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Design and Preparation of a 4:1 Lamivudine?Oxalic Acid CAB Cocrystal for Improving the Lamivudine Purification Process

机译:4:1拉米夫定?草酸CAB共结晶的设计与制备,以改善拉米夫定的纯化工艺

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摘要

Lamivudine (LMV), a cytosine derivative and a reverse transcriptase inhibitor, faces the challenge of inefficient purification after its chemical synthesis. Currently available methods of purification involve salt formation (salicylate or oxalate) followed by treatment with a toxic base, triethyl amine (TEA), to neutralize the protonated LMV. Any reduction in the use of TEA will make the purification process greener and more economical. In this context, we designed and successfully isolated a new and elusive 4:1 CAB cocrystal between LMV and oxalic acid (OXA) that has the potential to significantly improve the efficiency of the LMV purification process. The new CAB cocrystal of LMV was efficiently produced by carefully controlling the ratio of LMV to OXA in the crystallization medium. Compared to salts currently used for purification, much less TEA is required for the 4:1 CAB cocrystal (LMV/LMVH~+/ OXA~(2?) at 2:2:1 mole ratio) because only half of the LMV is protonated that requires TEA treatment.
机译:拉米夫定(LMV)是一种胞嘧啶衍生物和一种逆转录酶抑制剂,其化学合成后面临着纯化效率低下的挑战。当前可用的纯化方法包括成盐(水杨酸盐或草酸盐),然后用有毒碱三乙胺(TEA)处理以中和质子化的LMV。减少TEA的使用将使纯化过程更绿色,更经济。在这种情况下,我们设计并成功地分离了LMV和草酸(OXA)之间新的和难以捉摸的4:1 CAB共晶体,该晶体有可能显着提高LMV纯化过程的效率。通过仔细控制结晶介质中LMV与OXA的比例,可以有效地生产LMV的新型CAB共结晶。与目前用于纯化的盐相比,4:1 CAB共晶所需的TEA少得多(LMV / LMVH〜+ / OXA〜(2?)摩尔比为2:2:1),因为只有一半的LMV是质子化的需要TEA治疗。

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