Use of Levemir� Improves Metabolic and Clinical Status in Cystic Fibrosis-related Diabetes (CFRD)

Condition(s) targeted: Cystic Fibrosis Related Diabetes

Intervention: insulin detemir [rDNA origin] injection (Drug)

Phase: Phase 2/Phase 3

Status: Recruiting

Sponsored by: Nationwide Children's Hospital

Official(s) and/or principal investigator(s):
Dana S. Hardin, MD, Principal Investigator, Affiliation: OSU, Nationwide Children's Hospital

Overall contact:
Julie Rice, BSN, RN, Phone: 614-355-3142, Email: julie.rice@nationwidechildrens.org

This is a study to find out if Levemir® (a long acting or basal insulin) is safe and effective in treating cystic fibrosis related diabetes (CFRD).

Official title: Use of Levemir® Improves Metabolic and Clinical Status in CFRD

Study design: Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment

Primary outcome: To evaluate the effectiveness of Levemir to improve glycemic control in patients who have CFRD.

Secondary outcome: To evaluate the metabolic effects of Levemir and the effect on body weight and lean tissue mass.

Detailed description: Cystic fibrosis (CF) related diabetes (CFRD) and glucose intolerance affects more than 50%-75% of teens and adults with CF. The 1998 North American CF Foundation on CFRD categorized the disease differently than other types of diabetes: CFRD with fasting hyperglycemia (FH), CFRD without FH and transient CFRD. The outcome of this consensus conference was the use of insulin as the only recommended treatment of CFRD. Although the conference report mandated treatment for CFRD with FH, treatment was not mandated for the other types of CFRD, the choice to treat was left to the clinician's discretion. However, insulin was the only recommended therapy for all types of CFRD. Although some clinicians have used basal bolus regimens as the insulin management, many still use NPH. Given the need for CF patients to eat many frequent meals and snacks to maintain their weight, use of NPH insulin rarely renders good glycemic control. A basal bolus regimen is much more physiologic and would allow good glycemic control even with frequent meals and snacks. To date, there are no studies documenting safety and efficacy of true basal insulin, or a basal bolus regimen. Furthermore, protein catabolism and excessive muscle loss has been well documented in CF patients, both in those with and those without, glucose intolerance. Studies by our group and others have documented that a major reason for the catabolism is resistance to insulin's anti-catabolic effects on protein turnover. Thus, there is potential clinical benefit of improving muscle mass and general health by insulin treatment even for CF patients who do not have fasting hyperglycemia. A non-peaking basal insulin would be the only reasonable choice, yet studies are lacking. Our overall goal is to study the safety and efficacy of LevemirTM for the improvement of glycemic control of patients with CFRD. As a second goal, we will explore the ability of this basal insulin to improve protein catabolism and muscle mass. The study will be conducted as a six month trial.

Minimum age: 16 Years. Maximum age: 45 Years. Gender(s): Both.

Criteria:

Inclusion Criteria:

- Patients diagnosed with CFRD by oral glucose tolerance test (OGTT) who are medically

stable. Medical stability will be defined as:

- No hospital admission for six weeks or more before the study

- No oral or intravenous antibiotics for at least six weeks preceding the study

(subjects will be allowed to use low doses of inhaled corticosteroids).

Exclusion Criteria:

- Use of oral or intravenous corticosteroid medications within six weeks of the study.

- Evidence of clinically significant liver disease.

- Colonization with Burkholderia cepacia.

- Colonization with Aspergillus.

- Pregnancy.

- Medically unstable (stability defined above).

Julie Rice, BSN, RN, Phone: 614-355-3142, Email: julie.rice@nationwidechildrens.org

Nationwide Children's Hospital, Columbus, Ohio 43205, United States; Recruiting
Julie Rice, BSN, RN, Phone: 614-355-3142, Email: julie.rice@nationwidechildrens.org

Related publications:

Hardin DS, Moran A. Diabetes mellitus in cystic fibrosis. Endocrinol Metab Clin North Am. 1999 Dec;28(4):787-800, ix. Review.

Hardin DS, LeBlanc A, Para L, Seilheimer DK. Hepatic insulin resistance and defects in substrate utilization in cystic fibrosis. Diabetes. 1999 May;48(5):1082-7.

Moran A, Milla C, Ducret R, Nair KS. Protein metabolism in clinically stable adult cystic fibrosis patients with abnormal glucose tolerance. Diabetes. 2001 Jun;50(6):1336-43.

Moran A, Doherty L, Wang X, Thomas W. Abnormal glucose metabolism in cystic fibrosis. J Pediatr. 1998 Jul;133(1):10-17. Review. No abstract available.

Cucinotta D, Arrigo T, De Luca F, Di Benedetto A, Lombardo F, Scoglio R, Sferlazzas C, Magazzù G. Metabolic and clinical events preceding diabetes mellitus onset in cystic fibrosis. Eur J Endocrinol. 1996 Jun;134(6):731-6.

Nir M, Lanng S, Johansen HK, Koch C. Long-term survival and nutritional data in patients with cystic fibrosis treated in a Danish centre. Thorax. 1996 Oct;51(10):1023-7.

Starting date: August 2008
Last updated: August 10, 2009