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首页> 外文期刊>Food research international >Identification of angiotensin converting enzyme and dipeptidyl peptidase-Ⅳ inhibitory peptides derived from oilseed proteins using two integrated bioinformatic approaches
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Identification of angiotensin converting enzyme and dipeptidyl peptidase-Ⅳ inhibitory peptides derived from oilseed proteins using two integrated bioinformatic approaches

机译:两种集成的生物信息学方法鉴定油籽蛋白衍生的血管紧张素转化酶和二肽基肽酶-Ⅳ抑制肽

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摘要

Angiotensin-converting enzyme (ACE) and dipeptidyl peptidase-IV (DPP-IV) play critical roles in the development of hypertension and type 2 diabetes, respectively. Inhibiting ACE and DPP-IV activity using peptides has become part of new therapeutic strategies for supporting medicinal treatment of both diseases. In this study, oilseed proteins, including soybean, flaxseed, rapeseed, sunflower and sesame are evaluated for the possibility of generating ACE and DPP-IV inhibitory peptides using different integrated bioinformatic approaches (UniProt knowledgebase, ProtParam, BLAST, BIOPEP, PeptideRanker, Pepsite2 and ToxinPred), and three bovine proteins (beta-lactoglobulin, beta-casein and kappa-casein) as comparisons. Compared with bovine proteins, the potency indices of ACE and DPP-IV inhibitory peptides, calculated using the BIOPEP database, suggest that oilseed proteins may be considered as good precursors of ACE inhibitory peptides but generate a relative lower yield of DPP-IV inhibitory peptides following subtilisin, pepsin (pH = 1.3) or pepsin (pH 2) hydrolysis. Average scores aligned using PeptideRanker confirmed oilseed proteins as significant potential sources of bioactive peptides: over 105 peptides scored over 0.8. Pepsite2 predicted that these peptides would largely bind via G1n281, His353, Lys511, His513, Tyr520 and Tyr523 of ACE to inhibit the enzyme, while Trp629 would be the predominant binding site of peptides in reducing DPP-IV activity. All peptides were capable of inhibiting ACE and DPP-IV whilst 65 of these 105 peptides are not currently recorded in BIOPEP database. In conclusion, our in silica study demonstrates that oilseed proteins could be considered as good precursors of ACE and DPP-IV inhibitory peptides as well as so far unexplored peptides that potentially have roles in ACE and DPP-IV inhibition and beyond.
机译:血管紧张素转换酶(ACE)和二肽基肽酶-IV(DPP-IV)分别在高血压和2型糖尿病的发生中起关键作用。使用肽抑制ACE和DPP-IV活性已成为支持两种疾病药物治疗的新治疗策略的一部分。在这项研究中,使用不同的综合生物信息学方法(UniProt知识库,ProtParam,BLAST,BIOPEP,PeptideRanker,Pepsite2和与ToxinPred)和三种牛蛋白(β-乳球蛋白,β-酪蛋白和kappa-酪蛋白)作比较。与牛蛋白相比,使用BIOPEP数据库计算得出的ACE和DPP-IV抑制肽的效能指数表明,油籽蛋白可能被认为是ACE抑制肽的良好前体,但随后产生的DPP-IV抑制肽的产量相对较低枯草杆菌蛋白酶,胃蛋白酶(pH = 1.3)或胃蛋白酶(pH> 2)水解。使用PeptideRanker进行比对的平均分数证实了油籽蛋白是生物活性肽的重要潜在来源:超过105个肽的得分超过0.8。 Pepsite2预测这些肽将通过ACE的G1n281,His353,Lys511,His513,Tyr520和Tyr523很大程度上结合,从而抑制该酶,而Trp629将是肽在降低DPP-IV活性中的主要结合位点。所有的肽都能够抑制ACE和DPP-IV,而这105种肽中的65种目前尚未记录在BIOPEP数据库中。总之,我们在二氧化硅中的研究表明,油籽蛋白可以被视为ACE和DPP-IV抑制肽的良好前体,以及迄今为止尚未开发的,可能对ACE和DPP-IV抑制有作用的肽。

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