一种生长抑素类似物(SMS 201-995)对体内和体外胃泌素瘤分泌胃泌素的抑制作用的特征
Characterization of the in vivo and in vitro inhibition of gastrin secretion from gastrinoma by a somatostatin analogue (SMS 201-995).
作者信息
Ellison E C, Gower W R, Elkhammas E, Woltering E A, Sparks J, O'Dorisio T M, Fabri P J
出版信息
Am J Med. 1986 Dec 22;81(6B):56-64. doi: 10.1016/0002-9343(86)90585-1.
Earlier experiments characterized the effect of SMS 201-995 on gastrin secretion from gastrinoma in vivo. The results showed that the somatostatin analogue inhibits basal as well as secretin- and calcium-stimulated gastrin secretion. The current study examined the effect of SMS 201-995 on gastrin secretion from gastrinoma in vitro. Gastrinoma cells were prepared in cell culture or acute cell dispersion to study basal gastrin release. In cell culture, SMS 201-995 at 10(-9) M, 10(-8) M, and 10(-7) M significantly stimulated gastrin secretion (basal medium gastrin, 157 +/- 7.9 pg/ml; with SMS 201-995 10(-9) M, 786 +/- 62 pg/ml; with SMS 201-995 10(-8) M, 569 +/- 72 pg/ml; and with SMS 201-995 10(-7) M, 258 +/- 26 pg/ml). In contrast, in acute cell dispersion, the somatostatin analogue inhibited gastrin secretion (basal medium gastrin, 12.8 +/- 1.3 ng/ml; with SMS 201-995 10(-9) M, 9.0 +/- 0.1 ng/ml; with SMS 201-995 10(-8) M, 8.4 +/- 1.5 ng/ml; and with SMS 201-995 10(-7) M, 7.9 +/- 0.2 ng/ml). Gastrinoma cells were prepared in cell culture to study the effect of SMS 201-995 on gastrin secretion stimulated by secretin and by post-receptor increases in adenosine cyclic nucleotide. The somatostatin analogue inhibited gastrin secretion stimulated by secretin (10(-6) M) (797 +/- 48 pg/ml for secretin alone, compared with 396 +/- 9.4 pg/ml for secretin plus SMS 201-995). SMS 201-995 did not inhibit gastrin secretion stimulated by dibutyryl cyclic AMP (10(-7) M) (617 +/- 62 pg/ml for dibutyryl cyclic AMP alone, compared with 778 +/- 55 pg/ml for the two together). In vitro, SMS 201-995 inhibits basal gastrin secretion from gastrinoma prepared in acute cell dispersion, but not gastrinoma in cell culture, probably due to differences in basal secretory rates. The effect in vitro is less than that in vivo. SMS 201-995 does not inhibit postreceptor increases in adenosine nucleotide. This indirectly supports the hypothesis that SMS 201-995 acts in gastrinoma cells to inhibit gastrin secretion by inhibition of adenylate cyclase activity.
早期实验对SMS 201-995在体内对胃泌素瘤分泌胃泌素的作用进行了表征。结果显示,生长抑素类似物可抑制基础状态以及由促胰液素和钙刺激引起的胃泌素分泌。当前研究在体外检测了SMS 201-995对胃泌素瘤分泌胃泌素的作用。通过细胞培养或急性细胞分散制备胃泌素瘤细胞,以研究基础胃泌素释放情况。在细胞培养中,10⁻⁹M、10⁻⁸M和10⁻⁷M的SMS 201-995显著刺激胃泌素分泌(基础培养基胃泌素,157±7.9 pg/ml;使用10⁻⁹M的SMS 201-995时,786±62 pg/ml;使用10⁻⁸M的SMS 201-995时,569±72 pg/ml;使用10⁻⁷M的SMS 201-995时,258±26 pg/ml)。相比之下,在急性细胞分散中,生长抑素类似物抑制胃泌素分泌(基础培养基胃泌素,12.8±1.3 ng/ml;使用10⁻⁹M的SMS 201-995时,9.0±0.1 ng/ml;使用10⁻⁸M的SMS 201-995时,8.4±1.5 ng/ml;使用10⁻⁷M的SMS 201-995时,7.9±0.2 ng/ml)。通过细胞培养制备胃泌素瘤细胞,以研究SMS 201-995对促胰液素以及受体后腺苷环化核苷酸增加所刺激的胃泌素分泌的作用。生长抑素类似物抑制促胰液素(10⁻⁶M)刺激的胃泌素分泌(单独使用促胰液素时为797±48 pg/ml,促胰液素加SMS 201-995时为396±9.4 pg/ml)。SMS 201-995不抑制二丁酰环磷腺苷(10⁻⁷M)刺激的胃泌素分泌(单独使用二丁酰环磷腺苷时为617±62 pg/ml,两者同时使用时为778±55 pg/ml)。在体外,SMS 201-995抑制急性细胞分散制备的胃泌素瘤的基础胃泌素分泌,但不抑制细胞培养中的胃泌素瘤,这可能是由于基础分泌率的差异。体外作用小于体内作用。SMS 201-995不抑制受体后腺苷核苷酸的增加。这间接支持了以下假说:SMS 201-995在胃泌素瘤细胞中通过抑制腺苷酸环化酶活性来抑制胃泌素分泌。
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