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从人血红蛋白和牛血红蛋白的酶解产物中获得生物抗癌药物的新候选肽。

Obtaining New Candidate Peptides for Biological Anticancer Drugs from Enzymatic Hydrolysis of Human and Bovine Hemoglobin.

机构信息

Laboratories TBC, Laboratory of Pharmacology, Pharmacokinetics and Clinical Pharmacy, Faculty of Pharmacy, University of Lille, 3, rue du Professeur Laguesse, B.P. 83, 59000 Lille, France.

UMR Transfrontalière BioEcoAgro N_1158, Institut Charles Viollette, National Research Institute for Agriculture, Food and the Environment-Université Liège, UPJV, YNCREA, Université Artois, Université Littoral Côte d'Opale, Université Lille, 59000 Lille, France.

出版信息

Int J Mol Sci. 2023 Oct 19;24(20):15383. doi: 10.3390/ijms242015383.

DOI:10.3390/ijms242015383
PMID:37895063
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10607105/
Abstract

Enzymatic hydrolysis of bovine and human hemoglobin generates a diversity of bioactive peptides, mainly recognized for their antimicrobial properties. However, antimicrobial peptides stand out for their ability to specifically target cancer cells while preserving rapidly proliferating healthy cells. This study focuses on the production of bioactive peptides from hemoglobin and evaluates their anticancer potential using two distinct approaches. The first approach is based on the use of a rapid screening method aimed at blocking host cell protein synthesis to evaluate candidate anticancer peptides, using seed germination as an indicator. The results show that: (1) The degree of hydrolysis (DH) significantly influences the production of bioactive peptides. DH levels of 3 to 10% produce a considerably stronger inhibition of radicle growth than DH 0 (the native form of hemoglobin), with an intensity three to four times greater. (2) Certain peptide fractions of bovine hemoglobin have a higher activity than those of human hemoglobin. (3) The structural characteristics of peptides (random coil or alpha helix) play a crucial role in the biological effects observed. (4) The α137-141 peptide, the target of the study, was the most active of the fractions obtained from bovine hemoglobin (IC = 29 ± 1 µg/mL) and human hemoglobin (IC = 48 ± 2 µg/mL), proving to be 10 to 15 times more potent than the other hemoglobin fractions, attributed to its strong antimicrobial potential. The second approach to assessing anticancer activity is based on the preliminary in vitro analysis of hydrolysates and their peptide fractions, with a focus on the eL42 protein. This protein is of major interest due to its overexpression in all cancer cells, making it an attractive potential target for the development of anticancer molecules. With this in mind, astudy was undertaken using a method for labeling formylase (formyl-methionyl-tRNA transformylase (FMTS)) with oxidized tRNA. This approach was chosen because of the similarities in the interaction between formylase and the eL42 protein with oxidized tRNA. The results obtained not only confirmed the previous conclusions but also reinforced the hypothesis that the inhibition of protein synthesis plays a key role in the anticancer mechanism of these peptides. Indeed, the data suggest that samples containing α137-141 peptide (NKT) and total hydrolysates may have modulatory effects on the interaction between FMTS and oxidized tRNA. This observation highlights the possibility that the latter could influence molecular binding mechanisms, potentially resulting in a competitive situation where the ability of substrate tRNA to bind efficiently to ribosomal protein is compromised in their presence. Ultimately, these results suggest the feasibility of obtaining candidate peptides for biological anticancer drugs from both human and bovine hemoglobin sources. These scientific advances show new hope in the fight against cancer, which affects a large number of people around the world.

摘要

从牛血红蛋白和人血红蛋白中酶解生成多种生物活性肽,这些肽主要因具有抗菌特性而受到关注。然而,抗菌肽的突出特点是能够特异性地靶向癌细胞,同时保留快速增殖的健康细胞。本研究从血红蛋白中生产生物活性肽,并使用两种不同的方法评估其抗癌潜力。第一种方法基于使用快速筛选方法来阻断宿主细胞蛋白质合成,以评估候选抗癌肽,使用种子发芽作为指标。结果表明:(1)水解度(DH)显著影响生物活性肽的产生。DH 水平为 3%至 10%时,比 DH0(血红蛋白的天然形式)更强烈地抑制胚根生长,强度增加 3 至 4 倍。(2)某些牛血红蛋白的肽段比人血红蛋白的活性更高。(3)肽的结构特征(无规卷曲或α螺旋)在观察到的生物学效应中起着关键作用。(4)研究目标的α137-141 肽是从牛血红蛋白(IC=29±1μg/mL)和人血红蛋白(IC=48±2μg/mL)获得的肽段中最活跃的肽段,证明其比其他血红蛋白肽段强 10 至 15 倍,归因于其强大的抗菌潜力。评估抗癌活性的第二种方法是基于对水解物及其肽段的初步体外分析,重点是 eL42 蛋白。由于该蛋白在所有癌细胞中过度表达,因此它是开发抗癌分子的一个有吸引力的潜在靶点。考虑到这一点,进行了一项使用氧化 tRNA 标记甲酰甲硫氨酸-tRNA 转甲酰酶(formyl-methionyl-tRNA transformylase (FMTS))的研究。选择这种方法是因为甲酰甲硫氨酸-tRNA 转甲酰酶与 eL42 蛋白与氧化 tRNA 的相互作用存在相似性。得到的结果不仅证实了之前的结论,还强化了这样的假设,即抑制蛋白质合成在这些肽的抗癌机制中起着关键作用。事实上,数据表明,含有α137-141 肽(NKT)和总水解物的样品可能对 FMTS 和氧化 tRNA 之间的相互作用具有调节作用。这一观察结果突出表明,后者可能影响分子结合机制,从而导致底物 tRNA 与核糖体蛋白有效结合的能力在其存在下受到损害的竞争情况。最终,这些结果表明可以从人源和牛源血红蛋白中获得生物抗癌药物的候选肽。这些科学进展为抗击癌症带来了新的希望,癌症影响着全球大量人群。

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Potential of Human Hemoglobin as a Source of Bioactive Peptides: Comparative Study of Enzymatic Hydrolysis with Bovine Hemoglobin and the Production of Active Peptide α137-141.人血红蛋白作为生物活性肽来源的潜力:与人血红蛋白酶解及活性肽α137 - 141产生的比较研究
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