemic adverse events occurred either during or within the first hours after CAS, it is likely that the poorer outcome among patients with a high CRP level is a consequence of a greater thrombotic hazard. At least indirectly, this assumption is supported by a recent observation of an increased microembolization during CAS in patients with high preprocedural leukocyte counts,19 which are subsequently significantly correlated with CRP.20

Several mechanisms could account for an increased risk of thrombotic events after CAS in patients with elevated preprocedural CRP levels. Ligand-bound or aggregated human CRP is a potent activator of the complement cascade, unleashing various proinflammatory mediators, which have been associated with direct damage of endothelial cells, enhancement of clotting by induction of tissue factor expression, and the formation of procoagulant microvesicles.21, 22 In addition, CRP may cause human monocytes to synthesize tissue factor, a potent procoagulant.23 Finally, CRP also contributes to endothelial dysfunction and induces expression of cell adhesion molecules.24 Thus, with respect to possible mechanisms linking CRP to thromboembolic complications during CAS, CRP may be related to pathologic substrates, such as the diffuseness of disease and friability of the atheromatous lesion that predispose to microembolization or to the propensity of clot formation at the site of angioplasty-induced arterial injury.

This study has strengths but also several important limitations. Although we used the data from our prospective CAS series, the potential influence of preprocedural CRP values on cardiovascular complications after CAS was analyzed in a retrospective fashion. Therefore, our results must be confirmed in further prospective trials. At first, CRP values had not been obtained systematically in all patients, and neither high-sensitivity CRP testing nor repeated or serial measurements were performed. Conversely, the combined 30-day stroke and death rates within our entire CAS series did not differ between patients with (8.5%) and without (8.1%; data not shown) CRP values, indicating that selection bias did not play a major role in our findings. Finally, although we tried to control for baseline imbalances between patients with normal CRP values and those with elevated CRP levels, the possibility of residual or undetected confounding variables cannot be ruled out completely.

In conclusion, elevated serum CRP levels are associated with a less favorable prognosis in patients with a symptomatic carotid stenosis who undergo CAS. Our results suggest that the measurement of CRP at baseline may help to identify those who are at an increased risk of adverse ischemic events. Although future prospective studies are warranted to corroborate this relationship, these patients may benefit from a treatment strategy aimed at attenuating the systemic inflammation.

