一年的生长激素替代疗法不会改变生长激素缺乏的成年人的结肠上皮细胞增殖。
One year growth hormone replacement therapy does not alter colonic epithelial cell proliferation in growth hormone deficient adults.
作者信息
Beentjes J A, van Gorkom B A, Sluiter W J, de Vries E G, Kleibeuker J H, Dullaart R P
机构信息
Department of Internal Medicine, Divisions of; Endocrinology, University Hospital Groningen, The Netherlands.
出版信息
Clin Endocrinol (Oxf). 2000 Apr;52(4):457-62. doi: 10.1046/j.1365-2265.2000.00993.x.
OBJECTIVE
Increased colonic epithelial cell proliferation has been found in various conditions associated with increased risk of colorectal cancer including acromegaly. In a placebo-controlled study we determined the effect of growth hormone (GH) replacement therapy in GH deficient adults on the colonic epithelial proliferation rate.
PATIENTS AND DESIGN
Sixteen GH deficient adults were randomised to low dose GH therapy (1 U (0.5 mg) subcutaneously per day, n = 5), high dose GH therapy (2 U daily, n = 5) or placebo (n = 6) during 6 months. Thereafter, all patients were treated with 2 U of GH daily during a 6-months open extension period.
MEASUREMENTS
Plasma Insulin-like growth hormone I (IGF-I) and IGF binding protein 3 (IGF BP3) concentrations were measured using commercial RIA kits. The colonic epithelial proliferation rate, expressed as overall crypt labelling index (LI) using 5-bromo-2'-deoxyuridine (BrdU) immunostaining, was determined at baseline, after 6 months treatment and at the end of the 6 months open extension period.
RESULTS
IGF-I rose from 8.9 +/- 6.7 to 34.6 +/- 20.0 nmol/l after 6 months in 8 GH treated patients (P < 0.01 from baseline; P < 0.01 from change with placebo). In the extension study, plasma IGF-I was also increased in the patients who previously received placebo (P < 0.02, n = 5). LI was evaluable in 14 biopsies at baseline, in 16 after 6 months and in 14 after 12 months. Overall crypt LI did not change in 8 GH treated patients after 6 months (P > 0.40 from baseline; P > 0.80 from change with placebo). In the extension study, overall crypt LI was also unchanged in those patients who received GH after placebo (n = 5, P > 0.40) and in those who continued GH replacement (n = 9, P > 0.60; P > 0.80 from change in initially placebo treated patients). Separate evaluation of the LI at the basal, mid and luminal portions of the colonic crypts also did not reveal any effect of GH treatment on BrdU labelling.
CONCLUSIONS
Six to 12 months of GH replacement therapy, aimed to increase plasma IGF-I into the (high) physiological range, does not adversely affect colonic epithelial cell proliferation as a biomarker for the risk of development of colorectal cancer.
目的
在包括肢端肥大症在内的多种与结直肠癌风险增加相关的病症中,已发现结肠上皮细胞增殖增加。在一项安慰剂对照研究中,我们确定了生长激素(GH)替代疗法对GH缺乏的成年人结肠上皮增殖率的影响。
患者与设计
16名GH缺乏的成年人在6个月内被随机分为低剂量GH治疗组(每天皮下注射1 U(0.5 mg),n = 5)、高剂量GH治疗组(每天2 U,n = 5)或安慰剂组(n = 6)。此后,在6个月的开放延长期内,所有患者均接受每天2 U的GH治疗。
测量指标
使用商业放射免疫分析试剂盒测量血浆胰岛素样生长激素I(IGF-I)和IGF结合蛋白3(IGF BP3)浓度。在基线、治疗6个月后和6个月开放延长期结束时,使用5-溴-2'-脱氧尿苷(BrdU)免疫染色,以总隐窝标记指数(LI)表示结肠上皮增殖率。
结果
8名接受GH治疗的患者在6个月后IGF-I从8.9±6.7 nmol/l升至34.6±20.0 nmol/l(与基线相比P < 0.01;与安慰剂组变化相比P < 0.01)。在延长期研究中,先前接受安慰剂治疗的患者血浆IGF-I也升高(P < 0.02,n = 5)。基线时14份活检标本可评估LI,6个月后16份,12个月后14份。8名接受GH治疗的患者在6个月后总隐窝LI未改变(与基线相比P > 0.40;与安慰剂组变化相比P > 0.80)。在延长期研究中,接受安慰剂后再接受GH治疗的患者(n = 5,P > 0.40)以及继续接受GH替代治疗的患者(n = 9,P > 0.60;与最初接受安慰剂治疗患者的变化相比P > 0.80)总隐窝LI也未改变。对结肠隐窝底部、中部和管腔部分的LI进行单独评估也未发现GH治疗对BrdU标记有任何影响。
结论
旨在将血浆IGF-I提高到(高)生理范围内的6至12个月GH替代疗法,作为结直肠癌发生风险的生物标志物,不会对结肠上皮细胞增殖产生不利影响。
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