体重减轻通过激酶组重编程降低基底样乳腺癌。
Weight loss reduces basal-like breast cancer through kinome reprogramming.
作者信息
Qin Yuanyuan, Sundaram Sneha, Essaid Luma, Chen Xin, Miller Samantha M, Yan Feng, Darr David B, Galanko Joseph A, Montgomery Stephanie A, Major Michael B, Johnson Gary L, Troester Melissa A, Makowski Liza
机构信息
CB 7461, Department of Nutrition, Gillings School of Global Public Health, University of North Carolina at Chapel Hill, 2203 McGavran Greenberg Hall, Chapel Hill, NC 27599-7461 USA.
Department of Pharmacology, University of North Carolina at Chapel Hill, Chapel Hill, NC USA.
出版信息
Cancer Cell Int. 2016 Apr 1;16:26. doi: 10.1186/s12935-016-0300-y. eCollection 2016.
BACKGROUND
Obesity is associated with an aggressive subtype of breast cancer called basal-like breast cancer (BBC). BBC has no targeted therapies, making the need for mechanistic insight urgent. Reducing adiposity in adulthood can lower incidence of BBC in humans. Thus, this study investigated whether a dietary intervention to reduce adiposity prior to tumor onset would reverse HFD-induced BBC.
METHODS
Adult C3(1)-Tag mice were fed a low or high fat diet (LFD, HFD), and an obese group initially exposed to HFD was then switched to LFD to induce weight loss. A subset of mice was sacrificed prior to average tumor latency to examine unaffected mammary gland. Latency, tumor burden and progression was evaluated for effect of diet exposure. Physiologic, histology and proteomic analysis was undertaken to determine mechanisms regulating obesity and weight loss in BBC risk. Statistical analysis included Kaplan-Meier and log rank analysis to investigate latency. Student's t tests or ANOVA compared variables.
RESULTS
Mice that lost weight displayed significantly delayed latency compared to mice fed HFD, with latency matching those on LFD. Plasma leptin concentrations significantly increased with adiposity, were reduced to control levels with weight loss, and negatively correlated with tumor latency. HFD increased atypical ductal hyperplasia and ductal carcinoma in situ in mammary gland isolated prior to mean latency-a phenomenon that was lost in mice induced to lose weight. Importantly, kinome analysis revealed that weight loss reversed HFD-upregulated activity of PKC-α, PKD1, PKA, and MEK3 and increased AMPKα activity in unaffected mammary glands isolated prior to tumor latency.
CONCLUSIONS
Weight loss prior to tumor onset protected against the effects of HFD on latency and pre-neoplastic lesions including atypical ductal hyperplasia and DCIS. Using innovative kinomics, multiple kinases upstream of MAPK/P38α were demonstrated to be activated by HFD-induced weight gain and reversed with weight loss, providing novel targets in obesity-associated BBC. Thus, the HFD-exposed microenvironment that promoted early tumor onset was reprogrammed by weight loss and the restoration of a lean phenotype. Our work contributes to an understanding of underlying mechanisms associated with tumor and normal mammary changes that occur with weight loss.
背景
肥胖与一种侵袭性乳腺癌亚型——基底样乳腺癌(BBC)相关。BBC没有靶向治疗方法,因此迫切需要深入了解其发病机制。成年后减轻肥胖可降低人类患BBC的几率。因此,本研究调查了在肿瘤发生前通过饮食干预减轻肥胖是否能逆转高脂饮食诱导的BBC。
方法
给成年C3(1)-Tag小鼠喂食低脂或高脂饮食(LFD、HFD),对最初暴露于HFD的肥胖组小鼠随后改为LFD以诱导体重减轻。在平均肿瘤潜伏期之前处死一部分小鼠,以检查未受影响的乳腺。评估潜伏期、肿瘤负荷和进展情况,以了解饮食暴露的影响。进行生理、组织学和蛋白质组学分析,以确定调节肥胖和体重减轻对BBC风险影响的机制。统计分析包括Kaplan-Meier分析和对数秩分析以研究潜伏期。采用学生t检验或方差分析比较变量。
结果
与喂食HFD的小鼠相比,体重减轻的小鼠潜伏期显著延长,且潜伏期与喂食LFD的小鼠相当。血浆瘦素浓度随肥胖程度显著增加,体重减轻后降至对照水平,且与肿瘤潜伏期呈负相关。HFD增加了平均潜伏期之前分离的乳腺中的非典型导管增生和原位导管癌——这一现象在诱导体重减轻的小鼠中消失。重要的是,激酶组分析显示,体重减轻逆转了HFD上调的蛋白激酶C-α(PKC-α)、蛋白激酶D1(PKD1)、蛋白激酶A(PKA)和丝裂原活化蛋白激酶激酶3(MEK3)的活性,并增加了在肿瘤潜伏期之前分离的未受影响乳腺中的腺苷酸活化蛋白激酶α(AMPKα)活性。
结论
肿瘤发生前体重减轻可预防HFD对潜伏期和癌前病变(包括非典型导管增生和导管原位癌)的影响。通过创新的激酶组学方法,证明丝裂原活化蛋白激酶/ p38α上游的多种激酶被HFD诱导的体重增加激活,体重减轻后则逆转,这为肥胖相关的BBC提供了新的靶点。因此,促进肿瘤早期发生的HFD暴露微环境通过体重减轻和恢复瘦体型而被重新编程。我们的工作有助于理解与体重减轻相关的肿瘤和正常乳腺变化的潜在机制。
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