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质子泵抑制剂对溶酶体酶活性的抑制作用。

Inhibition of lysosomal enzyme activities by proton pump inhibitors.

机构信息

Women and Children's Hospital of Buffalo and Department of Pediatrics, SUNY at Buffalo, Buffalo, NY, 14222, USA.

出版信息

J Gastroenterol. 2013 Dec;48(12):1343-52. doi: 10.1007/s00535-013-0774-5. Epub 2013 Mar 12.

DOI:10.1007/s00535-013-0774-5
PMID:23478938
Abstract

BACKGROUND

Proton pump inhibitors (PPIs) are pro-drugs requiring an acidic pH for activation. The specificity of PPI toward the proton pump is mainly due to the extremely low pH at the parietal cell canalicular membrane where the pump is located. Reactivity of PPIs was also observed in moderately acidic environments like the renal collecting duct. But no PPI effect on lysosomal enzymes has been observed possibly because the previous studies were performed with liver tissue, where PPIs are metabolized.

METHODS

The reactivity of PPIs (omeprazole, lansoprazole and pantoprazole) with a cysteine-containing peptide was analyzed by mass spectrometry, and the impact of PPIs on lysosomal enzymes was evaluated in cultured cells and mice. The effect of PPIs on the immune system was examined with a mouse tumor immunotherapy model.

RESULTS

Incubation of a cysteine-containing peptide with PPIs at pH5 led to the conversion of most of the peptide into PPI-peptide adducts. Dose dependent inhibition of lysosomal enzyme activities by PPIs was observed in cultured cells and mouse spleen. Further, PPI counteracted the tumor immunotherapy in a mouse model.

CONCLUSIONS

Our data support the hypothesis that many of the PPI adverse effects are caused by systematically compromised immunity, a result of PPI inhibition of the lysosomal enzymes. This novel mechanism complements the existing mechanisms in explaining the increased incidence of tumorigenesis and infectious diseases among PPI users and underlie the ongoing concern about the overuse of PPIs in adult and pediatric populations.

摘要

背景

质子泵抑制剂(PPIs)是前体药物,需要酸性 pH 值才能激活。PPI 对质子泵的特异性主要归因于壁细胞管腔膜中泵所在的极低 pH 值。PPIs 在中等酸性环境(如肾集合管)中也表现出反应性。但尚未观察到 PPI 对溶酶体酶的影响,可能是因为之前的研究是在肝脏组织中进行的,PPIs 在肝脏组织中代谢。

方法

通过质谱分析研究了 PPIs(奥美拉唑、兰索拉唑和泮托拉唑)与含半胱氨酸肽的反应性,并在培养的细胞和小鼠中评估了 PPIs 对溶酶体酶的影响。使用小鼠肿瘤免疫治疗模型研究了 PPIs 对免疫系统的影响。

结果

在 pH5 下将含半胱氨酸的肽与 PPIs 孵育会导致大部分肽转化为 PPI-肽加合物。在培养的细胞和小鼠脾脏中观察到 PPIs 对溶酶体酶活性的剂量依赖性抑制。此外,PPI 会拮抗小鼠模型中的肿瘤免疫治疗。

结论

我们的数据支持这样一种假设,即许多 PPI 的不良反应是由系统性免疫受损引起的,这是 PPI 抑制溶酶体酶的结果。这种新机制补充了现有机制,解释了 PPI 用户中肿瘤发生和传染病发病率增加的原因,并说明了在成人和儿科人群中过度使用 PPI 的持续关注。

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