Abstract
Treatment with sodium tanshinone IIA sulfonate (STS) may ameliorate blood-brain barrier (BBB) damage in acute ischemic stroke patients receiving recombinant tissue plasminogen activator (rt-PA) thrombolysis and improve stroke patients’ outcome. This randomized, single-center, placebo-controlled clinical trial investigated the potential effects and underlying mechanisms of STS. Forty-two acute ischemic stroke patients receiving intravenous rt-PA thrombolysis were randomized to intravenous administration either with STS (60 mg/day) (n = 21) or with equivalent volume of saline as a placebo (n = 21) after randomization for 10 days. Clinical outcomes, computer tomography perfusion (CTP) imaging with permeability-surface area product (PS) maps and serum levels of BBB damage biomarkers, were compared between the two groups. The percentage of patients with excellent functional outcome indicated by a 90-day mRS ≤1 was significantly higher in the STS group than in the placebo group (p = 0.028). For patients with CTP imaging (n = 30), PS in the ipsilateral lesion (p = 0.034) and relative PS (p = 0.013) were significantly lower in the STS group than that in placebo. STS-treated patients also had lower levels of matrix metalloproteinase (MMP)-9 (p = 0.036) and claudin-5 (p = 0.026), but higher levels of tissue inhibitor of metalloproteinase (TIMP)-1 (p = 0.040) than those in the placebo group. Post-stroke STS treatment could improve neurologic functional outcomes for acute ischemic stroke patients following rt-PA treatment by reducing BBB leakage and damage, which might be mechanistically associated with MMP-9 inhibition.
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Introduction
Blood-brain barrier (BBB) breakdown is a major contributing factor to ischemic brain injury or hemorrhagic transformation (HT) and often leads to poor outcomes in acute ischemic stroke patients receiving recombinant tissue plasminogen activator (rt-PA) treatment [1, 2]. Tight-junction proteins such as claudin, junctional adhesion molecule, and occludin play essential roles in maintaining BBB integrity. Measurements of permeability-surface area product (PS), an indicator of BBB permeability, by computer tomography perfusion (CTP) imaging have been successfully applied for early identification of BBB damage and HT development in acute stroke patients [3, 4].
Sodium tanshinone IIA sulfonate (STS) is a water-soluble derivative of tanshinone IIA, a main bioactive component isolated from the roots of the Chinese herb Salviae miltiorrhiza Bunge (Danshen) [5]. STS has been widely used for treatments of cardiovascular and cerebrovascular diseases in China [6, 7]. In mice with cerebral ischemia, STS could protect BBB and had a patent in China [8, 9]. Here, we hypothesized that STS could work as a BBB protective agent that help acute ischemic stroke patients who received thrombolysis treatment recover better. In this study, we used CTP-derived PS to reveal whether treatment with STS could reduce BBB leakage in acute ischemic stroke patients receiving rt-PA thrombolysis and sought to investigate the underlying mechanisms.
Materials and Methods
Participants
This single-centered, randomized, double-blinded prospective study was approved by the ethics committee of Drum Tower Hospital, Medical School of Nanjing University. An entry was made in the Chinese clinical trial registry (ChiCTR-ONRC-14004659). The inclusion criteria were as follows: (1) acute ischemic stroke patients receiving rt-PA treatment, (2) at age between 18 to 80 years old, and (3) willing to participate in all follow-up neurologic and imaging examinations. We excluded patients with presence of platelet abnormalities (PLT < 100 or >300 × 109/L), severe bleeding disorders, contraindications to iodinated contrast agent, a history of severe renal failure, or known or suspected infection. Informed consents were obtained from all participants involved in this study. Randomization sequences were computer generated. The flow chart of patient cohort selection is shown in Fig. 1.
Treatments
After rt-PA thrombolysis, STS (60 mg per day) was intravenously administrated daily to patients in the STS group for 10 days, while patients in the placebo group received equivalent administrations of saline. All participants received aspirin after thrombolysis 24 h for acute ischemic stroke.
Neurologic Assessment
Neurologic function outcomes were assessed using the National Institutes of Health Stroke Scale (NIHSS) score at 0, 24 h, and 10 days; activities of daily living (ADLs) score at 0 h and 10 days; and the modified Rankin Scale (mRS) at 90 days.
