首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Tetrapeptide inhibitors of protein farnesyltransferase: amino-terminal substitution in phenylalanine-containing tetrapeptides restores farnesylation.
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Tetrapeptide inhibitors of protein farnesyltransferase: amino-terminal substitution in phenylalanine-containing tetrapeptides restores farnesylation.

机译:蛋白法尼基转移酶的四肽抑制剂:含苯丙氨酸的四肽中的氨基末端取代可恢复法尼基化。

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摘要

Protein farnesyltransferase from rat brain transfers farnesyl residues to cysteine residues in tetrapeptides that conform to the sequence CA1A2X, where C is cysteine, A1 and A2 are aliphatic amino acids, and X is methionine or serine. When the A2 residue is aromatic [e.g., phenylalanine as in Cys-Val-Phe-Met (CVFM)], the tetrapeptide continues to bind to the enzyme, but it can no longer accept a farnesyl group, and it becomes a pure inhibitor. The current studies show that this resistance to farnesylation also requires a positive charge on the cysteine amino group. Derivatization of this group with acetyl, octanoyl, or cholic acid residues or extension of the peptide with an additional amino acid restores the ability of phenylalanine-containing peptides to accept a farnesyl residue. The same result was obtained when the amino group of cysteine was deleted (mercaptopropionyl-VFM). These data suggest that the positive change on the cysteine amino group acts in concert with an aromatic residue in the A2 position to render peptides resistant to farnesylation by the rat brain enzyme.
机译:来自大鼠大脑的蛋白质法呢基转移酶将法呢基残基转移到符合序列CA1A2X的四肽中的半胱氨酸残基,其中C为半胱氨酸,A1和A2为脂肪族氨基酸,X为蛋氨酸或丝氨酸。当A2残基是芳族的时[例如,如Cys-Val-Phe-Met中的苯丙氨酸(CVFM)],四肽继续结合到该酶上,但是它不再能接受法呢基,而成为纯的抑制剂。目前的研究表明,这种对法尼基化的抗性还需要在半胱氨酸氨基上带正电荷。用乙酰基,辛酰基或胆酸残基将该基团衍生化,或用另外的氨基酸将肽延伸,可恢复含苯丙氨酸的肽接受法呢基残基的能力。当缺失半胱氨酸的氨基(巯基丙酰基-VFM)时,得到相同的结果。这些数据表明,半胱氨酸氨基上的正变化与A2位置的芳族残基协同作用,使肽具有抵抗大鼠脑酶法尼基化的能力。

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