Journal of Clinical Endocrinology and Metabolism Printed in U.S.A. Copyright © 1998 by The Endocrine Society Octreotide as Primary Therapy for Acromegaly*

The effects of octreotide (up to 5 yr) as primary treatment in 26 patients with acromegaly were compared with those in 81 patients with acromegaly who received octreotide as secondary or adjunctive therapy after previous surgery and/or pituitary radiation. These patients were part of a multicenter study that took place between 1989-1995. The study was divided into 3 phases beginning with a 1-month placebo-controlled treatment period followed by a 1-month washout period. In the second phase, patients were randomized to treatment with either 100 or 250 micrograms octreotide, sc, every 8 h for 6 months. Octreotide was then discontinued for 1 month and reinitiated at the lower dose for a total mean treatment duration of 39 months. The dose was titrated by each investigator to improve each patient's individual response, which included improvement in symptoms and signs of acromegaly as well as reduction of GH and insulin-like growth factor I (IGF-I) into the normal range. In the second phase of the study, in which patients were randomized to either 100 or 250 micrograms octreotide, three times daily, mean integrated GH and IGF-I concentrations after 3 and 6 months were equivalent in the primary and secondary treatment groups. During long term open label treatment, mean GH fell from 32.7 +/- 5.2 to 6.0 +/- 1.7 micrograms/L 2 h after octreotide injection in the primary therapy group and remained suppressed for a mean period of 24 months (range, 3-60 months). The mean final daily dose was 777 micrograms. In the patients receiving secondary treatment, mean GH fell from 30.2 +/- 7.6 to 5.6 +/- 1.1 micrograms/L after 3 months and remained suppressed for the remainder of the study (average dose, 635 micrograms daily). Mean IGF-I concentrations fell from 5.2 +/- 0.5 x 10(3) U/L (primary treatment group) and 4.7 +/- 0.4 x 10(3) U/L (secondary treatment group) to a mean of 2.2 +/- 0.3 x 10(3) U/L in both groups after 3 months of open label treatment and remained suppressed. IGF-I was reduced into the normal range during at least half of the study visits in 68% of the primary treatment group and in 62% of the secondary treatment group. Patients whose GH levels fell to at least 2 SD below the baseline mean GH were considered responders. There was no significant difference in the percentage of responders in the primary and secondary treatment groups (70% vs. 61%), nor was there a statistical difference in the mean GH concentrations between the groups. Symptoms of headache, increased perspiration, fatigue, and joint pain were reported at baseline by 46%, 73%, 69%, and 85%, respectively, of patients in the primary therapy group and improved during 3 yr of octreotide treatment in 50-100%. Similarly, these acromegaly-related symptoms were reported by 62%, 58%, 78%, and 60% of patients in the secondary therapy group, and improvement was noted in 62-88%. Pituitary magnetic resonance imaging scans were available in 13 of 26 patients in the primary treatment group before and after 6 months of octreotide treatment. Tumor shrinkage was observed in 6 of 13 patients, with reduction in tumor volume greater than 25% in only 3. Of 6 patients with documented tumor shrinkage, IGF-I was reduced into the normal range in 4 patients. Of the 7 remaining patients in whom tumor shrinkage was less than 10%, IGF-I was reduced into the normal range in 4 patients. Of the 7 remaining patients in whom tumor shrinkage was less than 10%, IGF-I was reduced into the normal range in 5 patients. The degree of tumor shrinkage did not correlate with the percent reduction in IGF-I or GH. In summary, octreotide was equally effective in 26 previously untreated acromegalic patients (primary treatment group) and 81 patients previously treated with either surgery or pituitary radiation (secondary treatment group). These observations call into question the current practice of surgical resection of all newly diagnosed GH-secreting pituitary adenomas regardless of the likelihood of cure. (AB

[1]  H. Sandler,et al.  Pituitary irradiation is ineffective in normalizing plasma insulin-like growth factor I in patients with acromegaly. , 1997, The Journal of clinical endocrinology and metabolism.

[2]  P. Cappabianca,et al.  Effect of octreotide pretreatment on surgical outcome in acromegaly. , 1997, The Journal of clinical endocrinology and metabolism.