CTP Scan Protocol and Image Analysis
CT perfusion and non-contrast CT scans were performed on a 64-slice CT scanner (Discovery CT750 HD, GE Healthcare, Milwaukee, WI, USA). CTP started with intravenous injection of 50 mL of iodinated contrast agent (350 mg/mL, Omnipaque, GE Healthcare, Shanghai, China) followed by a saline flush of 45 mL at 5 mL/s. CTP scans began after a delay of 5 s from contrast injection, and the following technical settings were applied: 80 kVp, 150 mAs, temporal sampling rate of 2 s for 60 s, and total axial coverage of 40 mm at 5-mm slice thickness.
All CTP images were analyzed by experienced radiologists who were blinded to this research. For the PS maps and data, manually drawn region of interests (ROIs) in the ipsilateral hemisphere were compared to those in the contralateral hemisphere. PS values were calculated using CTP software (CT Kinetics, GE Healthcare, China). The corresponding ROIs for the contralateral side were generated automatically by mirroring the ipsilateral ROIs, and the relative PS (rPS) was defined as ipsilateral/contralateral ROIs.
Measurement of BBB Damage Biomarkers
Venous blood were collected at 0, 24 h, and 10 days, and the separated serum was stored in aliquots at −80 °C until biochemical analysis.
Serum levels of matrix metalloproteinase (MMP)-2 (R&D, Minneapolis, IL, USA), MMP-9 (R&D, Minneapolis, IL, USA), tissue inhibitor of metalloproteinase (TIMP)-1 (R&D, Minneapolis, IL, USA), claudin-5 (CusaBio, Wu han, China), and zonula occluden (ZO)-1 (CusaBio, Wu han, China) were measured using commercially available ELISA kits according to the manufacturer’s instructions.
Study Outcomes
The outcomes were the integrity of blood-brain barrier by measurement of PS, MMP-9, MMP-2, TIMP-1, claudin-5, and ZO-1 and neurologic improvement by the score on NIHSS and the mRS at 90 days. Safety outcome measures the incidence of adverse event.
Statistical Analysis
All results were analyzed using SPSS (SPSS version 22.0, Chicago, Illinois, USA). The data were shown as mean ± standard deviation (SD) or medians with interquartile ranges for continuous variables and proportions for categorical variables. Continuous variables were compared using t tests, and categorical variables were analyzed using the Pearson χ 2 test or Fisher’s exact test. P value <0.05 was considered statistically significant.
Results
Patient Characteristics
From February 2014 to February 2016, 46 patients receiving rt-PA were included: 23 patients were treated with STS and 23 with placebo as control. Three patients had uncompleted treatment due to transferring to another department, and one patient was lost follow-up, thus leaving 21 patients in each group for clinical and prognostic analysis. General clinical characteristics (e.g., age, sex, risk factors, and NIHSS scores) and the distribution of baseline NIHSS at admission were similar (Table 1 and Fig. 2). In the 42 patients, 12 were unavailable to attend the second CT examinations, leaving 16 and 14 patients for imaging analysis in the STS and placebo groups, respectively.
Clinical Outcomes
A battery of neurologic function assessments was used to investigate whether patients with acute ischemic stroke could benefit from STS after rt-PA thrombolysis. Results showed that in whole 42 patients (21 STS and 21 placebo), there were more patients with a 90-day mRS score ≤1 (an excellent functional outcome) in the STS group than that in the placebo group. Though there is no statistical significance, STS did decrease the incidence of HT during hospitalization. No significant difference was found in the means of NIHSS and ADL score at 10 days after rt-PA treatment between the two groups (Table 2 and Fig. 3).
Neuroimaging of BBB Permeability between STS and Placebo Groups
CTP was performed to reveal the effects of STS treatment on BBB integrity. Twenty-four hours after rt-PA treatment, a baseline CTP was performed for each patient and there was no significant difference in BBB permeability (ipsilateral or contralateral and rPS) between the two groups. The follow-up CTP was performed at 10 days after the treatments. Moreover, the STS group showed significantly lower levels of ipsilateral PS and rPS than did the placebo group at 10 days (Table 3 and Fig. 4).
Serum BBB Damage Biomarkers
Serum levels of MMP-9, MMP-2, TIMP-1 and tight-junction proteins, including claudin-5 and ZO-1, in 30 patients (16 STS and 14 placebo) were measured to demonstrate BBB damage. The STS group had lower MMP-9 (633.352 vs 750.739 ng/ml, p = 0.036, Fig. 5a) and claudin-5 (337.822 vs 407.763 pg/ml, p = 0.026, Fig. 5b) levels but higher TIMP-1 expression (520.652 vs 459.567 ng/ml, p = 0.040, Fig. 5c) than did the placebo group at 10 days after thrombolytic therapy. However, at acute phase (0 and 24 h), there were no significant differences in all biomarkers between the two groups.
