A Serotonin 2A-Receptor Decoy Peptide Potently Lowers Blood Pressure in Male Zucker Diabetic, Fatty, Hypertensive Rats.

Mark B Zimering
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Abstract

Aims: To test whether a novel 5-hydroxytryptamine 2A decoy receptor peptide, SN..8 (Sertuercept), administered via intraperitoneal injection, acutely lowers arterial blood pressure in obese, hypertensive male Zucker diabetic rats (ZDF). To examine the safety, tolerability and possible reno-protective effects following chronic alternate daily administration of Sertuercept (for 10 weeks) in the male ZDF rat.

Methods: Systolic and diastolic blood pressure were determined at baseline and regular intervals for up to 48 hours after a single IP administration of either Sertuercept (2 mg/kg), vehicle (saline) or an identical concentration of a scrambled sequence of the decoy receptor peptide, LN…8, in male ZDF and Zucker lean rats using tail cuff plethysmography. Plasma autoantibodies were obtained in thirteen male ZDF rats for determination of 5-hydroxytryptamine 2A receptor-mediated neurotoxicity using an acute neurite retraction assay in mouse neuroblastoma cells. Rats were sacrificed at 25-weeks of age, the kidneys were perfused, fixed and sections were stained using Masson's trichrome for semi-quantitative determination of glomerular and interstitial fibrosis.

Results: Sertuercept (2 mg/kg IP) potently lowered systolic and diastolic blood pressure in both 11-week-old and 25-week-old male ZDF rats and in a subset of hypertensive Zucker lean rats. There was no significant blood pressure-lowering effect of vehicle (saline) or scrambled peptide sequence (LN.8). Blood pressure-lowering was rapid in onset (15-30 minutes following IP injection) and sustained for at least 24 hours. Alternate daily IP administration of 2 mg/kg dose of Sertuercept vs. scrambled peptide (for 10 weeks) was safe, well-tolerated and associated with a significant decrease in glomerulosclerosis in 25-week-old male ZDF rats. Plasma autoantibody-induced neurotoxicity correlated significantly with the global index of renal fibrosis severity in 25-week-old male ZDF rats.

Conclusions: These data indicate potent arterial blood pressure-lowering efficacy from a decoy receptor peptide comprised of a second extracellular loop region of the human 5-hydroxytryptamine receptor. Chronic administration of the decoy receptor peptide (10 weeks) was safe, well-tolerated and protected against renal glomerulosclerosis in the male ZDF rat.

一种羟色胺 2A 受体诱饵肽能有效降低雄性扎克糖尿病脂肪高血压大鼠的血压
目的:测试通过腹腔注射给药的新型5-羟色胺2A诱饵受体肽SN...8(Sertuercept)是否能急性降低肥胖、高血压雄性扎克糖尿病大鼠(ZDF)的动脉血压。研究雄性扎克糖尿病大鼠长期每天交替服用赛鲁肽(10 周)后的安全性、耐受性和可能的肾脏保护作用:方法:在雄性ZDF大鼠和Zucker瘦大鼠一次IP给药Sertuercept(2毫克/千克)、载体(生理盐水)或相同浓度的诱饵受体肽LN......8乱序序列后,使用尾套式压力计测定收缩压和舒张压,并在48小时内定期测定收缩压和舒张压。通过在小鼠神经母细胞瘤细胞中进行急性神经元回缩试验,获得了 13 只雄性 ZDF 大鼠的血浆自身抗体,以测定 5- 羟色胺 2A 受体介导的神经毒性。大鼠在 25 周龄时被处死,对肾脏进行灌注、固定,并使用马森三色染色法对切片进行染色,以半定量测定肾小球和肾间质纤维化:赛鲁肽(2 毫克/千克 IP)能有效降低 11 周大和 25 周大雄性 ZDF 大鼠以及高血压 Zucker 瘦大鼠的收缩压和舒张压。载体(生理盐水)或加扰肽序列(LN.8)没有明显的降压效果。降压作用起效迅速(IP 注射后 15-30 分钟),并可持续至少 24 小时。在25周大的雄性ZDF大鼠身上,每天交替IP注射2毫克/千克剂量的Sertuercept与加扰肽(持续10周)是安全的,耐受性良好,并能显著减少肾小球硬化。血浆自身抗体诱导的神经毒性与25周大雄性ZDF大鼠肾脏纤维化严重程度的总体指数显著相关:这些数据表明,由人类 5-羟色胺受体的第二个细胞外环区域组成的诱饵受体肽具有强效的降低动脉血压作用。长期服用诱饵受体肽(10 周)对雄性 ZDF 大鼠安全、耐受性良好,并能防止肾小球硬化。
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