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Cognitive Effects of Cancer and its Treatments at the Intersection of Aging: What do we Know; What do we Need to Know?

机译:衰老过程中癌症及其治疗的认知作用:我们知道什么;我们需要知道什么?

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There is a fairly consistent, albeit non-universal body of research documenting cognitive declines after cancer and its treatments. While few of these studies have included those 65 and older, it is logical to expect that older patients are at risk of cognitive decline. In this paper, we use breast cancer as an exemplar disease for inquiry into the intersection of aging and cognitive effects of cancer and its therapies. There are a striking number of common underlying potential biological risks and pathways for the development of cancer, cancer-related cognitive declines, and aging processes, including the development of a frail phenotype. Candidate shared pathways include changes in hormonal milieu, inflammation, oxidative stress, DNA damage and compromised DNA repair, genetic susceptibility, decreased brain blood flow or disruption of the blood-brain barrier, direct neurotoxicity, decreased telomere length, and cell senescence. There are also similar structure and functional changes seen in brain imaging studies of cancer patients and those seen with “normal” aging and Alzheimer’s disease. Disentangling the role of these overlapping processes is difficult since they require aged animal models and large samples of older human subjects. From what we do know, frailty and its low cognitive reserve seem to be a clinically useful marker of risk for cognitive decline after cancer and its treatments. This and other results from this review suggest the value of geriatric assessments to identify older patients at the highest risk of cognitive decline. Further research is needed to understand the interactions between aging, genetic predisposition, lifestyle factors and frailty phenotypes to best identify the sub-groups of older patients at greatest risk for decline and to develop behavioral and pharmacological interventions targeting this group. We recommend that basic science and population trials be developed specifically for older hosts with intermediate endpoints of relevance to this group, including cognitive function and trajectories of frailty. Clinicians and their older patients can advance the field by active encouragement of and participation in research designed to improve the care and outcomes of the growing population of older cancer patients.
机译:有相当一致的,尽管不是普遍的研究,记录了癌症及其治疗后认知能力下降。尽管这些研究中很少有65岁及以上的研究,但可以合理地预期,老年患者有认知下降的风险。在本文中,我们将乳腺癌作为一种典型疾病,用于研究癌症及其疗法对衰老和认知作用的影响。癌症的发展,与癌症相关的认知能力下降和衰老过程(包括脆弱表型的发展)有许多常见的潜在潜在生物学风险和途径。共有的候选途径包括激素环境变化,炎症,氧化应激,DNA损伤和受损的DNA修复,遗传易感性,脑血流量减少或血脑屏障破坏,直接神经毒性,端粒长度减少和细胞衰老。在癌症患者和“正常”衰老和阿尔茨海默氏病患者的脑成像研究中,也观察到了相似的结构和功能变化。很难区分这些重叠过程的作用,因为它们需要年龄较大的动物模型和较大年龄的人体样本。据我们所知,虚弱及其低的认知储备似乎是癌症及其治疗后认知衰退风险的临床有用标志。这项审查的结果和其他结果表明,老年病评估的价值对识别认知下降风险最高的老年患者具有重要意义。需要进一步的研究来了解衰老,遗传易感性,生活方式因素和脆弱表型之间的相互作用,以最好地识别出下降风险最大的老年患者亚组,并针对该组制定行为和药物干预措施。我们建议基础科学和人口试验专门针对年龄较晚的宿主而开发,这些宿主的中间终点与该人群有关,包括认知功能和身体虚弱的轨迹。临床医生及其老年患者可以通过积极鼓励和参与旨在改善日益增长的老年癌症患者群体的护理和治疗效果的研究来推动这一领域的发展。

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