Discussion
Current rt-PA thrombolytic therapy could augment BBB disruption in the acute stroke patients, which increase ischemic brain injury or HT [10]. Therefore, therapeutic strategies designed to alleviate BBB damage are needed to improve clinical outcomes of rt-PA thrombolysis [11]. Prognosis of rt-PA-treated patients with mRS ≤1 (an excellent functional outcome) was reported differently, from 42.7% to 54.6% at 3 months [12–14]. As Tsivgoulis reported, mRS ≤1 scores was 42.7%, which is similar to our control group (mRS ≤ 1 scores was 42.86%). Effect of rt-PA therapy is affected by many factors, such as treatment time since stroke onset, age, stroke severity, BBB integrity, and so on. Our study found that there were more patients with a 90-day mRS score ≤1 in the STS group compared with the placebo group.
To investigate whether the neuroprotection of STS is associated with decreasing BBB disruption, PS was detected by dynamic contrast-enhanced CT [10, 15, 16]. Recently, CTP-derived PS quantification has been used to predict BBB permeability and HT for acute stroke patients because of its good reproducibility in hemodynamic measurement, wide accessibility, and relatively low cost [2, 4, 10]. The neuroimaging results from this study showed that STS treatment could reduce BBB-PS to ameliorate BBB damage and benefit clinical outcomes post-rt-PA thrombolysis in acute stroke patients. Pathologically, release of tight junction adhesion molecules to blood circulation is associated with compromised BBB integrity in ischemic stroke [3]. Tanshinone IIA (precursor of STS) treatment has been previously shown to diminish BBB breakdown in experimental model of ischemic stroke [8, 9] and autoimmune encephalomyelitis [17]. Similarly, in this study, we found that STS treatment decreased the levels of BBB damage biomarkers, MMP-9 and claudin-5, in acute ischemic stroke patients after intravenous thrombolysis. From our observations, STS seemed to reduce the effects of BBB disruption by inhibiting MMP-9 activity and increasing expression of TIMP-1.
Next, we evaluated the infarct volumes and found no difference between the STS group (2.020 ± 1.762 cm3) and the placebo group (2.415 ± 3.083 cm3) after 10 days of treatment (p = 0.676). It suggested that STS did not reduce BBB damage through decreasing infarct volumes.
Furthermore, to study whether STS decreases cerebral hemorrhagic transformation, STS did reduce the trend of cerebral hemorrhagic transformation, but it was not significant, which may be correlated to the small sample research. STS could inhibit peripheral inflammatory cells into brain after stroke by suppressing BBB injury, which protects brain from immuno-inflammation and improves recover of stroke patients.
How STS protects the BBB from injury after stroke remains unclear. STS might improve BBB damage by suppressing astrocyte-mediated inflammation or decreasing brain microvascular endothelial cell apoptosis after stroke.
Together, the neuroimaging and pathological evidence of our study could delineate the mechanistic pathway of STS treatment in improving BBB dysfunction post-rt-PA thrombolysis.
However, we had several limitations in the current work. First, to better elucidate the relation between BBB damage biomarkers and PS, MMPs and tight junction proteins obtained from cerebrospinal fluid (CSF) examination by lumbar puncture and a correlation study are needed in the future. Second, lack of BBB-PS measurements from CTP imaging at 90 days could not fully evaluate the effects of STS treatment on BBB repair. In addition, our study had a small sample size although the randomization has been applied. These questions will be addressed in our future work.
In conclusion, both neuroimaging and serum biomarkers of BBB damage in this study demonstrated that acute ischemic stroke patients might benefit from STS treatment by ameliorating/diminishing BBB disruption following rt-PA thrombolysis.
Reference
Chaturvedi M, Kaczmarek L. Mmp-9 inhibition: a therapeutic strategy in ischemic stroke. Mol Neurobiol. 2014;49:563–73.
Horsch AD, Dankbaar JW, van Seeters T, et al. Relation between stroke severity, patient characteristics and ct-perfusion derived blood-brain barrier permeability measurements in acute ischemic stroke. Clin Neuroradiol. 2016;26:415–21.
Kazmierski R, Michalak S, Wencel-Warot A, et al. Serum tight-junction proteins predict hemorrhagic transformation in ischemic stroke patients. Neurology. 2012;79:1677–85.
Avsenik J, Bisdas S, Popovic KS. Blood-brain barrier permeability imaging using perfusion computed tomography. Radiol Oncol. 2014;49:107–14.
