Effects of statins-use for patients with aneurysmal subarachnoid hemorrhage: a meta-analysis of randomized controlled trials.

Aneurysmal subarachnoid hemorrhage (aSAH)-induced cerebral vasospasm and delayed ischemic neurological deficit (DIND) are the major causes of morbidity and mortality in patients with aSAH. The effects of statins-use for patients with aSAH remain controversial. Here,a total of 249 patients from six randomized controlled trials(RCTs) were subjected to meta-analysis. No significant decrease was found in the incidence of vasospasm(RR, 0.80; 95% CI, 0.54-1.17), with substantial heterogeneity (I(2) = 49%, P = 0.08), which was verified by the further sensitivity analysis and subgroup meta-analysis. Furthermore, no significant difference was presented in the incidence of poor neurological outcome(RR, 0.94; 95% CI, 0.77-1.16), and potential side effects(RR, 2.49; 95% CI, 0.75-8.33). Nevertheless, significant difference was reported in the occurrence of DIND(RR, 0.58; 95% CI, 0.37-0.92) and mortality(RR, 0.30; 95% CI, 0.14-0.64). At present, although statins-use in the patients with aSAH should not be considered standard care at present, statins-use may have the potential effects in the prevention of mortality in patients with aSAH.

Aneurysmal subarachnoid hemorrhage (aSAH)-induced cerebral vasospasm and delayed ischemic neurological deficit (DIND), especially those associated with arterial vasospasm, remain the major causes of morbidity and mortality in patients with aSAH1. Although treatment with nimodipine confirms the effect of improving outcomes after subarachnoid hemorrhage (SAH), its benefit is modest and the mechanism is uncertain234. Recently, there has been growing interest in the use of 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitors (statins), which has been demonstrated to raise cerebral endothelial nitric oxide synthase expression, improve endothelial function, increase cerebral blood flow and protect against ischemia56. In some clinical studies, statins-use could reduce vasospasm, DIND, and mortality78910. Conversely, negative effects of statins-use were presented in other studies111213141516.

Due to only 5% stroke caused by aSAH17 and a proportion of death in patients with aSAH before admission in hospital, the prospective, multicenter and large sample size randomized controlled trials (RCT) regarding statins-use seems too difficult to complete. Hence, the meta-analysis would be the available methodology to speculate the identified effects of statins-use for patients with aSAH. To our knowledge, four meta-analyses with regards to this aspect had been published previously18192021. Nevertheless, different viewpoints were raised in the four studies. The effects of statins-use for patients with aSAH still remain controversial and no recommendation was presented in the guideline122. In previous meta-analyses, different clinical studies (prospective or retrospective) might enhance the methodological heterogeneity. Besides, a new RCT of simvastatin-use for patients with aSAH has been published16. A further meta-analysis which only included RCTs might be some interesting to explore the effects of statins-use for patients with aSAH. In addition, the potential side effects of statins-use would be investigated in our study.

Results

Study Identification and Selection

The combined search strategy identified 89 papers. After title, abstract, and full text screening, five RCTs met our inclusion criteria. An additional RCT was identified by hand searching. Thus, eventually six RCTs were included in the present meta-analysis. Unfortunately, we did not receive any missing analytical data for meta-analysis from the corresponding authors of the included studies. The selection process is shown in Figure 1.

Figure 1

Selection process for RCTs.

RCTs: randomized controlled trials.

Study Characteristics

Characteristics of patients with aSAH are presented in Table 1. The six RCTs were all small sample size and single-center studies, enrolling a total of 249 patients7814151623. Most of patients were female. One RCT has been published as abstract23. One RCT reported the population descent7. Hunt-Hess and WFNS grades were described in four RCTs8141516. 44 (23%) of 189 patients' initial status was comatose (WFNS or Hunt-Hess grade > IV). Fisher grade was confirmed in three RCTs71623. 10 (10%) of 98 patients were in Fisher grade IV. Management of culprit aneurysms was mentioned in five RCTs78141516. 147(64%) of 228 patients underwent microsurgical clipping. Five studies administered simvastatin at a dose of 80 mg/d within 96 hours for 14–21 days, while one study used pravastatin at a dose of 40 mg/d within 72 hours for 14 days.

