Gallstones in Acromegalic Patients Undergoing Different Treatment Regimens

Overview

Journal Clin Investig

Specialty General Medicine

Date 1992 Jul 1

PMID 1356530

Citations 3

Authors

K Schmidt

M Leuschner

A G Harris

P H Althoff

V Jacobi

E Jungmann

P M Schumm-Draeger

H Rau

C Braulke

K H Usadel

Affiliations

Soon will be listed here.

Abstract

The frequency of gallstones during long-term treatment with the somatostatin analogue octreotide reported in different studies varies from 0% to 50%, the reason for this variation being unknown. Therefore, we examined 58 acromegalic patients undergoing different treatment regimens for the frequency of gallstones. Thirteen were treated with octreotide, 20 with bromocriptine, and 25 had no medical treatment after successful neurosurgery. Also, 58 patients without known gallbladder disease served as controls. The postprandial gallbladder contraction was also investigated in 27 acromegalic patients (10 with octreotide, 10 with bromocriptine, and 7 with no medical therapy). Ten of the 58 acromegalic patients were found to have gallstones, 4 of 25 receiving no medical treatment, 4 of 20 treated with dopamine agonists, and 2 of 13 treated with octreotide. In 9 of the 58 control patients, gallstones were detected. Although in the octreotide group the gallstones were newly formed under therapy, there was no difference in gallstone prevalence between the different treatment regimens and the control group. However, the postprandial gallbladder contraction was significantly more often inhibited during octreotide therapy, and this effect was most pronounced during the first hours following injection. Differences in the timing of injections therefore may be an explanation of the variable incidence of cholelithiasis in the different studies.

Citing Articles

Octreotide induced prolongation of colonic transit increases faecal anaerobic bacteria, bile acid metabolising enzymes, and serum deoxycholic acid in patients with acromegaly.

Thomas L, Veysey M, Murphy G, Russell-Jones D, French G, Wass J Gut. 2005; 54(5):630-5.

PMID: 15831907 PMC: 1774470. DOI: 10.1136/gut.2003.028431.

Epidemiology of acromegaly.

Holdaway I, Rajasoorya C Pituitary. 2000; 2(1):29-41.

PMID: 11081170 DOI: 10.1023/a:1009965803750.

A risk-benefit assessment of octreotide in the treatment of acromegaly.

Lely A, de Herder W, Lamberts S Drug Saf. 1997; 17(5):317-24.

PMID: 9391775 DOI: 10.2165/00002018-199717050-00004.

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