Evaluation Of Intra-Arterial Nimodipine Therapy In Post-Subarachnoid Hemorrhage Refractory Cerebral Vasospasm

DOI: https://doi.org/10.21203/rs.3.rs-482464/v1

Abstract

Background: Cerebral vasospasm is a major cause of morbidity and mortality in patients with subarachnoid hemorrhage. Vasospasm is managed with triple H and vasodilators but sometimes, patients do not respond. Intra-arterial vasodilator infusion has been shown to improve outcome in such patients. In this study, we try to evaluate the efficacy of intra-arterial nimodipine therapy in 43 patients of post-aneurysmal subarachnoid hemorrhage refractory cerebral vasospasm. 

Methods: It is a prospective observational study of a group of 43 patients presenting with refractory cerebral vasospasm as per the inclusion criteria. Pre-procedure neurological assessment and Transcranial Doppler (TCD) monitoring were done. Endovascular spasmolysis was conducted and post-operative morbidity and outcomes were noted. Follow up of the patients was done at the time of discharge and at 6 months according to the Modified Rankin Scale and NCCT head. 

Results: Most of the patients developing refractory cerebral vasospasm belonged to Hunt and Hess Grade 2 and 3 and Fisher grade 3 and 4. 87.5% of the patients showed clinical recovery following endovascular spasmolysis and 58% of the patients showed complete angiographic recovery. Outcome after 6 months was good in 76%, moderate in 12% and poor in 12% patients. NCCT head showed no infarct in 58%, minor infarct in 28% and major vascular territorial infarct in 14% patients. 

Conclusions: Intra-arterial nimodipine infusion is a safe and effective therapy with minimum risk of complications if adhered to standard endovascular practice. By timely intervention, major ischemic insult to the brain can be averted, thereby significantly improving the prognosis. 

Introduction

Cerebral vasospasm is a major cause of morbidity and mortality in patients of subarachnoid hemorrhage (SAH), occurring in 30–50% of the patients. It is an important factor to determine the prognosis and eventual outcome of the patient. It results in a decrease in cerebral blood flow, disturbance in autoregulation and delayed cerebral ischaemia.

Pathogenesis of vasospasm after SAH has been related to hemolysis of the subarachnoid blood.[29] Contraction of vessels also occurs in response to vasoactive substances released from erythrocyte hemosylate, the key components being haemoglobin and other vasoactive factors including serotonin, norepinephrine, bradykinins, angiotensin, prostaglandin, thromboxanes and free radicals.[1, 2]

Vasospasm can be diagnosed by clinical examination, Doppler ultrasound or by angiography. Transcranial Doppler uses low frequency ultrasound (1–2 MHz) to assess the blood flow velocity in the cerebral vessels. It is a safe, inexpensive and readily available method, that promptly identifies vessels in spasm. Angiography is the main modality of investigation and offers combined advantage of a diagnostic as well as therapeutic tool, in the form of mechanical (balloon angioplasty) and pharmacological angioplasty.

Management of vasospasm requires double or triple H therapy as hypervolemia is not recommended nowadays.[7] In addition, calcium channel blockers are particularly useful in vasospasm management. Nimodipine is most commonly used agent in view of its cerebro-selective nature. Jan et al[14] reported a 36% reduction in bad outcome in patients treated with nimodipine. Other calcium channel blockers including nicardipine and verapamil, free oxygen radical scavengers, statins, endothelin receptor antagonists and nitric oxide donor drugs have also been used in the vasospasm management.

In patients with cerebral vasospasm, not responding to medical management, cerebrospinal fluid drainage and endovascular intervention remain viable options. Balloon angioplasty has shown promising results in dilatation of proximal major cerebral arteries but has no effect in distal cerebral artery vasospasm. In cases of distal vessel spasm, pharmacological dilatation of the vessels intra-arterially is useful. Authors attempt to study the efficacy and complications of intra-arterial instillation of nimodipine in patients with refractory cerebral vasospasm.

Methods And Materials

It is a single institutional observational prospective study wherein, 43 patients were analyzed for efficacy and complications of intra-arterial nimodipine from December 2013 to June 2017. Patients considered were those who developed cerebral vasospasm in post-aneurysmal rupture subarachnoid hemorrhage, not responding to medical management. Patients excluded from the study were those with traumatic SAH, children, pregnant or lactating women or patients with well-developed infarct.

A detailed history and thorough physical examination was done on patients, along with their clinical grading according to Hunt and Hess scale Non contrast computed tomography (NCCT) head was done for confirmation of SAH along with grading according to Fisher grade. Angiography was done for confirmation of aneurysm and transcranial doppler (TCD) was performed for baseline mean velocity of intracranial vessels. Definitive treatment of the aneurysm (clipping/coiling) was done according to variable aneurysm and patient factors.