Tian XH, Wu JH. Tanshinone derivatives: a patent review (January 2006- September 2012). Expert Opin Ther Pat. 2013;23:19–29.
Zhang H, Long M, Wu Z, et al. Sodium tanshinone IIA silate as an add-on therapy in patients with unstable angina pectoris. J Thorac Dis. 2014;6:1794–9.
Shang Q, Wang H, Li S, et al. The effect of sodium tanshinone IIA sulfate and simvastatin on elevated serum levels of inflammatory markers in patients with coronary heart disease: a study protocol for a randomized controlled trial. Evid Based Complement Alternat Med. 2013;2013:756519.
Zhang WJ, Feng J, Zhou R, et al. Tanshinone IIA protects the human blood-brain barrier model from leukocyte-associated hypoxia-reoxygenation injury. Eur J Pharmacol. 2010;648:146–52.
Wang L, Zhang X, Liu L, et al. Tanshinone ii a down-regulates hmgb1, rage, tlr4, nf-kappab expression, ameliorates BBB permeability and endothelial cell function, and protects rat brains against focal ischemia. Brain Res. 2010;1321:143–51.
Ozkul-Wermester O, Guegan-Massardier E, Triquenot A, et al. Increased blood-brain barrier permeability on perfusion computed tomography predicts hemorrhagic transformation in acute ischemic stroke. Eur Neurol. 2014;72:45–53.
Shi Y, Leak RK, Keep RF, et al. Translational stroke research on blood-brain barrier damage: challenges, perspectives, and goals. Transl Stroke Res. 2016;7:89–92.
Hacke W, Kaste M, Bluhmki E, et al. Thrombolysis with alteplase 3 to 4.5 hours after acute ischemic stroke. N Engl J Med. 2008;359:1317–29.
Emberson J, Lees KR, Lyden P, et al. Effect of treatment delay, age, and stroke severity on the effects of intravenous thrombolysis with alteplase for acute ischaemic stroke: a meta-analysis of individual patient data from randomised trials. Lancet. 2014;384:1929–35.
Tsivgoulis G, Kadlecová P, Kobayashi A, et al. Safety of statin pretreatment in intravenous thrombolysis for acute ischemic stroke. Stroke. 2015;46:2681–4.
Ivanidze J, Kesavabhotla K, Kallas ON, et al. Evaluating blood-brain barrier permeability in delayed cerebral infarction after aneurysmal subarachnoid hemorrhage. AJNR Am J Neuroradiol. 2015;36:850–4.
Neumann-Haefelin C, Brinker G, Uhlenkuken U, et al. Prediction of hemorrhagic transformation after thrombolytic therapy of clot embolism: an MRI investigation in rat brain. Stroke; J Cereb Circ. 2002;33:1392–8.
Yang X, Yan J, Feng J. Treatment with tanshinone iia suppresses disruption of the blood-brain barrier and reduces expression of adhesion molecules and chemokines in experimental autoimmune encephalomyelitis. Eur J Pharmacol. 2016;771:18–28.
Acknowledgements
Xu Yun designed the experiments and edited the manuscript. Ji Biying, Li Shanshan, Li Jingwei, and Zhang Xin collected patients and blood samples. Ji Biying performed ELISA test. Zhou Fei, Fan Haijian, and Yang Jun scanned and analyzed the CTP. Han Lijuan and Ji Biying wrote the manuscript. Wang Xiaoying and Chen Xiangyan revised this paper. All authors contributed to the data analysis and the manuscript preparation. We thank Brad Peterson for editing the English.
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This research was supported by the National Natural Science Foundation of China (81230026, 81630028, 81601016, 81171085), the Natural Science Foundation (BE2016610, BK20160119) of Jiangsu Province, the National Key Research and Development Program of China (2016YFC1300500-504).
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The authors declare that they have no conflict of interest.
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All procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 Helsinki Declaration and its later amendments or comparable ethical standards.
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Informed consent was obtained from all individual participants included in the study.
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None of the authors are financially tied to the patent mentioned above.
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Biying Ji, Fei Zhou, and Lijuan Han contributed equally to this article.
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Ji, B., Zhou, F., Han, L. et al. Sodium Tanshinone IIA Sulfonate Enhances Effectiveness Rt-PA Treatment in Acute Ischemic Stroke Patients Associated with Ameliorating Blood-Brain Barrier Damage. Transl. Stroke Res. 8, 334–340 (2017). https://doi.org/10.1007/s12975-017-0526-6
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DOI: https://doi.org/10.1007/s12975-017-0526-6