Seco-cyclic phorbol derivatives and their anti-HIV-1 activities

IF 4 2区 医学 Q1 INTEGRATIVE & COMPLEMENTARY MEDICINE Chinese Journal of Natural Medicines Pub Date : 2024-04-01 DOI:10.1016/S1875-5364(24)60630-8
Xiaolei HUANG , Xusheng HUANG , Qirun LI , Mengdi MA , Yadong CUI , Liumeng YANG , Haibo WANG , Ronghua LUO , Jinglei CHEN , Jingxuan YANG , Jinrong LIN , Duxin LI , Yongtang ZHENG , Jian ZHANG
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Abstract

Phorbol esters are recognized for their dual role as anti-HIV-1 agents and as activators of protein kinase C (PKC). The efficacy of phorbol esters in binding with PKC is attributed to the presence of oxygen groups at positions C20, C3/C4, and C9 of phorbol. Concurrently, the lipids located at positions C12/C13 are essential for both the anti-HIV-1 activity and the formation of the PKC-ligand complex. The influence of the cyclopropane ring at positions C13 and C14 in phorbol derivatives on their anti-HIV-1 activity requires further exploration. This research entailed the hydrolysis of phorbol, producing seco-cyclic phorbol derivatives. The anti-HIV-1 efficacy of these derivatives was assessed, and the affinity constant (Kd) for PKC-δ protein of selected seco-cyclic phorbol derivatives was determined through isothermal titration calorimetry. The findings suggest that the chemical modification of cyclopropanols could affect both the anti-HIV-1 activity and the PKC binding affinity. Remarkably, compound S11, with an EC50 of 0.27 μmol·L−1 and a CC50 of 153.92 μmol·L−1, demonstrated a potent inhibitory effect on the intermediate products of HIV-1 reverse transcription (ssDNA and 2LTR), likely acting at the viral entry stage, yet showed no affinity for the PKC-δ protein. These results position compound S11 as a potential candidate for further preclinical investigation and for studies aimed at elucidating the pharmacological mechanism underlying its anti-HIV-1 activity.

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仲环植物醇衍生物及其抗 HIV-1 活性
薄荷醇酯被认为具有双重作用,既可作为抗 HIV-1 药物,又可作为蛋白激酶 C(PKC)的激活剂。薄荷醇酯之所以能与 PKC 结合,是因为在薄荷醇的 C20、C3/C4 和 C9 位置存在氧基。同时,位于 C12/C13 位的脂质对于抗 HIV-1 活性和 PKC 配体复合物的形成都至关重要。至于山梨醇衍生物中位于 C13 和 C14 位置的环丙烷环对其抗 HIV-1 活性的影响,还需要进一步探讨。这项研究需要对植物醇进行水解,生成仲环植物醇衍生物。评估了这些衍生物的抗 HIV-1 效能,并通过等温滴定量热法测定了所选的仲环辛醇衍生物对 PKC-δ 蛋白的亲和力常数(Kd)。研究结果表明,环丙醇的化学修饰会影响其抗 HIV-1 活性和 PKC 结合亲和力。值得注意的是,化合物 S11 的 EC50 值为 0.27 μmol-L-1,CC50 值为 153.92 μmol-L-1,它对 HIV-1 逆转录的中间产物(ssDNA 和 2LTR)有很强的抑制作用,可能在病毒进入阶段发挥作用,但对 PKC-δ 蛋白却没有亲和力。这些结果将化合物 S11 定位为进一步临床前研究和旨在阐明其抗 HIV-1 活性药理机制的研究的潜在候选药物。
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来源期刊
Chinese Journal of Natural Medicines
Chinese Journal of Natural Medicines INTEGRATIVE & COMPLEMENTARY MEDICINE-PHARMACOLOGY & PHARMACY
CiteScore
7.50
自引率
4.30%
发文量
2235
期刊介绍: The Chinese Journal of Natural Medicines (CJNM), founded and sponsored in May 2003 by China Pharmaceutical University and the Chinese Pharmaceutical Association, is devoted to communication among pharmaceutical and medical scientists interested in the advancement of Traditional Chinese Medicines (TCM). CJNM publishes articles relating to a broad spectrum of bioactive natural products, leading compounds and medicines derived from Traditional Chinese Medicines (TCM). Topics covered by the journal are: Resources of Traditional Chinese Medicines; Interaction and complexity of prescription; Natural Products Chemistry (including structure modification, semi-and total synthesis, bio-transformation); Pharmacology of natural products and prescription (including pharmacokinetics and toxicology); Pharmaceutics and Analytical Methods of natural products.
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