Table 1

Characteristics of patients with aSAH in the six RCTs

Study ID	Design	Category of statins	Number of patients (S/P)	Patients age (years)	Female	Hunt- Hess or WFNS grade > IV	Fisher scale > IV	Clipping for aSAH	Dose of statins	Initial time and duration of statins treatment	Definiton of vasospasm	Definiton of DIND	Outcome evaluation	Definiton of potential side effects
Lynch 2005	RCT	simvastatin	19/20	56 ± 15	85%(33/39)	—	5%(2/39)	44%(17/39)	80mg/d	within 48h/14 days	TCD VMCA > 160 cm/sec	clinical manifestation and TCD VMCA > 160 cm/sec or angiography	—	ALT/AST or CK/CPK > 3-fold times the normal (>180 U/L,>1000 U/L respectively)
Chou 2008	RCT	simvastatin	19/20	53 ± 13	74%(29/39)	23%(9/39)	—	85%(33/39)	80mg/d	within 96h/21 days	TCD VMCA(peak systolic velocity) > 200 cm/sec and a Lindegaard ratio > 3 or angiography	unaccountable new focal neurological deficit lasting ≥2 hours or GCS↓≥2 points	MRS at discharge	ALT/AST or CPK > 3-fold times the normal (>180 U/L,>1000 U/L respectively)
Macedo 2009	RCT (no blind)	simvastatin	11/10	—	—	—	38%(8/21)	—	80mg/d	within 72h/21 days	cerebral arteriography examination	Changes in clinical status and CT scan or angiography	GOS at discharge	ALT/AST > 3-fold times the normal (>180 U/L) or creatinine ≥2.5 or total CK ≥1000 U/l
Vergouwen 2009	RCT	simvastatin	16/16	54 ± 11	63%(20/32)	25% (8/32)	—	22%(7/32)	80mg/d	within 72h/14 days	TCD VMCA/ACA ≥120 cm/sec	Focal cerebral deficit OR GCS↓≥2 points	GOS at 6 month	ALT/AST > 3-fold times the normal (>180 U/L)
Grag 2013	RCT	simvastatin	19/19	49 ± 9	45%(17/38)	3% (1/38)	0%(0/38)	100%(38/38)	80mg/d	within 96h/14 days	TCD VMCA > 160 cm/sec or angiography	New ischemic neurologic deficits in first two weeks after the ictus(not attributable to be due to hydrocephalus, clip-induced infarct, metabolic derangement, infection or rebleed)	GOS, MRS and MBI at 6 month	ALT/AST or CPK > 3-fold times the normal (>180 U/L,>1000 U/L respectively)
Tseng 2005	RCT	pravastatin	40/40	53 ± 12	55%(44/80)	33% (26/80)	—	65%(52/80)	40mg/d	Within 72h/14 days	TCD VMCA > 120 cm/sec with Lindegaard ratio > 3	focal neurological deficits or GCS↓≥2 points	MRS at discharge	—

aSAH: aneurysmal subarachnoid hemorrhage; RCTs: randomized controlled trials; TCD: transcranial doppler; MCA: middle cerebral artery; ACA: anterior cerebral artery; DIND: delayed ischemic neurological deficit; GCS: glasgow coma scale; MRS: modified rankin scale; GOS: glasgow outcome scale; MBI: modified barthel index; ALT: alanine aminotransferase; AST: aspartate aminotransferase; CK: creatine kinase; CPK: creatine phosphokinase

Three studies used TCD cerebral artery velocity as the detected methodology for vasospasm7815, while the other three required TCD cerebral artery velocity or cerebral arteriographic evidence of vasospasm141623. Definition for DIND also varied. Clinical symptoms, TCD and angiographic results were confirmed as DIND in two RCTs723. However, new ischemic neurologic deficits or Glasgow Coma Scale (GCS) were performed as the criteria of DIND in the other RCTs8141516. GOS and MRS were presented in five RCTs814151623. The timing of outcome assessment varied from as early as hospital discharge81423 to as late as 6 months1516. Potential side effects were demonstrated in four RCTs7141516, the definition of that was consistent in the studies.

