Abstract 2580: Synergistic effect of magnesium with metformin for the prevention of liver and colorectal cancer

L. Fan, D. Yu, Xiangzhu Zhu, Xuehong Zhang, Xiang Huang, H. Murff, M. Azcarate-Peril, M. Shrubsole, Q. Dai
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Abstract

The obesity epidemic has dramatically increased the type 2 diabetes (T2D) prevalence in the US over the past two decades. Previous studies have relatively consistently found individuals with T2D are at increased risks of cancer, including liver and colorectal cancer in which insulin resistance may play an important role. However, the mechanism remains largely unknown. Metformin, the primary first-line medication for the treatment of T2D, has been shown to improve insulin resistance and be linked to a reduced risk of hepatocellular carcinoma (HCC) and colorectal cancer (CRC). Two recent Cell and Cell metabolism publications identified that imidazole propionate (ImP), a microbial metabolite of histidine, significantly increased in patients with T2D and causally induced insulin resistance in mice. Furthermore, the therapeutic effects of metformin on insulin resistance disappeared when ImP was elevated, indicating that ImP plays a key role in developing insulin resistance and resistance to metformin treatment. Our recent work together with a subsequent study from others demonstrated higher magnesium (Mg) intake is associated with a substantially reduced risk of HCC, HCC mortality and mortality from liver diseases. Accumulative evidence, including our prior work, has also linked higher Mg intake to a reduced risk of colorectal neoplasia. Previous studies found that the process of the histidine utilization (Hut) system to metabolize histidine in some bacterial taxa depends on concentrations of divalent metal ion Mg2+. We hypothesize that low availability of Mg2+ in gut microbiota could terminate the Hut system and increase the production of intermediate metabolites, including ImP, over other end products. This will lead to increased levels of ImP in the gut and, in turn, liver and circulation. We tested our hypothesis in the Personalized Prevention of Colorectal Cancer Trial (PPCCT) (registered at clinicaltrials.gov as NCT01105169), a precision-based randomized trial enrolling 240 participants at high risk of Mg deficiency. Among 68 participants (34 treatment/34 placebo), we found that compared to the placebo, Mg treatment significantly reduced ImP by 39.9% compared to a 6.0% increase in the placebo arm after adjustment for baseline ImP (P=0.02). However, we found Mg treatment did not significantly affect the levels of trans-urocanate, the precursor of ImP. Since Mg deficiency leads to insulin resistance and as high as 50% of patients with T2D have hypomagnesemia, Mg deficiency may lead to an increased risk of ImP and, in turn, resistance to metformin which subsequently increases risk of HCC and CRC. Thus, futures studies should evaluate whether the joint use of Mg supplementation and metformin synergistically maximizes the efficacy of metformin and minimizes the treatment resistance on insulin resistance and, subsequently, prevention of HCC and CRC. Citation Format: Lei Fan, Danxia Yu, Xiangzhu Zhu, Xuehong Zhang, Xiang Huang, Harvey J. Murff, M. Andrea Azcarate-Peril, Martha J. Shrubsole, Qi Dai. Synergistic effect of magnesium with metformin for the prevention of liver and colorectal cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 2580.
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摘要:镁与二甲双胍在预防肝癌和结直肠癌中的协同作用
在过去的二十年里,肥胖的流行极大地增加了美国2型糖尿病(T2D)的患病率。先前的研究相对一致地发现,患有T2D的个体患癌症的风险增加,包括肝癌和结直肠癌,其中胰岛素抵抗可能起重要作用。然而,其机制在很大程度上仍然未知。二甲双胍是治疗T2D的主要一线药物,已被证明可以改善胰岛素抵抗,并与降低肝细胞癌(HCC)和结直肠癌(CRC)的风险有关。最近的两篇Cell和Cell metabolism出版物发现,组氨酸的微生物代谢物咪唑丙酸酯(ImP)在T2D患者中显著增加,并在小鼠中引起胰岛素抵抗。此外,当ImP升高时,二甲双胍对胰岛素抵抗的治疗作用消失,表明ImP在胰岛素抵抗和二甲双胍治疗抵抗中起关键作用。我们最近的工作和其他人随后的研究表明,较高的镁(Mg)摄入量与HCC风险、HCC死亡率和肝脏疾病死亡率的显著降低相关。累积的证据,包括我们之前的工作,也将较高的镁摄入量与降低结直肠肿瘤的风险联系起来。以往的研究发现,在某些细菌类群中,组氨酸利用(Hut)系统代谢组氨酸的过程取决于二价金属离子Mg2+的浓度。我们假设,肠道微生物群中Mg2+的低利用率可能会终止Hut系统,并增加中间代谢物(包括ImP)的产生,而不是其他最终产物。这将导致肠道内ImP水平的增加,进而导致肝脏和血液循环的增加。我们在个体化预防结直肠癌试验(PPCCT)(在clinicaltrials.gov注册为NCT01105169)中验证了我们的假设,这是一项基于精确的随机试验,招募了240名镁缺乏症高风险参与者。在68名参与者中(34名治疗组/34名安慰剂组),我们发现与安慰剂组相比,Mg治疗组在调整基线ImP后显着降低了39.9%,而安慰剂组则增加了6.0% (P=0.02)。然而,我们发现Mg治疗并没有显著影响ImP的前体反式尿毒酸的水平。由于Mg缺乏导致胰岛素抵抗,高达50%的T2D患者有低镁血症,Mg缺乏可能导致ImP的风险增加,进而导致对二甲双胍的抵抗,从而增加HCC和CRC的风险。因此,未来的研究应该评估Mg补充剂和二甲双胍联合使用是否能协同最大化二甲双胍的疗效,最小化对胰岛素抵抗的治疗抵抗,从而预防HCC和CRC。引用格式:范磊,于丹霞,朱祥珠,张雪红,黄翔,Harvey J. Murff, M. Andrea Azcarate-Peril, Martha J. Shrubsole,戴琦。镁与二甲双胍预防肝癌和结直肠癌的协同作用[摘要]。见:美国癌症研究协会2021年年会论文集;2021年4月10日至15日和5月17日至21日。费城(PA): AACR;癌症杂志,2021;81(13 -增刊):2580。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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