Post-procedure, patient was monitored and managed under strict guidelines on triple H therapy. Intravenous or oral nimodipine was initiated post-procedure to prevent vasospasm. Intravenous fluids were given to the patients to maintain the central venous pressure. Regular monitoring of these patients was done and daily detailed neurological examination as well as Transcranial Doppler monitoring was conducted.

In patients who developed delayed neurological deficits clinically, alternative causes of neurological deterioration like hydrocephalus, re-bleeding, hyponatraemia or seizure were investigated for and managed accordingly. After excluding such causes, mean blood pressure was raised upto 110 mm Hg. With persistence of neurological deficit or showing TCD mean velocity of greater than 150 cm/sec or an increase of 40 cm/s or more from the established baseline, patients were considered in refractory vasospasm and were taken up for Angiography. Vasospasm was classified as mild (< 25% decrease in vessel lumen), moderate (25–50% decrease in vessel lumen) and severe (> 50% decrease in vessel lumen).

After taking the informed consent, patient underwent check cerebral DSA and intra-arterial nimodipine infusion using microcatheter. Upto 3 mg of Nimodipine per vascular territory was given slowly at the rate of 0.15 to 0.3 mg per hour. In case of hypotension during nimodipine infusion, inotropic support was added. However, in case of inability to maintain blood pressure, nimodipine infusion was discontinued. The details of the procedure were noted.

The outcome of the patient, post-procedure, was noted angiographically, clinically and radiologically.(Fig. 1) Angiographic response was classified into mild, moderate and complete depending on the circulation time and dilation of the vessel previously in spasm, i.e.,

Clinical outcome was noted in terms of improvement in focal deficit, improvement in clinical status and post-procedure TCD mean velocity in the affected vessels. Any requirement of repeat procedure was noted depending on the outcome of the patient or in case of continued deterioration of the above parameters.

Radiological outcome was noted on the presence or absence of any infarct (major arterial territory or minor) post-procedure done at the time of discharge and after 6 months of follow up.(Fig. 2) Follow up of the patient was done at the time of discharge and 6 months clinically, in terms of Modified Rankin Scale. Outcome was considered as:

Statistical Analysis

Data entry was done in Microsoft excel and Data analysis was done using stata 12. Demographic and clinical data were described as percentages. Comparison of pre-procedural and post-procedural neurological status was analyzed using paired t test. A p- value of less than 0.05 was considered significant.

Results

43 patients were evaluated in the study, whose demographic and clinical profiles are illustrated in Table 1. Male to female ratio was 20:23, with average age or presentation being 53 years and range from 20 to 73 years. 58% of the patients presented with Glasgow Coma Scale (GCS) above 14 with 51% of the patients presenting with focal neurological deficit. Majority of the patients belonged to Hunt and Hess grade II and III (67%); and Fisher grade III and IV (47% and 32%, respectively). 56% of the patients underwent coiling and 44% underwent clipping as definitive treatment of the aneurysm.

Table 1. 43 patients were evaluated in the study, whose demographic and clinical profiles are illustrated in table.

Total number of Patients

43

Sex (Male : Female)

20:23

Age in years (Range, Mean) 

20-73; 53

Glasgow coma scale (GCS), no. (%)

     Greater than equal to 14

     11-13

     0-10

 

25(58)

13(30)

5(12)

Focal Deficits at admission, no. (%)

21 (49)

Hunt & Hess grade, no. (%)

     I

     II

     III

     IV

     V

 

9 (21)

16 (37)

13 (30)

5 (12)

0 (0)

Fisher grade, no. (%)

      I

      II

     III

     IV

 

0 (0)

9 (21)

20 (47)

14 (32)

Location of Aneurysm, no. (%)

     Anterior communicating artery

     Middle cerebral artery

     Posterior communicating artery

     Vertebro-basilar artery

     Internal carotid artery

     Anterior choroidal artery

     Distal anterior cerebral artery

 

13 (30)

9 (21)

5 (12)

7 (16)

4 (9)

3 (7)

2 (5)

 

Treatment of anueryms, no. (%)

     Clipping 

     Coiling

 

19 (44)

24 (56)

49% of the patients developed vasospasm on post-ictal day 9 with earliest ranging from day 4 to latest on day 13 as depicted in Graph 1. Details about the cerebral vasospasm development and its management are illustrated in Table 2. 56% of the patients presented with clinical deterioration while 88% of the patients were found to be developing vasospasm on the basis of elevated flow velocity on TCD. 54% of the patients were found to have vasospasm in unilateral vessels while severity of vasospasm was found to be moderate and severe in 37% and 37% patients, respectively.

Table 2. Details about the cerebral vasospasm development and its management are illustrated in table.