The quality of the included RCTs was assessed by Cochrane risk of bias assessment. If no specific descriptions were found in the trials, we tended to choose the answer of unclear risk. However, the results only reflected our viewpoint (Figure 2).

Figure 2

Quality of the included RCTs assessed by Cochrane risk of bias assessment.

If no specific descriptions were found in the trials, we tended to choose the answer of unclear risk. RCTs: randomized controlled trials.

Meta-analysis Outcomes

All the pooled results are shown in Figure 3. The incidence of vasospasm was 41% (51/124) and 54% (68/125) in statins-use patients and placebo-use patients respectively. All the six RCTs with 249 patients were combined using a fixed-effects model. statins-use were associated with a slight significant reduction in the incidence of vasospasm (RR, 0.76; 95% CI, 0.59–0.98). However, there was evidence of moderate heterogeneity (I2 = 49%, P = 0.08). A random-effects model was considered more appropriate. The result of meta-analysis using random-effects model showed no statistically significant (RR, 0.80; 95% CI, 0.54–1.17). Further exclusion of any single study did not materially alter the overall combined RR, with a range of from 0.70 (95% CI, 0.45–1.08) to 0.89 (95% CI, 0.61–1.29). The sensitivity analysis were also performed to examine the influence of various criteria on the combined estimates. No significant changes were found using sensitivity analyses, indicating that our results were reliable (Table 2).

Figure 3

Efficacy of statins-use in the prevention of vasospasm, DIND, poor neurological outcome and mortality, and the potential side effects of statins.

DNID: delayed ischemic neurological deficit.

Table 2

Sensitivity analysis based on various criteria for vasospasm

outcome	No. patients	No.RCTs	statins	placebo	RR (95%CI)	I2	P Value for Heterogeneity
All trials7814151623	249	6	51 of 124	68 of 125	0.80 (0.54–1.17)	49%	0.08
Trials with simvastatin-use714151623	169	5	34 of 84	43 of 85	0.81 (0.49–1.35)	53%	0.08
Trials with pravastatin-use8	80	1	17 of 40	25 of 40	0.68 (0.44–1.05)	—	—
Full text trials78141516	228	5	50 of 113	64 of 115	0.84 (0.58–1.21)	48%	0.1
Only TCD vasospasm* 71415	110	3	30 of 54	33 of 56	0.95 (0.54–1.66)	64%	0.06
Quality of trials withouthigh risk78141516	228	5	50 of 113	64 of 115	0.84 (0.58–1.21)	48%	0.1
statins treatment for 14 days781516	189	4	37 of 94	53 of 95	0.74 (0.49–1.12)	42%	0.16

*in RCT of Chou 2005, 10 patients in statins group and 13 patients in placebo group developed TCD vasospasm.

RCTs: randomized controlled trials; RR: risk ratio; TCD: transcranial doppler.

Although the definition of DIND was mentioned in all the trials, we only acquired the number of patients with DIND in four trials8141516. We tried to contact the corresponding authors of included RCTs for the missing analytical data, unfortunately, we did not get any reply. Therefore, only four RCTs were included in the meta-analysis of DIND. DIND was observed in 21% (20/94) statins-treated patients and 37% (35/95) placebo-treated patients respectively. Statins-use could significantly reduce the occurrence of DIND (RR, 0.58; 95% CI, 0.37–0.92), with no substantial heterogeneity (I2 = 46%, P = 0.14).

