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含新型亲脂性胞壁酰肽衍生物MDP-L-丙氨酰-胆固醇(MTP-CHOL)的脂质体在体外激活巨噬细胞的抑制细胞生长和细胞毒性活性。

Activation of macrophage cytostatic and cytotoxic activity in vitro by liposomes containing a new lipophilic muramyl peptide derivative, MDP-L-alanyl-cholesterol (MTP-CHOL).

作者信息

Phillips N C, Moras M L, Chedid L, Petit J F, Tenu J P, Lederer E, Bernard J M, Lefrancier P

出版信息

J Biol Response Mod. 1985 Oct;4(5):464-74.

PMID:3935756
Abstract

The ability of liposomes containing a new lipophilic muramyl peptide derivative, MDP-L-alanyl-cholesterol (MTP-CHOL), to induce peritoneal macrophage cytostatic activity and alveolar macrophage cytotoxic activity toward tumor cell targets in vitro was determined. MTP-CHOL was shown to be efficiently incorporated and subsequently retained in distearoylphosphatidylcholine/phosphatidylserine liposomes (DSPC/PS; 7:3 molar ratio), whereas hydrosoluble muramyl dipeptide (MDP) was rapidly lost due to leakage. Liposomes containing MTP-CHOL were able to stimulate mouse peritoneal macrophage cytostatic activity under conditions where free MDP was without effect. MTP-CHOL incorporated into liposomes was approximately eightfold more effective than liposomes containing entrapped MDP and 7,400-fold more effective than free MDP in inducing rat alveolar macrophage cytotoxic activity. These results provide evidence that the coupling of MDP to a lipophilic molecule, cholesterol, results in the formation of a viable liposome formulation that is a potent inducer of macrophage-mediated antitumor activity.

摘要

测定了含有新型亲脂性胞壁酰肽衍生物MDP-L-丙氨酰-胆固醇(MTP-CHOL)的脂质体在体外诱导腹膜巨噬细胞对肿瘤细胞靶标的细胞抑制活性以及肺泡巨噬细胞细胞毒活性的能力。结果表明,MTP-CHOL能有效掺入并随后保留在二硬脂酰磷脂酰胆碱/磷脂酰丝氨酸脂质体(DSPC/PS;摩尔比7:3)中,而水溶性胞壁酰二肽(MDP)则因渗漏而迅速丢失。在游离MDP无效的条件下,含有MTP-CHOL的脂质体能够刺激小鼠腹膜巨噬细胞的细胞抑制活性。在诱导大鼠肺泡巨噬细胞细胞毒活性方面,掺入脂质体的MTP-CHOL比含有包裹MDP的脂质体有效约8倍,比游离MDP有效7400倍。这些结果证明,MDP与亲脂性分子胆固醇偶联可形成一种可行的脂质体制剂,该制剂是巨噬细胞介导的抗肿瘤活性的有效诱导剂。

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