Patients with delayed neurological deficit, no. (%)

24 (56)

Site of Vasospasm, no. (%)

     Middle cerebral artery

     Anterior cerebral artery

     Internal carotid artery

     Posterior cerebral artery

     Bilateral vessels

 

21 (49)

16 (47)

21 (49)

3 (7)

20 (46)

Degree of vasospasm, no. (%)

     Mild

     Moderate

     Severe

 

11 (26)

16 (37)

16 (37)

Dosage of nimodipine (mg) instilled, no. (%)

     3

     6

     7

     8

     9

 

10 (23)

24 (56)

1 (2)

2 (5)

6 (14)

Angiographic recovery, no. (5%)

      Mild

      Moderate

      Complete

 

9 (21)

9 (21)

25 (58)

Clinical recovery, no. (%)

21 (87.5)

Repeat spasmolysis, no. (%)

5 (12)

As per the protocol, all patients were locally administered intra-arterial nimodipine infusion up to a maximum dosage of 3 mg per vascular territory. 58% of the patients showed complete angiographic recovery while 87.5% of the patients showed clinical recovery after the intervention. Post-procedural TCD velocity was found to decrease in accordance with angiographic recovery in the patients with the mean difference of 40.46 cm/sec (Graph 2). Out of all the patients, 5 patients (12%) needed a repeat procedure at a later date in view of inadequate recovery.

Final Outcome has been illustrated in Table 3. At the time of discharge, 72% of patients had good outcome, 16% had moderate with 12% had poor outcome. On NCCT head, 58% had no infarcts while 28% had minor infarcts. On follow-up after 6 months, 76% patients had good clinical outcome while 12% patient died before the follow up period. NCCT head findings remained the same as at the time of discharge.

Table 3. Final Outcome has been illustrated in table.

Clinical outcome on discharge, no. (%)

     Good

     Moderate

     Poor

 

31 (72)

7 (16)

5 (12)

Vasospasm related infarction on discharge, no. (%)

     No infarct

     Minor infarct

     Major Discharge

 

25 (58)

12 (28)

6 (14)

Mortality, no. (%)

5 (12)

Clinical outcome at 6 moths follow up, no. (%)

     Good

     Moderate

     Poor

 

33 (76)

5 (12)

0 (0)

Vasospasm related infarction at 6 months follow up, no. (%)

     No infarct

     Minor infarct

     Major infarct

 

25 (58)

12 (28)

1 (3)

Discussion

Cerebral vasospasm is one of the most common treatable complication with aneurysmal subarachnoid hemorrhage, causing death and disability in 12–17% of SAH patients.[8, 9, 17, 18] Clinical features of vasospasm depends on the vascular territory being affected. Although, other causes of neurological deterioration must be ruled out including electrolyte disturbance (hyponatremia), infection (meningitis and sepsis), hydrocephalus and seizures. TCD provides a cheap, reliable, repeatable and portable test for early diagnosis of vasospasm. Sensitivity and specificity of TCD in detecting vasospasm is high and is reported to be 84–85% and 89–98% respectively[15]. Angiography remains the gold standard for the diagnosis of vasospasm. CT head can be used for prognostication but is not a useful technique for early diagnosis of vasospasm.

Management of vasospasm requires good intensive care including measurement of central venous pressure, cardiac output monitoring along with good neuro-nursing care. Triple H therapy is targeted at increasing cerebral blood flow (CBF) and decreasing hematocrit, improving the rheological properties of blood. Solomon et al[28] suggested that immediate aneurysm surgery and aggressive post-operative prophylactic volume expansion in all patients can substantially reduce re-bleeding and delayed cerebral ischaemia, potential cause of morbidity after aneurysmal SAH. According to latest international guidelines, hypervolaemia is not recommended anymore and HH therapy is preferred nowadays.[7]

Among pharmacological prevention of vasospasm, calcium channel antagonist are drugs of choice. Nimodipine has selective central nervous system (CNS) action and blocks dihydropyridine sensitive (L-type) calcium channels. It blocks calcium influx in smooth muscle cell and leads to reduced vascular smooth muscle constriction and consequent improved cerebral perfusion. Other possible mechanisms having direct neuroprotective effects include decrease in the release of vasoactive substances from endothelium and platelets, blockage of free-radical attack on the intra neuronal mitochondria, and improvement of CO2 reactivity and cerebral oxygen metabolism, or a reduction of tissue damage caused by calcium overload at reperfusion. Its short half-life requires frequent dosing in order to maintain sustained concentration. Recently, several trials have been conducted to assess efficacy of statins, endothelin-1 antagonists and magnesium sulfate.[25]