Neurological outcome was evaluated by GOS or MRS in five RCTs814151623. However, the detailed data of neurological outcome was reported in four trials8141516. For the definition of poor outcome, a GOS of 1 to 4 points was considered equivalent to a MRS of 3 to 6 points21. Poor outcome occurred in 61% (57/94) statins-treated patients, which presented in 64% (61/95) placebo-treated patients. The difference between two groups was not statistically significant (RR, 0.94; 95% CI, 0.77–1.16), with no substantial heterogeneity (I2 = 1%, P = 0.39).

Mortality was observed in all the six RCTs, which occurred in 6% (7/124) statins-treated patients versus 20% (25/125) placebo-treated patients. Statins-use was associated with a significant reduction in the occurrence of mortality (RR, 0.30; 95% CI, 0.14–0.64), with no substantial heterogeneity (I2 = 0%, P = 0.83).

Potential side effects of statins-use were reported in four studies7141516, which occurred in 11%(8/73) statins-use patients and 4% (3/75) placebo-use patients respectively. No significant difference (RR, 2.49; 95% CI, 0.75–8.33), with no substantial heterogeneity (I2 = 0%, P = 0.88), was found between two groups.

Subgroup meta-analysis Outcomes

According to the solubility in lipids or water, statins are classified as lipophilic statins and hydrophilic statins. Lipophilic statins (simvastatin) cross the blood-brain barrier and penetrate cell membranes more effectively and may be more efficient theoretically in the treatment of intracranial diseases than the hydrophilic statins (pravastatin). In addition, the dose of simvastatin in the included trials was 80 mg/d, while the dose of pravastatin in the included study was 40 mg/d. It may enhance the potential clinical heterogeneity if the trials using simvastatin and the study using pravastatin were pooled together in the meta-analysis. Thus, we further conducted the subgroup meta-analysis. Outcomes from simvastatin or pravastatin are shown in Table 3. According to meta-analysis from simvastatin, the incidence of mortality was significantly reduced in simvastatin-use group, whereas the occurrence of vasospasm, DIND and poor neurological outcome was not materially changed between simvastatin-use group and placebo-use group. Based on the RCT using pravastatin, pravastatin-use could prevent the occurrence of DIND, while no difference was found for vasospasm, mortality and poor neurological outcome between patients with pravastatin-use and patients without pravastatin-use.

Table 3

Subgroup meta-analysis outcomes

Outcomes	No. patients	No.RCTs	statins	placebo	RR (95%CI)	I2	P Value for Heterogeneity
Vasospasm
Simvastatin714151623	169	5	34 of 84	43 of 85	0.81 (0.49–1.35)	53%	0.08
Pravastatin8	80	1	17 of 40	25 of 40	0.68 (0.44–1.05)	—	—
DIND
Simvastatin141516	109	3	18 of 54	23 of 55	0.80 (0.49–1.30)	0%	0.6
Pravastatin8	80	1	2 of 40	12 of 40	0.17 (0.04–0.70)	—	—
Poor neurological outcome
Simvastatin141516	109	3	40 of 54	40 of 55	1.01 (0.82–1.25)	0%	0.53
Pravastatin8	80	1	17 of 40	21 of 40	0.81 (0.51–1.29)	—	—
Mortality
Simvastatin714151623	169	5	5 of 84	17 of 85	0.33 (0.14–0.77)	0%	0.74
Pravastatin8	80	1	2 of 40	8 of 40	0.25 (0.06–1.11)	—	—
Potential side effects
Simvastatin7141516	148	4	8 of 73	3 of 75	2.49 (0.75–8.33)	0%	0.88
Pravastatin8	—		—	—	—	—	—

RCTs: randomized controlled trials; DIND: delayed ischemic neurological deficit; RR: risk ratio.

Publication Bias

Publication bias was assessed by funnel plot, but the weak power with only six studies limited the interpretability of the finding.

