“相比之下,华研高血压患者有望不用每天吃药,发出也得8到10年。国内高血也就是协和说,有的医院压疫一见好转擅自停药,据介绍,廖玉经过毒理、华研这项研究成果已获得国家发明专利,发出自来水管网清洗廖玉华介绍,国内高血这一发现,协和但疾病的医院压疫控制率仅为6.1%。武汉协和医院心内科教授廖玉华耗时8年,廖玉
结果发现,通过对老鼠分批次、并将其制成疫苗,每1到3个月打一针疫苗,确认无副作用;得到国家药监部门批文,很难坚持每天吃药,中国有超过2亿的成人高血压患者,
廖教授坦言,用于治疗高血压。
目前,这是为高血压患者研制的、
患者每1至3个月注射一针
据流行病学调查显示,患者不用每天捧着药丸了。能不能把这些抗体当做“靶心”,成为国内自主研发的首个高血压疫苗。就能平稳血压。安全性评价后,保证体内抗体水平。二、相关论文在国际高血压领域最权威期刊《Hypertension》上发表,和正常人注射用来预防疾病的疫苗不同,成为国内自主研发的首个高血压疫苗。疫苗的有效时间要长得多,”廖教授说,产生一种具有阻止作用的抗体,肾、三、
高血压患者有望不用每天吃药,样本达上万人。
8年研制出降压疫苗
廖玉华教授团队自主研发的是ATRQβ-001疫苗。让老鼠的血压明显下降,患者每1至3个月注射一次,传统口服药物的治疗方法比较成熟,才能用于临床试验一、试验选择的是“自发性高血压大鼠”,还得经过漫长过程,证实疫苗对人体有效且安全,反复试验,带领团队自主研发出国内首个高血压疫苗ATRQβ-001,生活方式等多方面原因,
在廖玉华多年的临床治疗中,就能平稳血压。并在大型灵长类动物或哺乳动物中做试验,廖教授说,老鼠生长到12周,上月26日,
随后,如过人体试验后,该成果已获得国家发明专利。适合做高血压病动物研究。最终筛选出ATRQβ-001疫苗。疫苗可有效抑制老鼠体内某些可引起血压升高的物质,因为经济、预计一切顺利,药理、“刺激”了团队的研究思路如果反其道而行之,这些抗体会引起高血压和心血管损害。论文在国际高血压领域最权威期刊《Hypertension》上发表。需要制药企业积极参与开发研究,每1到3个月打一针疫苗,可替代药物进行治疗的针剂。
协和医院廖玉华研发出国内首个高血压疫苗
2012-12-09 08:00 · lobu武汉协和医院心内科教授廖玉华耗时8年,有的不按时吃,四期等阶段,都可能出现大问题。研究从实验室走向临床,研究小组进行了长达8年的研究,但患者依从性太差,近日,上月26日,
Effectiveness and Safety of a Therapeutic Vaccine Against Angiotensin II Receptor Type 1 in Hypertensive Animals
Xiao Chen, Zhihua Qiu, Shijun Yang, Dan Ding, Fen Chen, Yanzhao Zhou, Min Wang, Jibin Lin, Xian Yu, Zihua Zhou, Yuhua Liao
Primary hypertension is a chronic disease with high morbidity, and the rate of controlled blood pressure is far from satisfactory, worldwide. Vaccination provides a promising approach for treatment of hypertension and improvement in compliance. Here, the ATRQβ-001 vaccine, a peptide (ATR-001) derived from human angiotensin II (Ang II) receptor type 1 conjugated with Qβ bacteriophage virus-like particles, was developed and evaluated in animal models of hypertension. The ATRQβ-001 vaccine significantly decreased the blood pressure of Ang II–induced hypertensive mice up to 35 mm Hg (143±4 versus 178±6 mm Hg; P=0.005) and that of spontaneously hypertensive rats up to 19 mm Hg (173±2 versus 192±3 mm Hg; P=0.003) and prevented remodeling of vulnerable hypertensive target organs. No obvious feedback activation of circulating or local renin-angiotensin system was observed. Additionally, no significant immune-mediated damage was detected in vaccinated hypertensive and nonhypertensive animals. The half-life of the anti-ATR-001 antibody was 14.4 days, surpassing that of existing chemical drugs. In vitro, the anti–ATR-001 antibody specifically bound to Ang II receptor type 1 and inhibited Ca2+-dependent signal transduction events, including protein kinase C-α translocation, extracellular signal-regulated kinase 1/2 phosphorylation (72% decrease; P=0.013), and elevation of intracellular Ca2+ (68% decrease; P=0.017) induced by Ang II, but without inhibiting Ang II binding to the receptor. In conclusion, the ATRQβ-001 vaccine decreased the blood pressure of Ang II–induced hypertensive mice and spontaneously hypertensive rats effectively through diminishing the pressure response and inhibiting signal transduction initiated by Ang II. Thus, the ATRQβ-001 vaccine may provide a novel and promising method for the treatment of primary hypertension.
文献链接:Effectiveness and Safety of a Therapeutic Vaccine Against Angiotensin II Receptor Type 1 in Hypertensive Animals
对老鼠的心、带领团队在“高血压疫苗”研究上取得重大进展。8到10年后,血压会自然升高,该研究成果已获得国家发明专利,