References

  1. Hansson GK. Inflammation, atherosclerosis, and coronary artery disease. N Engl J Med 2005;352:1685–95
    CrossRefPubMed
  2. Schillinger M, Exner M, Mlekusch W, et al. Inflammation and Carotid Artery-Risk for Atherosclerosis Study (ICARAS). Circulation 2005;111:2203–09
    Abstract/FREE Full Text
  3. Rerkasem K, Shearman CP, Williams JA, et al. C-reactive protein is elevated in symptomatic compared with asymptomatic patients with carotid artery disease. Eur J Vasc Endovasc Surg 2002;23:505–09
    CrossRefPubMed
  4. Alvarez Garcia B, Ruiz C, Chacon P, et al. High-sensitivity C-reactive protein in high-grade carotid stenosis: risk marker for unstable carotid plaque. J Vasc Surg 2003;38:1018–24
    CrossRefPubMed
  5. Beneficial effect of carotid endarterectomy in symptomatic patients with high-grade carotid stenosis. North American Symptomatic Carotid Endarterectomy Trial Collaborators. N Engl J Med 1991;325:445–53
    CrossRefPubMed
  6. Randomised trial of endarterectomy for recently symptomatic carotid stenosis: final results of the MRC European Carotid Surgery Trial (ECST). Lancet 1998;351:1379–87
    CrossRefPubMed
  7. Ringleb PA, Allenberg J, Bruckmann H, et al. 30 day results from the SPACE trial of stent-protected angioplasty versus carotid endarterectomy in symptomatic patients: a randomised non-inferiority trial [published erratum appears in Lancet 2006;368:1238]. Lancet 2006;368:1239–47
    CrossRefPubMed
  8. Goodney PP, Schermerhorn ML, Powell RJ. Current status of carotid artery stenting. J Vasc Surg 2006;43:406–11
    CrossRefPubMed
  9. Kastrup A, Gröschel K, Schulz JB, et al. Clinical predictors of transient ischemic attack, stroke, or death within 30 days of carotid angioplasty and stenting. Stroke 2005;36:787–91
    Abstract/FREE Full Text
  10. Yadav JS, Wholey MH, Kuntz RE, et al. Protected carotid-artery stenting versus endarterectomy in high-risk patients. N Engl J Med 2004;351:1493–501
    CrossRefPubMed
  11. Buffon A, Liuzzo G, Biasucci LM, et al. Preprocedural serum levels of C-reactive protein predict early complications and late restenosis after coronary angioplasty. J Am Coll Cardiol 1999;34:1512–21
    CrossRefPubMed
  12. Chew DP, Bhatt DL, Robbins MA, et al. Incremental prognostic value of elevated baseline C-reactive protein among established markers of risk in percutaneous coronary intervention. Circulation 2001;104:992–97
    Abstract/FREE Full Text
  13. Dibra A, Mehilli J, Braun S, et al. Association between C-reactive protein levels and subsequent cardiac events among patients with stable angina treated with coronary artery stenting. Am J Med 2003;114:715–22
    CrossRefPubMed
  14. Goldberg A, Gruberg L, Roguin A, et al. Preprocedural C-reactive protein levels predict myocardial necrosis after successful coronary stenting in patients with stable angina. Am Heart J 2006;151:1265–70
    CrossRefPubMed
  15. Gröschel K, Ernemann U, Schulz JB, et al. Statin therapy at carotid angioplasty and stent placement: effect on procedure-related stroke, myocardial infarction, and death. Radiology 2006;240:145–51
    CrossRefPubMed
  16. Kastrup A, Schulz JB, Raygrotzki S, et al. Comparison of angioplasty and stenting with cerebral protection versus endarterectomy for treatment of internal carotid artery stenosis in elderly patients. J Vasc Surg 2004;40:945–51
    CrossRefPubMed
  17. Mathur A, Roubin GS, Iyer SS, et al. Predictors of stroke complicating carotid artery stenting. Circulation 1998;97:1239–45
    Abstract/FREE Full Text
  18. Jialal I, Stein D, Balis D, et al. Effect of hydroxymethyl glutaryl coenzyme a reductase inhibitor therapy on high sensitive C-reactive protein levels. Circulation 2001;103:1933–35
    Abstract/FREE Full Text
  19. Aronow HD, Shishehbor M, Davis DA, et al. Leukocyte count predicts microembolic Doppler signals during carotid stenting: a link between inflammation and embolization. Stroke 2005;36:1910–14
    Abstract/FREE Full Text
  20. Danesh J, Whincup P, Walker M, et al. Low grade inflammation and coronary heart disease: prospective study and updated meta-analyses. BMJ 2000;321:199–204
    Abstract/FREE Full Text
  21. Lagrand WK, Visser CA, Hermens WT, et al. C-reactive protein as a cardiovascular risk factor: more than an epiphenomenon? Circulation 1999;100:96–102
    Abstract/FREE Full Text
  22. Mortensen RF. C-reactive protein, inflammation, and innate immunity. Immunol Res 2001;24:163–76
    CrossRefPubMed
  23. Cermak J, Key NS, Bach RR, et al. C-reactive protein induces human peripheral blood monocytes to synthesize tissue factor. Blood 1993;82:513–20
    Abstract/FREE Full Text
  24. Pasceri V, Willerson JT, Yeh ET. Direct proinflammatory effect of C-reactive protein on human endothelial cells. Circulation 2000;102:2165–68
    Abstract/FREE Full Text
  • Received January 5, 2007.
  • Accepted after revision February 15, 2007.
View Abstract
Back to top

In this issue

Advertisement
Print
Download PDF
Email Article
Cite this article
0 Responses
Respond to this article
Bookmark this article
Preprocedural C-Reactive Protein Levels Predict Stroke and Death in Patients Undergoing Carotid Stenting
K. Gröschel, U. Ernemann, J. Larsen, M. Knauth, F. Schmidt, J. Artschwager, A. Kastrup
American Journal of Neuroradiology Oct 2007, 28 (9) 1743-1746; DOI: 10.3174/ajnr.A0650
del.icio.us logo Twitter logo Facebook logo Mendeley logo
Purchase

Jump to section

Related Articles

  • No related articles found.

Cited By...

More in this TOC Section

Similar Articles

Advertisement