Discussion

The results from previous meta-analyses remain controversial. Sillberg et al.18 supported all the benefits of statins-use in patients with aSAH from three RCTs. Tseng et al.19 reported that the benefit of statins was the reduced DIND from six RCTs, which was consistent with Kramer et al.20 from four RCTs and two “pseudo” RCTs. Nevertheless, Kramer et al.20 concluded that statins-use was not associated with any reduction in vasospasm, DIND, poor outcome and mortality from four RCTs, two “pseudo” RCTs, five cohort studies and one case–control study, which was also observed by Vergouwen et al.21 from four RCTs. To our knowledge, RCTs are the preferred study design to assess the efficacy of treatment, since the process of randomization ensures that confounders are balanced between different treatment groups. Restricting meta-analysis only to RCTs would be more appropriate to speculate the effects of treatment. At present, there are a new published RCT with respect to statins-use. Given the consideration of the above circumstances and no published large sample size, multicenter RCT of statins-use, it might be a deserved choice for us to further investigate the efficacy and safety of statins-use in patients with aSAH under the current RCTs.

In our study, owing to the inconsistent definitions of vasospasm in the six studies, moderate heterogeneity was presented in the meta-analysis of the incidence of vasospasm. Therefore, we chose random-effects model for this analysis. We found statins-use could not significantly affect the incidence of vasospasm in patients with aSAH. Exclusion of any single study, subgroup meta-analysis and sensitivity analysis based on various conditions did not materially alter the pooled results, which might make our finding reliable. For poor neurological outcome, the results from overall meta-analysis and subgroup meta-analysis consistently indicated that statins-use was not associated with the reduction of poor neurological outcome. Furthermore, Our meta-analysis showed that statins-use significantly decreased the occurrence of DIND. Although no substantial heterogeneity was found in the meta-analysis of the occurrence of DIND, subgroup meta-analysis demonstrated different result that DIND could not be decreased in simvastatin-use patients. Because we only acquired the data of vasospasm-related DIND, which was defined as the DIND associated with severe vasospasm on TCD in the pravastatin-use RCT8, and these was not the accurate data of overall DIND, thus, we should be very cautious to this result. In our opinion, we tended to believe the meta-analysis result from the simvastatin-use RCTs.

Interestingly, our important finding was that statins-use could prevent the occurrence of mortality although it could not significantly ameliorate cerebrovascular events caused by aSAH. To the best of our knowledge, firstly, in a Finnish prospective cohort study24 and in the International Subarachnoid Aneurysm Trial25, cerebrovascular diseases other than recurrent SAH and cardiovascular diseases were important causes of death, indicating that the increased mortality after SAH was caused by other vascular diseases. In addition, patients with SAH may have an increased risk of cardiovascular events because of shared risk factors26. Furthermore, SAH-associated myocardial injury was found by Nguyen et al27 from Aneurysm Surgery Trial. Lastly, in an autopsy study28, SAH accounted for 15.7% cases of the cardiovascular related deaths. Thus, we speculated that the direct cause of death in some SAH patients was not intracranial pathologies (vasospasm, DIND, poor neurological outcome, etc.) but cardiovascular events. However, statins-use could significantly decrease the cardiovascular mortality2930. Therefore, this might be the reason why statins-use could prevent the occurrence of mortality although it could not significantly ameliorate cerebrovascular events caused by aSAH in patients with aSAH.

There are some potential limitations in our present meta-analysis study. Firstly, so far, published RCTs regarding statins-use for patients with aSAH were all small sample size. Hence, the number of pooled patients in the meta-analysis is only 249. There is a greater chance that the baseline characteristics will be unbalanced between two groups. Second, the RCT with only abstract included in our study presented the high risk in the blinding of participants and blinding of outcome assessment. Finally, substantial differences in the study design among RCTs, including important differences in the treatment and outcome evaluation, could not be actually avoided in the present meta-analysis.

