Abstract

Oral alendronate has been shown to be generally safe and efficacious in the treatment of osteoporosis in postmenopausal women, and is currently marketed in the United States and several other countries for the prevention and treatment of osteoporosis. Alendronate (10 mg daily for 3 years) has been shown to increase bone mineral density relative to placebo treatment by approximately 9% at the spine and 6 to 8% at the hip in well controlled studies conducted in the United States and other countries. Chronic alendronate treatment of postmenopausal women with osteoporosis has been associated with the production of histologically normal bone. Most importantly, increases in bone mineral density and normal bone histology associated with alendronate therapy have been shown to translate into a significant decrease in the incidence of fractures of the spine, hip and forearm. Although compliance with a daily dosing regimen has been excellent in clinical trials, less frequent dosing regimens may be more desirable for use in clinical practice. Preclinical data in both rat and baboon models treated with alendronate support similar efficacy with dosing at intervals of up to two weeks. Weekly dosing had not been investigated in postmenopausal women because tolerability of daily orally administered aminobisphosphonates is dose dependent. Therefore, even if the efficacy of weekly oral alendronate were equivalent to that of daily dosing, the higher daily doses required to deliver the same total cumulative dose might result in a diminished safety and tolerability profile. However, recent preclinical studies of the esophageal irritancy of alendronate suggest that a weekly exposure to a single high dose is less irritating than daily exposure to multiple lower doses. The once weekly dosing of alendronate would offer convenience to the patient, should result in similar efficacy, and may offer a safety advantage. Although, due to the excellent safety profile of alendronate 5 mg in clinical trials, it is not anticipated that any difference in safety can be clinically demonstrated. The design and success of the extensive preclinical alendronate development program strongly support the clinical investigation of less frequent oral dosing regimens.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
General Clinical Research Centers Program (M01)
Project #
2M01RR000750-28
Application #
6307199
Study Section
Project Start
1999-12-01
Project End
2000-11-30
Budget Start
Budget End
Support Year
28
Fiscal Year
2000
Total Cost
Indirect Cost

  Institution

Name
Indiana University-Purdue University at Indianapolis
Department
Type
DUNS #
005436803
City
Indianapolis
State
IN
Country
United States
Zip Code
46202

  Publications

Robinson-Cohen, Cassianne; Bartz, Traci M; Lai, Dongbing et al. (2018) Genetic Variants Associated with Circulating Fibroblast Growth Factor 23. J Am Soc Nephrol 29:2583-2592
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Srinivasan, Lakshmi; Page, Grier; Kirpalani, Haresh et al. (2017) Genome-wide association study of sepsis in extremely premature infants. Arch Dis Child Fetal Neonatal Ed 102:F439-F445
Gupta, Samir K; Yeh, Eunice; Kitch, Douglas W et al. (2017) Bone mineral density reductions after tenofovir disoproxil fumarate initiation and changes in phosphaturia: a secondary analysis of ACTG A5224s. J Antimicrob Chemother 72:2042-2048
Robarge, Jason D; Desta, Zereunesay; Nguyen, Anne T et al. (2017) Effects of exemestane and letrozole therapy on plasma concentrations of estrogens in a randomized trial of postmenopausal women with breast cancer. Breast Cancer Res Treat 161:453-461
Hertz, Daniel L; Speth, Kelly A; Kidwell, Kelley M et al. (2017) Variable aromatase inhibitor plasma concentrations do not correlate with circulating estrogen concentrations in post-menopausal breast cancer patients. Breast Cancer Res Treat 165:659-668
Patel, Yash R; Kirkman, M Sue; Considine, Robert V et al. (2017) Retinopathy predicts progression of fasting plasma glucose: An Early Diabetes Intervention Program (EDIP) analysis. J Diabetes Complications 31:605-610
Robarge, Jason D; Metzger, Ingrid F; Lu, Jessica et al. (2017) Population Pharmacokinetic Modeling To Estimate the Contributions of Genetic and Nongenetic Factors to Efavirenz Disposition. Antimicrob Agents Chemother 61:
Hertz, D L; Kidwell, K M; Seewald, N J et al. (2017) Polymorphisms in drug-metabolizing enzymes and steady-state exemestane concentration in postmenopausal patients with breast cancer. Pharmacogenomics J 17:521-527
Kadakia, Kunal C; Kidwell, Kelley M; Seewald, Nicholas J et al. (2017) Prospective assessment of patient-reported outcomes and estradiol and drug concentrations in patients experiencing toxicity from adjuvant aromatase inhibitors. Breast Cancer Res Treat 164:411-419

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