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Dietary geranylgeraniol can limit the activity of pitavastatin as a potential treatment for drug-resistant ovarian cancer

机译:饮食中的香叶基香叶醇可限制匹伐他汀的活性作为抗药性卵巢癌的潜在治疗方法

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摘要

Pre-clinical and retrospective studies of patients using statins to reduce plasma cholesterol have suggested that statins may be useful to treat cancer. However, prospective clinical trials have yet to demonstrate significant efficacy. We have previously shown that this is in part because a hydrophobic statin with a long half-life is necessary. Pitavastatin, the only statin with this profile, has not undergone clinical evaluation in oncology. The target of pitavastatin, hydroxymethylglutarate coenzyme-A reductase (HMGCR), was found to be over-expressed in all ovarian cancer cell lines examined and upregulated by mutated TP53, a gene commonly altered in ovarian cancer. Pitavastatin-induced apoptosis was blocked by geranylgeraniol and mevalonate, products of the HMGCR pathway, confirming that pitavastatin causes cell death through inhibition of HMGCR. Solvent extracts of human and mouse food were also able to block pitavastatin-induced apoptosis, suggesting diet might influence the outcome of clinical trials. When nude mice were maintained on a diet lacking geranylgeraniol, oral pitavastatin caused regression of Ovcar-4 tumour xenografts. However, when the animal diet was supplemented with geranylgeraniol, pitavastatin failed to prevent tumour growth. This suggests that a diet containing geranylgeraniol can limit the anti-tumour activity of pitavastatin and diet should be controlled in clinical trials of statins.
机译:使用他汀类药物降低血浆胆固醇的患者的临床前和回顾性研究表明,他汀类药物可能对治疗癌症有用。但是,前瞻性临床试验尚未显示出明显的疗效。先前我们已经表明,这部分是因为具有长半衰期的疏水性他汀类药物是必需的。匹伐他汀是唯一具有这种特征的他汀类药物,尚未经过肿瘤学的临床评估。发现匹伐他汀的靶标羟甲基戊二酸辅酶A还原酶(HMGCR)在所有卵巢癌细胞系中均过表达,而TP53突变是卵巢癌中普遍改变的一种基因,该细胞系被上调。匹伐他汀诱导的细胞凋亡被HMGCR途径的香叶基香叶基香叶醇和甲羟戊酸所阻断,证实匹伐他汀通过抑制HMGCR导致细胞死亡。人类和小鼠食物的溶剂提取物也能够阻断匹伐他汀诱导的细胞凋亡,这表明饮食可能会影响临床试验的结果。当裸鼠维持缺乏香叶基香叶醇的饮食时,口服匹伐他汀会导致Ovcar-4肿瘤异种移植物退化。然而,当动物饮食中添加香叶基香叶醇时,匹伐他汀不能阻止肿瘤的生长。这表明含香叶基香叶醇的饮食可限制匹伐他汀的抗肿瘤活性,应在他汀类药物的临床试验中控制饮食。

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