In conclusion, statin-use in the patients with aSAH, which might not be associated with the reduction in the incidence of vasospasm and poor neurological outcome, may reduce the occurrence of DIND and mortality. Furthermore, drug-induced hepatitis or myositis might not be the potential side effects of statins. Owing to the variations in methodology of included RCTs and small sample size, we should be very cautious to treat the results, which should be confirmed in the ongoing multicenter, double-blind RCT(Simvastatin in Aneurysmal Subarachnoid Haemorrhage; http://www.stashtrial.com/home.html). In our opinion, although statins-use in the patients with aSAH should not be considered standard care at present, statins-use may have the potential effects in the prevention of mortality in patients with aSAH. Moreover, cardiovascular risk assessment and subgroup analysis of cardiovascular death might be a deserved choice in the future study regarding statins-use in patients with aSAH.

Methods

Search Strategy and inclusion criteria

PubMed, EMBASE and three Chinese databases (SinoMed, CNKI and VIP) were searched for relevant articles published up to February, 2014. Search terms included “simvastatin”, “pravastatin”, “statin”, “statins” and “aneurysmal subarachnoid hemorrhage”, “aneurysmal subarachnoid haemorrhage” and “random”, “random*”. Furthermore, citations in the retrieved articles were reviewed to search for additional relevant studies. All studies included into this meta-analysis must meet the following criteria: (i) patients with aSAH; (ii) statins compared with placebo agent; (iii) randomized controlled trials. Duplicated studies, review, editorial and comment were excluded.

Data Extraction and Outcome Measures

Two authors(Y.-F.W and W.X) independently extracted the following data: first author, year of publication, number of patients, patients' characteristics, study design, statins group, placebo group, definitions of vasospasm, DIND, poor neurological outcome, mortality, potential side effects, and other outcomes data. Extracted data were checked by another author (J.H). Any disagreements were resolved by discussion and consensus.

Outcomes were the incidence of vasospasm, DIND, poor neurological outcome, mortality and potential side effects. Vasospasm included transcranial doppler(TCD) vasospasm and angiographic vasospasm. DIND was defined as clinical symptoms, TCD or angiographic results and signs of new ischemic neurologic deficits (not attributable to be due to hydrocephalus, clip-induced infarct, metabolic derangement, infection or rebleed). Poor neurological outcome was evaluated by Modified Rankin Scale (MRS) of 3–6 points and Glasgow Outcome Scale (GOS) of 1–4 points at the end of blinded follow-up period213132, which was either at discharge or 6 months after SAH. Serum alanine aminotransferase(ALT)/aspartate aminotransferase(AST) and creatine kinase(CK)/creatine phosphokinase (CPK) > 3-fold times the normal (ALT/AST > 180 U/L, CK/CPK > 1000 U/L) were regarded as potential side effects, which indicated the drug-induced hepatitis or myositis.

Quality Assessment

Cochrane risk of bias assessment33 was used to evaluated the methodologic quality of each trial. This scale consists of seven items including random sequence generation, allocation concealment, blinding of participants and personnel, blinding of outcome assessment, incomplete outcome data, selective reporting and other bias, each of which could be divided as low risk, high risk and unclear risk. Each RCT was evaluated independently by two authors(S.-H.S and F. Y). Any disagreements were resolved by consensus between all the authors.

Statistical Analysis

We performed meta-analysis using Cochrane RevMan (version 5.1) software. Differences were expressed as relative risk (RR) with 95% confidence interval(CI) for dichotomous outcomes. Heterogeneity for each pooled summary was estimated using Cochran's Q statistic and the I2 statistic. Substantial heterogeneity will be considered to exist with I2 > 50% or Chi square test P < 0.1. Meta-analysis was performed via fixed-effects model if there was no evidence of statistical heterogeneity. The random-effects model was employed to pool studies when statistical heterogeneity occurred. Meanwhile, we further conducted sensitivity analyses to explore possible explanations for heterogeneity and to examine the influence of various inconsistent criteria on the overall pooled estimate. We also investigated the influence of a single study on the overall pooled estimate by omitting one study in each turn. Publication bias was tested by a funnel plot.