使用尼古丁和青春期对青少年 C 反应蛋白水平影响的性别差异:超越逆境的影响

IF 3.7 Q2 IMMUNOLOGY
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引用次数: 0

摘要

炎症可能是尼古丁使用与不良健康后果之间的中介。在尼古丁的使用与炎症的联系中已经观察到了性别差异,而青春期的生理过程可能会导致这些差异的产生。在这项针对 498 名青少年(8-13 岁,52% 为女孩,77% 有儿童虐待(CM)调查史)的横断面研究中,探讨了自我报告的尼古丁使用情况与高敏 C 反应蛋白(hs-CRP)之间的性别差异。此外,还研究了自我报告的青春期阶段对尼古丁使用与高敏C反应蛋白之间关系的调节作用。分层广义估计方程模型对各种逆境效应进行了调整:根据州记录得出的 CM 调查史、自我和照顾者对创伤性生活事件的报告、与逆境相关的人口风险因素(即对历史上被边缘化的种族和民族群体的认同、家庭收入)以及可能影响相关变量的其他特征(如药物使用、年龄、体重指数)。尼古丁的使用对男孩的 hs-CRP 有负主效应(β = -0.50,p = 0.02),而青春期阶段并没有缓和这种关联(β = 0.06,p = 0.71)。与此相反,青春期阶段对女孩使用尼古丁与 hs-CRP 之间的关系有调节作用(β = 0.48,p = 0.02),因此在青春期阶段越高,使用尼古丁与 hs-CRP 水平之间的正相关关系越强(β = 0.45,SE = 0.21,95% CI [0.03,0.87])。研究结果表明,青春期可能会以性别差异的方式影响尼古丁对炎症的作用,并对旨在减少青少年使用尼古丁及随后与炎症相关的健康风险的预防和治疗工作的时机选择产生影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Sex differences in the roles of nicotine use and puberty on youth C-reactive protein levels: Effects above and beyond adversity

Inflammation likely mediates associations between nicotine use and negative health outcomes. Sex differences have been observed in nicotine use–inflammation links, and physiological processes during puberty might allow for these differences to arise. In this cross-sectional study of 498 youth (ages 8–13, 52% girls, 77% with history of child maltreatment (CM) investigation), sex-differentiated associations between self-reported nicotine use and high-sensitivity C-reactive protein (hs-CRP) were explored. Additionally, self-reported pubertal stage was investigated as a moderator of such nicotine use–hs-CRP links. Hierarchical generalized estimating equation models were adjusted for a wide range of adversity effects: CM investigation history derived from state records, self- and caregiver-report of traumatic life events, adversity-related demographic risk factors (i.e., identification with historically marginalized racial and ethnic groups, household income), and other characteristics that may influence the variables of interest (e.g., medication use, age, body mass index). Nicotine use had a negative main effect on hs-CRP among boys (β = −0.50, p = 0.02), and pubertal stage did not moderate this association (β = 0.06, p = 0.71). In contrast, pubertal stage moderated the association between nicotine use and hs-CRP among girls (β = 0.48, p = 0.02) such that a positive association between nicotine use and hs-CRP levels was stronger at more advanced pubertal stages (β = 0.45, SE = 0.21, 95% CI [0.03, 0.87]). Findings suggest that puberty may influence the effect of nicotine on inflammation in sex-differentiated ways and have implications for timing of prevention and treatment efforts geared toward reducing nicotine use and subsequent inflammation-related health risk among youth.

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来源期刊
Brain, behavior, & immunity - health
Brain, behavior, & immunity - health Biological Psychiatry, Behavioral Neuroscience
CiteScore
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97 days
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