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首款获美国食品药品监督管理局批准用于颅内刺激、记录和监测脑活动的薄膜电极——第1部分:生物相容性测试。

First Food and Drug Administration Cleared Thin-Film Electrode for Intracranial Stimulation, Recording, and Monitoring of Brain Activity-Part 1: Biocompatibility Testing.

作者信息

Kullmann Aura, Kridner Debra, Mertens Steve, Christianson Mark, Rosa Dave, Diaz-Botia Camilo A

机构信息

NeuroOne Medical Technologies Corporation, Eden Prairie, MN, United States.

出版信息

Front Neurosci. 2022 Apr 29;16:876877. doi: 10.3389/fnins.2022.876877. eCollection 2022.

DOI:10.3389/fnins.2022.876877
PMID:35573282
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9100917/
Abstract

Subdural strip and grid invasive electroencephalography electrodes are routinely used for surgical evaluation of patients with drug-resistant epilepsy (DRE). Although these electrodes have been in the United States market for decades (first FDA clearance 1985), their fabrication, materials, and properties have hardly changed. Existing commercially available electrodes are made of silicone, are thick (>0.5 mm), and do not optimally conform to brain convolutions. New thin-film polyimide electrodes (0.08 mm) have been manufactured to address these issues. While different thin-film electrodes are available for research use, to date, only one electrode is cleared by Food and Drug Administration (FDA) for use in clinical practice. This study describes the biocompatibility tests that led to this clearance. Biocompatibility was tested using standard methods according to International Organization for Standardization (ISO) 10993. Electrodes and appropriate control materials were bent, folded, and placed in the appropriate extraction vehicles, or implanted. The extracts were used for and tests, to assess the effects of any potential extractable and leachable materials that may be toxic to the body. studies included cytotoxicity tested in L929 cell line, genotoxicity tested using mouse lymphoma assay (MLA) and Ames assay, and hemolysis tested in rabbit whole blood samples. The results indicated that the electrodes were non-cytotoxic, non-mutagenic, non-clastogenic, and non-hemolytic. studies included sensitization tested in guinea pigs, irritation tested in rabbits, acute systemic toxicity testing in mice, pyrogenicity tested in rabbits, and a prolonged 28-day subdural implant in sheep. The results indicated that the electrodes induced no sensitization and irritation, no weight loss, and no temperature increase. Histological examination of the sheep brain tissue showed no or minimal immune cell accumulation, necrosis, neovascularization, fibrosis, and astrocyte infiltration, with no differences from the control material. In summary, biocompatibility studies indicated that these new thin-film electrodes are appropriate for human use. As a result, the electrodes were cleared by the FDA for use in clinical practice [510(k) K192764], making it the first thin-film subdural electrode to progress from research to clinic. Its readiness as a commercial product ensures availability to all patients undergoing surgical evaluation for DRE.

摘要

硬膜下条形和栅格状侵入性脑电图电极通常用于药物难治性癫痫(DRE)患者的手术评估。尽管这些电极在美国市场上已经存在了几十年(1985年首次获得美国食品药品监督管理局(FDA)批准),但其制造工艺、材料和特性几乎没有改变。现有的市售电极由硅酮制成,较厚(>0.5毫米),不能很好地贴合脑沟回。新型薄膜聚酰亚胺电极(0.08毫米)已被制造出来以解决这些问题。虽然有不同的薄膜电极可用于研究,但迄今为止,只有一种电极获得了FDA批准可用于临床实践。本研究描述了促成该批准的生物相容性测试。根据国际标准化组织(ISO)10993使用标准方法测试生物相容性。将电极和适当的对照材料弯曲、折叠,置于适当的提取介质中,或进行植入。提取物用于进行 和 测试,以评估任何可能对身体有毒的潜在可提取物和可浸出物的影响。 研究包括在L929细胞系中测试细胞毒性、使用小鼠淋巴瘤试验(MLA)和艾姆斯试验测试遗传毒性,以及在兔全血样本中测试溶血。结果表明电极无细胞毒性、无致突变性、无染色体断裂作用且无溶血作用。 研究包括在豚鼠中测试致敏性、在兔中测试刺激性、在小鼠中测试急性全身毒性、在兔中测试热原性,以及在绵羊中进行为期28天的硬膜下长期植入。结果表明电极未引起致敏和刺激,无体重减轻,体温未升高。对绵羊脑组织的组织学检查显示无或仅有极少的免疫细胞聚集、坏死、新生血管形成、纤维化和星形胶质细胞浸润,与对照材料无差异。总之,生物相容性研究表明这些新型薄膜电极适用于人体。因此,该电极获得了FDA批准可用于临床实践[510(k) K1927,64],使其成为首个从研究进展到临床的薄膜硬膜下电极。其作为商业产品的就绪状态确保了所有接受DRE手术评估的患者都可使用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b71/9100917/db957fefe9e4/fnins-16-876877-g002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b71/9100917/cd3bd2b35a18/fnins-16-876877-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b71/9100917/db957fefe9e4/fnins-16-876877-g002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b71/9100917/cd3bd2b35a18/fnins-16-876877-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b71/9100917/db957fefe9e4/fnins-16-876877-g002.jpg

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