Inder W J, Joyce P R, Ellis M J, Evans M J, Livesey J H, Donald R A
Department of Endocrinology, Christchurch Hospital, New Zealand.
Clin Endocrinol (Oxf). 1995 Sep;43(3):283-90. doi: 10.1111/j.1365-2265.1995.tb02033.x.
Abnormal baseline hypothalamic-pituitary-adrenal axis function and dexamethasone suppressibility seen in withdrawing alcoholics returns to normal on abstinence, but some studies report blunting of the ACTH response to CRH persisting during the early abstinence phase. Reduced central levels of endogenous opioid peptides have been postulated to have an aetiological role in alcohol addiction.
To evaluate hypothalamic-pituitary-adrenal axis function in a group of recently abstinent alcoholics using basal hormone data, naloxone (an opioid receptor antagonist), and ovine CRH.
Nine alcoholics (age 41.4 +/- 3.1 years) studied more than one week after the acute withdrawal period but within 6 weeks of cessation of drinking, and nine age and sex matched non-alcoholic controls.
Cortisol, ACTH, CRH and AVP levels were measured every 20 minutes for 2 hours between 0900 and 1100h Twenty mg naloxone i.v. was administered at 1100h (0 minutes) and further samples for the above hormones were taken at 15, 30, 45, 60, 90 and 120 minutes. On a separate occasion, again at 1100h, oCRH 1 microgram/kg (n = 7 alcoholics, n = 6 controls) was administered, with samples for cortisol, ACTH and AVP taken at the same times.
Results were examined by analysis of variance for repeated measures (ANOVA), while incremental hormone response and area under the secretory curve (AUC) in alcoholics versus controls were compared by the two-tailed Student's t-test. Linear regression analysis was carried out to examine the relation between basal cortisol and hormone responses to naloxone and oCRH.
Basal hormone levels did not differ between the groups. The alcoholics had a blunted ACTH incremental response to naloxone (11.4 +/- 3.0 vs 21.1 +/- 2.5 pmol/l, P < 0.05) but the cortisol response was not significantly different (205 +/- 51 vs 305 +/- 42 nmol/l, P = 0.15). The alcoholics also had a blunted ACTH incremental response to oCRH (28.7 +/- 4.2 vs 41.2 +/- 3.7 pmol/l, P = 0.052) and by ANOVA a significant main effect of group (alcoholic vs control) was seen (P < 0.02) for the ACTH response to oCRH. There was no difference between the groups in the cortisol incremental response to oCRH. In the control subjects, a negative correlation was found between basal cortisol and the cortisol increment (r = -0.82, P < 0.05) and ACTH increment (r = -0.81, P = 0.052) following oCRH, while in contrast, basal cortisol correlated positively with cortisol increment (r = 0.72, P < 0.05) following naloxone. There was also a trend for basal cortisol to correlate positively with ACTH increment following naloxone in the controls (r = 0.63, P < 0.07). In the alcoholics, the normal negative effect of basal cortisol on the cortisol increment after oCRH was reversed, with a positive correlation between basal cortisol and cortisol increment (r = 0.75, P = 0.05).
Recently abstinent alcoholics with normal basal HPA axis hormone levels have a blunted ACTH response to naloxone and oCRH. While reduced levels of central endogenous opioid peptides may be a factor in the blunted ACTH response to naloxone in the alcoholics, it is proposed that the alcoholics have reduced pituitary responsiveness to CRH. This may be via a direct pituitary effect of the chronic ethanol exposure or by a reduction in hypothalamic-hypophyseal vasopressin levels.
戒酒者中观察到的下丘脑 - 垂体 - 肾上腺轴基线功能异常及地塞米松抑制反应在戒酒时恢复正常,但一些研究报告称在戒酒早期促肾上腺皮质激素(ACTH)对促肾上腺皮质激素释放激素(CRH)的反应迟钝仍持续存在。内源性阿片肽中枢水平降低被认为在酒精成瘾中具有病因学作用。
利用基础激素数据、纳洛酮(一种阿片受体拮抗剂)和羊CRH评估一组近期戒酒的酗酒者的下丘脑 - 垂体 - 肾上腺轴功能。
9名酗酒者(年龄41.4±3.1岁),在急性戒断期后1周以上但戒酒6周内进行研究,以及9名年龄和性别匹配的非酗酒对照者。
在09:00至11:00之间,每20分钟测量一次皮质醇、ACTH、CRH和抗利尿激素(AVP)水平,持续2小时。11:00(0分钟)静脉注射20mg纳洛酮,在15、30、45、60、90和120分钟采集上述激素的进一步样本。在另一个单独的时间,同样在11:00,给予1μg/kg的羊CRH(7名酗酒者,6名对照者),同时在相同时间采集皮质醇、ACTH和AVP的样本。
结果通过重复测量方差分析(ANOVA)进行检验,而酗酒者与对照者之间的激素增量反应和分泌曲线下面积(AUC)通过双侧Student t检验进行比较。进行线性回归分析以检查基础皮质醇与对纳洛酮和羊CRH的激素反应之间的关系。
两组之间基础激素水平无差异。酗酒者对纳洛酮的ACTH增量反应迟钝(11.4±3.0对21.1±2.5pmol/L,P<0.05),但皮质醇反应无显著差异(205±51对305±42nmol/L,P = 0.15)。酗酒者对羊CRH的ACTH增量反应也迟钝(28.7±4.2对41.2±3.7pmol/L,P = 0.052),并且通过ANOVA发现,对于对羊CRH的ACTH反应,组(酗酒者与对照者)有显著的主效应(P<0.02)。两组之间对羊CRH的皮质醇增量反应无差异。在对照受试者中,发现基础皮质醇与羊CRH后皮质醇增量(r = -0.82,P<0.05)和ACTH增量(r = -0.81,P = 0.052)之间呈负相关,而相反,基础皮质醇与纳洛酮后皮质醇增量呈正相关(r = 0.72,P<0.05)。在对照者中,基础皮质醇与纳洛酮后ACTH增量也有正相关趋势(r = 0.63,P<0.07)。在酗酒者中,基础皮质醇对羊CRH后皮质醇增量的正常负效应被逆转,基础皮质醇与皮质醇增量之间呈正相关(r = 0.75,P = 0.05)。
基础下丘脑 - 垂体 - 肾上腺轴激素水平正常的近期戒酒酗酒者对纳洛酮和羊CRH的ACTH反应迟钝。虽然中枢内源性阿片肽水平降低可能是酗酒者对纳洛酮的ACTH反应迟钝的一个因素,但有人提出酗酒者垂体对CRH的反应性降低。这可能是通过慢性乙醇暴露对垂体的直接作用或通过下丘脑 - 垂体血管加压素水平的降低。
