Design, synthesis, potency, and cytoselectivity of anticancer agents derived by parallel synthesis from alpha-aminosuberic acid

Kahnberg P; Lucke AJ; Glenn MP; Boyle GM; Tyndall JDA; Parsons PG; Fairlie DP

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Design, synthesis, potency, and cytoselectivity of anticancer agents derived by parallel synthesis from alpha-aminosuberic acid

机译：通过平行合成衍生自α-氨基异丁烯酸的抗癌药的设计，合成，效价和细胞选择性

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Chemotherapy in the last century was characterized by cytotoxic drugs that did not discriminate between cancerous and normal cell types and were consequently accompanied by toxic side effects that were often dose limiting. The ability of differentiating agents to selectively kill cancer cells or transform them to a nonproliferating or normal phenotype could lead to cell- and tissue-specific drugs without the side effects of current cancer chemotherapeutics. This may be possible for a new generation of histone deacetylase inhibitors derived from amino acids. Structure-activity relationships are now reported for 43 compounds derived from 2-aminosuberic acid that kill a range of cancer cells, 26 being potent cytotoxins against MM96L melanoma cells (IC50 20 nM-1 mu M), while 17 were between 5- and 60-fold more selective in killing MM96L melanoma cells versus normal (neonatal foreskin fibroblasts, NFF) cells. This represents a 10- to 100-fold increase in potency and up to a 10-fold higher selectivity over previously reported compounds derived from cysteine (J. Med. Chem. 2004, 47, 2984). Selectivity is also an underestimate, because the normal cells, NFF, are rarely all killed by the drugs that also induce selective blockade of the cell cycle for normal but not cancer cells. Selected compounds were tested against a panel of human cancer cell lines (melanomas, prostate, breast, ovarian, cervical, lung, and colon) and found to be both selective and potent cytotoxins (IC50 20 nM-1 mu M). Compounds in this class typically inhibit human histone deacetylases, as evidenced by hyperacetylation of histones in both normal and cancer cells, induce expression of p21, and differentiate surviving cancer cells to a nonproliferating phenotype. These compounds may be valuable leads for the development of new chemotherapeutic agents.

机译：上个世纪的化学疗法的特点是细胞毒性药物不能区分癌性细胞和正常细胞类型，因此伴有经常限制剂量的毒性副作用。分化剂选择性杀死癌细胞或将其转化为非增殖或正常表型的能力可能导致细胞和组织特异性药物的产生，而没有当前癌症化学疗法的副作用。对于衍生自氨基酸的新一代组蛋白脱乙酰基酶抑制剂来说，这可能是可能的。现在报道了43种衍生自2-氨基磺酸的化合物的结构-活性关系，这些化合物杀死了一系列癌细胞，其中26种是针对MM96L黑色素瘤细胞的有效细胞毒素（IC50 20 nM-1μM），而17种在5至60之间杀MM96L黑色素瘤细胞的选择性比正常（新生儿包皮成纤维细胞，NFF）细胞高两倍。与先前报道的衍生自半胱氨酸的化合物相比，这表示效力增加了10至100倍，并且选择性提高了多达10倍（J. Med。Chem。2004，47，2984）。选择性也被低估了，因为正常细胞NFF很少会被药物杀死，这些药物也会诱导选择性阻断正常细胞而不是癌细胞的细胞周期。针对一组人类癌细胞系（黑素瘤，前列腺癌，乳腺癌，卵巢癌，宫颈癌，肺癌和结肠癌）测试了选定的化合物，发现它们既是选择性的也是有效的细胞毒素（IC50 20 nM-1μM）。此类化合物通常可抑制人组蛋白脱乙酰基酶，如正常细胞和癌细胞中组蛋白的超乙酰化所证明的那样，可诱导p21的表达，并使尚存的癌细胞分化为非增殖表型。这些化合物可能是开发新化学治疗剂的有价值的线索。

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《Journal of Medicinal Chemistry 》 |2006年第26期| 共12页
作者
Kahnberg P; Lucke AJ; Glenn MP; Boyle GM; Tyndall JDA; Parsons PG; Fairlie DP;
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正文语种 eng
中图分类药学 ;
关键词
HISTONE DEACETYLASE INHIBITORS; SUBEROYLANILIDE HYDROXAMIC ACID; TUMOR-CELLS; CYCLIC TETRAPEPTIDE; TRICHOSTATIN-A; HUMAN HDAC8; DIFFERENTIATION; CANCER; ANALOGS; FAMILY;

机译：组蛋白去乙酰化酶抑制剂;羟丙二酸氢羟酸;肿瘤细胞;环四肽;曲古他汀-A;人HDAC8;分化;癌症;类似物;家族;

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机译：通过平行合成衍生自α-氨基异丁烯酸的抗癌药的设计，合成，效价和细胞选择性
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4. Enzymatic Synthesis of Glycerol and Sucrose-Palm Oil Fatty Acid Esters Produced and Their Potency as Antimicrobial Agents [C] . R. A. Naulidia, E. Juliana, S. Handayani, International Conference of the Indonesian Chemical Society . 2020

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Design, synthesis, potency, and cytoselectivity of anticancer agents derived by parallel synthesis from alpha-aminosuberic acid

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