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解脂耶氏酵母脂肪酶 2 在测试餐中稳定且高度活跃,并增加胰腺外分泌功能不全动物模型中的脂肪吸收。

Yarrowia lipolytica Lipase 2 Is Stable and Highly Active in Test Meals and Increases Fat Absorption in an Animal Model of Pancreatic Exocrine Insufficiency.

机构信息

CNRS-Aix-Marseille Université-UMR7282 Enzymology at Interfaces and Physiology of Lipolysis, Marseille, France; Laboratoires Mayoly Spindler SAS, Chatou, France.

CNRS-Aix-Marseille Université-UMR7282 Enzymology at Interfaces and Physiology of Lipolysis, Marseille, France; Proteabio Europe SAS, Langlade, France.

出版信息

Gastroenterology. 2015 Dec;149(7):1910-1919.e5. doi: 10.1053/j.gastro.2015.08.047. Epub 2015 Aug 29.

Abstract

BACKGROUND & AIMS: Pancreatic exocrine insufficiency (PEI) reduces pancreatic secretion of digestive enzymes, including lipases. Oral pancreatic enzyme replacement therapy (PERT) with pancreatin produces unsatisfactory results. The lipase 2 produced by the yeast Yarrowia lipolytica (YLLIP2; GenBank: AJ012632) might be used in PERT. We investigated its ability to digest triglycerides in a test meal and its efficacy in reducing fecal fat in an animal model of PEI.

METHODS

YLLIP2 was produced by genetically engineered Y lipolytica and purified from culture media. YLLIP2 or other gastric (LIPF) and pancreatic (PNLIPD) lipases were added to a meal paste containing dietary triglycerides, at a range of pH values (pH 2-7), with and without pepsin or human bile and incubated at 37°C. We collected samples at various time points and measured lipase activities and stabilities. To create an animal model of PEI, steatorrhea was induced by embolization of the exocrine pancreas gland and pancreatic duct ligation in minipigs. The animals were given YLLIP2 (1, 4, 8, 40, or 80 mg/d) or pancreatin (100,000 US Pharmacopeia lipase units/d, controls) for 9 days. We then collected stool samples, measured fat levels, and calculated coefficient of fat absorption (CFA) values.

RESULTS

YLLIP2 was highly stable and poorly degraded by pepsin, and had the highest activity of all lipases tested on meal triglyceride at pH 4-7 (pH 6 with bile: 94 ± 34 U/mg; pH 4 without bile: 43 ± 13 U/mg). Only gastric lipase was active and stable at pH 3, whereas YLLIP2 was sensitive to pepsin hydrolysis after pH inactivation. From in vitro test meal experiments, the lipase activity of YLLIP2 (10 mg) was estimated to be equivalent to that of pancreatin (1200 mg; 100,000 US Pharmacopeia units) at pH 6. In PEI minipigs, CFA values increased from 60.1% ± 9.3% before surgery to 90.5% ± 3.2% after administration of 1200 mg pancreatin (P < .05); CFA values increased to a range of 84.6% ± 3.0% to 90.0% ± 3.8% after administration of 4-80 mg YLLIP2 (P < .05).

CONCLUSIONS

The yeast lipase YLLIP2 is stable and has high levels of activity against test meal triglycerides in a large pH range, with and without bile. Oral administration of milligram amounts of YLLIP2 significantly increased CFA values, similar to that of 1.2 g pancreatin, in a minipig model of PEI.

摘要

背景与目的

胰腺外分泌不足(PEI)会减少胰腺分泌的消化酶,包括脂肪酶。口服胰酶替代疗法(PERT)用胰酶治疗效果不理想。产朊假丝酵母(Yarrowia lipolytica)产生的脂肪酶 2(YLLIP2;GenBank:AJ012632)可能用于 PERT。我们研究了它在测试餐中消化甘油三酯的能力及其在 PEI 动物模型中减少粪便脂肪的功效。

方法

通过基因工程改造产朊假丝酵母生产 YLLIP2,并从培养基中纯化。将 YLLIP2 或其他胃(LIPF)和胰腺(PNLIPD)脂肪酶添加到含有膳食甘油三酯的糊状物中,在 pH 值(2-7)范围内,有或没有胃蛋白酶或人胆汁,并在 37°C 下孵育。我们在不同时间点采集样本,测量脂肪酶活性和稳定性。为了建立 PEI 动物模型,通过栓塞胰腺外分泌腺和结扎胰腺导管诱导脂肪泻。将动物给予 YLLIP2(1、4、8、40 或 80 mg/d)或胰酶(100,000 美国药典单位/d,对照组)治疗 9 天。然后收集粪便样本,测量脂肪含量,并计算脂肪吸收率(CFA)值。

结果

YLLIP2 高度稳定,对胃蛋白酶的降解作用较小,在 pH 4-7(pH 6 加胆汁:94 ± 34 U/mg;pH 4 无胆汁:43 ± 13 U/mg)范围内所有测试脂肪酶中活性最高。只有胃脂肪酶在 pH 3 时具有活性和稳定性,而 YLLIP2 在 pH 失活后对胃蛋白酶水解敏感。从体外测试餐实验中,估计 YLLIP2(10 mg)的脂肪酶活性相当于胰酶(1200 mg;100,000 美国药典单位)在 pH 6 时的活性。在 PEI 小型猪中,手术后 CFA 值从 60.1%±9.3%增加到给予 1200 mg 胰酶后 90.5%±3.2%(P<0.05);给予 4-80 mg YLLIP2 后,CFA 值增加至 84.6%±3.0%至 90.0%±3.8%(P<0.05)。

结论

酵母脂肪酶 YLLIP2 稳定,在较大 pH 范围内对测试餐中的甘油三酯具有高活性,有或没有胆汁。在 PEI 小型猪模型中,口服毫克剂量的 YLLIP2 可显著增加 CFA 值,与 1.2 g 胰酶相似。

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