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环糊精暴露后血液中耳毒性诱导的 prestin 爆发的自动 Western Blot 分析。

Automated Western Blot Analysis of Ototoxin-Induced Prestin Burst in the Blood after Cyclodextrin Exposure.

机构信息

Frequency Therapeutics, Lexington, Massachusetts.

Division of Otolaryngology-Head and Neck Surgery, Department of Surgery, University of Connecticut School of Medicine, Farmington, Connecticut.

出版信息

Otol Neurotol. 2023 Oct 1;44(9):e653-e659. doi: 10.1097/MAO.0000000000003994. Epub 2023 Aug 8.

Abstract

HYPOTHESIS

Ototoxin cyclodextrin (CDX) will induce a burst in serum prestin when quantified with automated Western blot analysis.

BACKGROUND

In the clinical realm, we primarily rely on audiological measures for diagnosis and surveillance of sensorineural hearing loss (SNHL) and have limited therapeutic options. We have proposed a blood-based biomarker approach to overcome this challenge by measuring the outer hair cell's (OHC) electromotile protein, prestin, in the blood. Previously, we demonstrated a burst in serum prestin after cisplatin exposure using enzyme-linked immunosorbent assayELISA.

METHODS

Guinea pigs were treated with either 3,000 or 4,000 mg/kg CDX, and serum samples were obtained through 3 days after exposure. Serum prestin levels were quantified using automated blot analysis, western and hair cell counts were obtained.

RESULTS

Both 3,000 and 4,000 mg/kg resulted in robust OHC loss, although more variability was seen at the lower dose. Automated Western blot analysis demonstrated that the prestin profile after CDX exposure is different than baseline. Specifically, a new ~134- kDa band accounted for the prestin burst after ototoxin ablation of OHCs at both doses.

CONCLUSIONS

We reproduced the prestin burst seen after cisplatin administration using CDX. Automated Western blot western analysis revealed that a ~a ~ 134- kDa species of prestin is responsible for the burst. We suggest that the induced band may be a prestin dimer, which could serve as a biomarker for early detection of ototoxicity in the clinical setting. These results add further promise to the potential of serum prestin to serve as an ototoxicity biomarker when using therapeutics with ototoxic properties.

摘要

假设

使用自动化 Western blot 分析定量检测时,耳毒性环糊精 (CDX) 会引起血清 prestin 的爆发。

背景

在临床领域,我们主要依靠听力学测量来诊断和监测感音神经性听力损失 (SNHL),并且治疗选择有限。我们提出了一种基于血液的生物标志物方法,通过测量血液中外毛细胞 (OHC) 的电活动蛋白 prestin 来克服这一挑战。之前,我们使用酶联免疫吸附试验 (ELISA) 证明了顺铂暴露后血清 prestin 的爆发。

方法

豚鼠接受 3000 或 4000mg/kg CDX 治疗,暴露后 3 天获取血清样本。使用自动化印迹分析定量检测血清 prestin 水平,同时获取 Western 和毛细胞计数。

结果

3000 和 4000mg/kg 均导致 OHC 大量丢失,尽管较低剂量的结果更具变异性。自动化 Western blot 分析表明,CDX 暴露后的 prestin 谱与基线不同。具体来说,在两种剂量下,OHC 耳毒性消融后,新的约 134kDa 带负责 prestin 的爆发。

结论

我们使用 CDX 复制了顺铂给药后观察到的 prestin 爆发。自动化 Western blot 分析表明,一种约 134kDa 的 prestin 物种负责爆发。我们建议诱导的带可能是 prestin 二聚体,它可以作为临床环境中检测耳毒性的早期标志物。这些结果进一步证明了血清 prestin 在使用具有耳毒性的治疗药物时作为耳毒性生物标志物的潜力。

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