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鉴定和临床前研究 3-O-环己烷甲酰基-11-酮-β-乳香酸作为一种外用药物治疗银屑病。

Identification and pre-clinical investigation of 3-O-cyclohexanecarbonyl-11-keto-β-boswellic acid as a drug for external use to treat psoriasis.

机构信息

Precision Research Center for Refractory Diseases, Shanghai General Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, China.

BCY Pharm Co., Ltd., Suzhou, China.

出版信息

Br J Pharmacol. 2024 Apr;181(8):1290-1307. doi: 10.1111/bph.16253. Epub 2024 Jan 11.

DOI:10.1111/bph.16253
PMID:37749894
Abstract

BACKGROUND AND PURPOSE

Psoriasis vulgaris is a refractory skin inflammatory disorder with 80% of the cases belonging to the mild-to-moderate type, which can be controlled by topical treatment. Nevertheless, the drugs for external use have not been upgraded for decades. We modified acetyl-11-keto-beta-boswellic acid (ABKA), a natural compound shown to treat psoriasis animal models, to improve efficacy and solubility for topical use.

EXPERIMENTAL APPROACH

Eleven compounds were synthesized using AKBA as a lead compound, and their effects on Th17 cell differentiation were screened. 3-O-cyclohexanecarbonyl-11-keto-β-boswellic acid (CKBA) potently inhibited Th17 cell differentiation. Its efficacy in a mouse model of psoriasis was assessed along with its pharmacology and safety profile when topically or systemically delivered to several animal species.

KEY RESULTS

CKBA inhibited mouse and human Th17 cell differentiation with an IC of 3.28 and 3.61 μM, respectively, and directly targeted acetyl-CoA carboxylase 1 (ACC1). Safety evaluation and toxicity tests suggested that systemically delivered high-dose CKBA for 14 days had no dose-associated adverse effects on the CNS, haematopoietic, cardiovascular, respiratory and digestive systems of cynomolgus monkeys. CKBA ointment permeated the skin and did not irritate or sensitize intact skin. CKBA ointment mediated dose-dependent suppression of imiquimod-induced psoriasis-like skin inflammation with slow absorption and limited bioavailability (<10% in rats and <1% in minipigs).

CONCLUSIONS AND IMPLICATIONS

CKBA is safe when topically or systemically delivered to animals. The beneficial effects of CKBA ointment in a mouse model of psoriasis indicate that this is a promising drug candidate for further development as a treatment for psoriasis.

摘要

背景与目的

寻常型银屑病是一种难治性皮肤炎症性疾病,其中 80%的病例属于轻中度,可通过局部治疗控制。然而,外用药物几十年来并未得到升级。我们对乙酰-11-酮-β-乳香酸(ABKA)进行了修饰,该化合物已被证明可用于治疗银屑病动物模型,以提高其治疗效果和外用溶解度。

实验方法

以 AKBA 为先导化合物合成了 11 种化合物,并筛选了它们对 Th17 细胞分化的影响。3-O-环己烷甲酰基-11-酮-β-乳香酸(CKBA)能有效抑制 Th17 细胞分化。评估了 CKBA 在银屑病小鼠模型中的疗效,以及当局部或全身给药于几种动物物种时的药理学和安全性特征。

主要结果

CKBA 抑制小鼠和人 Th17 细胞分化的 IC50 分别为 3.28 和 3.61μM,并且直接靶向乙酰辅酶 A 羧化酶 1(ACC1)。安全性评估和毒性试验表明,在恒河猴中系统给予高剂量 CKBA 长达 14 天,不会引起与剂量相关的中枢神经系统、造血、心血管、呼吸和消化系统不良反应。CKBA 软膏能渗透皮肤,不会刺激或致敏完整皮肤。CKBA 软膏介导的咪喹莫特诱导的银屑病样皮肤炎症呈剂量依赖性抑制,吸收缓慢,生物利用度有限(大鼠<10%,小型猪<1%)。

结论和意义

CKBA 经皮或全身给药对动物安全。CKBA 软膏在银屑病小鼠模型中的有益作用表明,这是一种很有前途的候选药物,可进一步开发用于治疗银屑病。

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