Plöckinger U, Liehr R M, Quabbe H J
Department of Endocrinology, Klinikum Steglitz, Freie Universität, Berlin, Germany.
J Clin Endocrinol Metab. 1993 Jul;77(1):157-62. doi: 10.1210/jcem.77.1.8325938.
We studied a possible persistence of low GH concentrations after drug withdrawal in eight acromegalic patients who had been receiving octreotide treatment continuously for 42 months. Since octreotide induces chronic active gastritis, intragastric pH and serum gastrin were also determined before and during drug withdrawal. Results were compared to the respective pretreatment (pre-Tx) values. GH and insulin-like growth factor-I (IGF-I) increased after 4 weeks of octreotide withdrawal to pre-Tx values (GH, 12-h profile, 4.5 +/- 0.6, 2.6 +/- 0.7, and 5.6 +/- 1.1 micrograms/L; IGF-I, three samples, 3.4 +/- 0.4, 0.8 +/- 0.1, and 2.5 +/- 1.0 IU x 10(3)/L; means +/- SE, pre-Tx, on and off octreotide). A reduced insulin and augmented glucose response to oral glucose during therapy normalized after octreotide withdrawal (insulin, 527 +/- 84, 289 +/- 62, and 733 +/- 110 pmol/L; glucose, 6.2 +/- 0.3, 8.5 +/- 0.4, and 6.8 +/- 0.2 mmol/L; pre-Tx, on and off octreotide, means +/- SE). During octreotide treatment, the median 24-h intragastric pH value was 2.8 (pre-Tx pH not determined), and the median serum gastrin concentration (areas under the curve of 12-h profiles) was 1275 +/- 153 ng/L.12 h (n = 7). During octreotide withdrawal, pH decreased to 1.4, while serum gastrin increased to a median of 2937 +/- 472 ng/L.12 h. We conclude that GH and IGF-I suppression by long term octreotide therapy does not persist after drug withdrawal, indicating a need for life-long treatment. Octreotide-induced insulin suppression and glucose elevation are reversible. A high gastric pH during treatment may facilitate the development of octreotide-related gastritis. The gastrin increase during octreotide withdrawal probably reflects a response to chronic active gastritis after release from octreotide-induced gastrin inhibition.
我们研究了8例肢端肥大症患者在持续接受奥曲肽治疗42个月后停药后低生长激素(GH)浓度可能的持续性。由于奥曲肽可诱发慢性活动性胃炎,因此在停药前和停药期间还测定了胃内pH值和血清胃泌素水平。将结果与各自的治疗前(Tx前)值进行比较。奥曲肽停药4周后,GH和胰岛素样生长因子-I(IGF-I)升高至Tx前值(GH,12小时曲线,4.5±0.6、2.6±0.7和5.6±1.1微克/升;IGF-I,三个样本,3.4±0.4、0.8±0.1和2.5±1.0 IU×10³/L;平均值±标准误,Tx前、使用奥曲肽时和停用奥曲肽时)。治疗期间对口服葡萄糖的胰岛素反应降低和葡萄糖反应增强在奥曲肽停药后恢复正常(胰岛素,527±84、289±62和733±110 pmol/L;葡萄糖,6.2±0.3、8.5±0.4和6.8±0.2 mmol/L;Tx前、使用奥曲肽时和停用奥曲肽时,平均值±标准误)。在奥曲肽治疗期间,24小时胃内pH值中位数为2.8(未测定Tx前pH值),血清胃泌素浓度中位数(12小时曲线下面积)为1275±153 ng/L.12小时(n = 7)。在奥曲肽停药期间,pH值降至1.4,而血清胃泌素升高至中位数2937±472 ng/L.12小时。我们得出结论,长期奥曲肽治疗对GH和IGF-I的抑制作用在停药后不会持续,这表明需要终身治疗。奥曲肽诱导的胰岛素抑制和血糖升高是可逆的。治疗期间高胃pH值可能促进奥曲肽相关胃炎的发展。奥曲肽停药期间胃泌素升高可能反映了从奥曲肽诱导的胃泌素抑制中释放后对慢性活动性胃炎的反应。