[3]  P. Caron,et al.  Three year follow-up of acromegalic patients treated with intramuscular slow-release lanreotide. , 1997, The Journal of clinical endocrinology and metabolism.

[4]  I. Lancranjan,et al.  Sandostatin LAR in acromegalic patients: long-term treatment. , 1997, The Journal of clinical endocrinology and metabolism.

[5]  A. Grossman,et al.  Outcome of transsphenoidal surgery for acromegaly using strict criteria for surgical cure , 1996, Clinical endocrinology.

[6]  A. Beckers,et al.  Presurgical Octreotide: treatment in acromegaly. , 1993, Metabolism: Clinical and Experimental.

[7]  S. Lamberts,et al.  Drug therapy : octreotide , 1996 .

[8]  S. Melmed,et al.  Clinical review 75: Recent advances in pathogenesis, diagnosis, and management of acromegaly. , 1995, The Journal of clinical endocrinology and metabolism.

[9]  I. Lancranjan,et al.  Depot long-acting somatostatin analog (Sandostatin-LAR) is an effective treatment for acromegaly. , 1995, The Journal of clinical endocrinology and metabolism.

[10]  W. Young,et al.  Safety and efficacy of long-term octreotide therapy of acromegaly: results of a multicenter trial in 103 patients--a clinical research center study. , 1995, The Journal of clinical endocrinology and metabolism.

[11]  Consensus statement: benefits versus risks of medical therapy for acromegaly. , 1994, The American journal of medicine.

[12]  C. Bardin Current Therapy in Endocrinology and Metabolism , 1994 .

[13]  B. Scheithauer,et al.  Results of surgical treatment for growth hormone-secreting pituitary adenomas. , 1993, Journal of neurosurgery.

[14]  W. Young,et al.  Octreotide treatment of acromegaly. A randomized, multicenter study. , 1992, Annals of internal medicine.

[15]  J. Honegger,et al.  Surgical management of acromegaly. , 1992, Endocrinology and metabolism clinics of North America.

[16]  A. Barkan Acromegaly , 1890, Trends in Endocrinology & Metabolism.

[17]  A. Harris,et al.  Long-term treatment of 189 acromegalic patients with the somatostatin analog octreotide. Results of the International Multicenter Acromegaly Study Group. , 1991, Archives of internal medicine.

[18]  L. Frohman Clinical review 22: Therapeutic options in acromegaly. , 1991, The Journal of clinical endocrinology and metabolism.

[19]  A. Harris,et al.  Long Term Effect of Incremental Doses of the Somatostatin Analog SMS 201–995 in 58 Acromegalic Patients* , 1990 .

[20]  A. Harris,et al.  A randomized study of SMS 201-995 versus bromocriptine treatment in acromegaly: clinical and biochemical effects. , 1990, The Journal of clinical endocrinology and metabolism.

[21]  B. Bengtsson,et al.  Epidemiology and long-term survival in acromegaly. A study of 166 cases diagnosed between 1955 and 1984. , 2009, Acta medica Scandinavica.

[22]  S. Gebarski,et al.  Preoperative treatment of acromegaly with long-acting somatostatin analog SMS 201-995: shrinkage of invasive pituitary macroadenomas and improved surgical remission rate. , 1988, The Journal of clinical endocrinology and metabolism.

[23]  D. Ross,et al.  Results of transsphenoidal microsurgery for growth hormone-secreting pituitary adenoma in a series of 214 patients. , 1988, Journal of neurosurgery.

[24]  F. Roelfsema,et al.  LONG‐TERM RESULTS OF TRANSSPHENOIDAL PITUITARY MICROSURGERY IN 60 ACROMEGALIC PATIENTS , 1985, Clinical endocrinology.

[25]  W. Grove Statistical Methods for Rates and Proportions, 2nd ed , 1981 .

[26]  D. Appleton,et al.  EPIDEMIOLOGY OF ACROMEGALY IN THE NEWCASTLE REGION , 1980, Clinical endocrinology.

[27]  J. Fleiss,et al.  Statistical methods for rates and proportions , 1973 .

[28]  C. Lowy,et al.  MORTALITY IN ACROMEGALY1 , 1970 .

[29]  C. Lowy,et al.  Mortality in acromegaly. , 1970, The Quarterly journal of medicine.