Patients who fail to respond adequately, endovascular therapy including balloon angioplasty and chemical vasodilatation, have been shown to play crucial role. Mechanical angioplasty has demonstrated permanent reversal of vasospasm in treated vessels, but it can be applied to only proximal vessel segments [19, 26]. Numaguchi et al demonstrated successfully that pharmacologic dilation by means of intra-arterial papaverine has the advantage of also acting on smaller distal branches and diffuse vasospasm. However, its beneficial effects are transient, and repeat treatment sessions are often necessary[23]. Use of papaverine for intra-arterial infusion has largely been abandoned in view of limited success, frequent dosing and serious side effects including exacerbation of vasospasm[6], thrombocytopenia[21] and increase in intracranial pressure[20]. Milrinone was shown to have recurrence rate of cerebral vasospasm more than 20% following intra-arterial bolus injection.[10, 27] Other drugs used for intra-arterial infusion include nicardipine, verapamil, colforsin daropate, but no studies have shown significant advantage of these drugs over nimodipine.

There have been several studies performed to assess efficacy of intra-arterial nimodipine infusion in management of refractory cerebral vasospasm.[3, 4, 5, 11, 12, 13, 22, 24, 30] It was observed that majority of the patients developing cerebral vasospasm belonged to Hunt & Hess Grade II and III along with Fisher grade III and IV. The number of patients in refractory cerebral vasospasm were found to be more in the coiling group (56%) in the present study however, this does not suggest that patients who undergo coiling have more chances of going into cerebral vasospasm as it was evaluated in the study. Out of 43 patients, 24 patients (56%) developed delayed neurological deficits at the onset of vasospasm while 40 patients (93%) were detected on the basis of increased flow velocity on TCD. TCD velocity corroborated with clinical deterioration in 21 off 24 patients (88%). This stresses over the importance of regular TCD monitoring and clinical examination as effective means of early detection and management of vasospasm.

In our study, local administration of intra-arterial nimodipine was done at a dosage of 3 mg/territory. Total nimodipine dose used in 43 patients ranged from a minimum of 3 mg to a maximum of 9 mg. Inotropic support was started intra-procedure to maintain hemodynamic status of the patient. In 5 patients (12%), we were not able to give nimodipine sufficiently in view of inability to maintain hemodynamic status. In a study conducted by Biondi et al, 1–3 mg of nimodipine was given per vessel. The total dose of nimodipine injected intra-arterially for a given patient was maintained within 5 mg.[4] Cho et al kept the dose of nimodipine from 3 to 6 mg at a rate of 6 mg/h per vessel. When transient hypotension occurred during procedure, infusion was stopped temporarily until blood pressure became normalized.[5]

In our study, 25 patients off 43 (58%) showed complete angiographic recovery and 9 patients (21%) showed moderate angiographic recovery. 21 off 24 patients (87.5%) who had developed neurological deficits, clinically improved after spasmolysis while 3 patients (12.5%) did not show any improvement. When compared with Bondi et al, only 7% showed excellent angiographic response, 37% showed good and 57% showed poor response. 76% patients showed substantial and stable clinical improvement in their clinical condition.[4] On the other hand, in study conducted by Cho et al, 83% cases showed good angiographic response post-intervention while neurological deficits improved in 69% of the patients after spasmolysis.[5] A correlation can be established with the dosage of nimodipine infused intra-arterially with better response being seen in studies where high dosage was used.

On discharge and follow up, it was observed in our study that by timely intervention, mortality of refractory cerebral vasospasm was reduced to 12% as compared to 14–26% without endovascular intervention as reported by Kassell et al.[16] Patient with good clinical outcome was comparable to other studies assessing efficacy of intra-arterial nimodipine therapy. Most of the patients tolerated intra-arterial nimodipine infusion well with only 12% of the patients developing systemic hypotension. No other systemic side effect was noticed in any of the patient following intra-arterial nimodipine therapy. There was no procedural complication found in any of the patients.

Authors are of the opinion that the study conducted was of small sample size and a larger study is required to really assess the effect of alteration in dosage of nimodipine during intra-arterial instillation for a better outcome. Also, with intra-arterial nimodipine infusion, 58% of the patients showed complete angiographic recovery while 87.5% showed clinical recovery. This warrants additional investigation in combination of nimodipine with alternative pharmaceutical agents like milrinone and fasudil for better outcome in patients.

Conclusion

Cerebral vasospasm remains the major cause of morbidity and mortality in post-subarachnoid period and one should be watchful for timely detection and intervention of vasospasm for good outcome. With regular detailed neurological examination and TCD monitoring, it is possible to timely diagnose and manage cerebral vasospasm. Intra-arterial nimodipine infusion is safe and effective therapy with minimum risk of complications if adhered to standard endovascular practice. By timely intervention, major ischaemic insult to the brain can be averted as seen by low number of large infarcts in follow up CT scan and thereby significantly improving the prognosis.

Declarations

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