Periodic courses of human 1–34 parathyroid peptide alternating with calcitriol paradoxically reduce bone remodelling in spinal osteoporosis

Reeve, J.; Arlot, M.; Price, TB; Edouard, C.; Hesp, R.; Hulme, P.; Ashby, J. P.; Zanelli, Joan M.; Green, J. R.; Tellez, M.; Katz, David; Spinks, T.J.; Meunier, Pierre J.

doi:10.1111/j.1365-2362.1987.tb01137.x

Cited by 31 publications

(2 citation statements)

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“…Although in hyperparathyroidism this catabolic effect leads to loss of bone mineral content, PTH has an anabolic effect on bone remodeling when administered intermittently 78. Teriparatide (1–34 amino acid peptide) is a human PTH analog which also has an osteoanabolic effect when administered intermittently at low doses 79. Teriparatide (Forteo ® ) is effective (20 μg/day subcutaneously) at increasing BMD in postmenopausal and glucocorticoid-induced osteoporosis and is more effective than alendronate at reducing the incidence of vertebral and hip fractures 80–82.…”

Section: Current Therapeutic Management Options For Osteoporosismentioning

confidence: 99%

“…The administration of raloxifene prior to teriparatide improves BMD above that of teriparatide alone 83. In open-label studies, alendronate blunted the ability of teriparatide to increase BMD when the therapies were combined,79 whereas in another study patients that had been previously treated with risedronate showed better improvement in BMD in response to teriparatide than patients that had previously been on alendronate therapy 8484.…”

Section: Current Therapeutic Management Options For Osteoporosismentioning

confidence: 99%

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Osteoporosis – a current view of pharmacological prevention and treatment

Das¹,

Crockett²

2013

DDDT

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Postmenopausal osteoporosis is the most common bone disease, associated with low bone mineral density (BMD) and pathological fractures which lead to significant morbidity. It is defined clinically by a BMD of 2.5 standard deviations or more below the young female adult mean (T-score =−2.5). Osteoporosis was a huge global problem both socially and economically – in the UK alone, in 2011 £6 million per day was spent on treatment and social care of the 230,000 osteoporotic fracture patients – and therefore viable preventative and therapeutic approaches are key to managing this problem within the aging population of today. One of the main issues surrounding the potential of osteoporosis management is diagnosing patients at risk before they develop a fracture. We discuss the current and future possibilities for identifying susceptible patients, from fracture risk assessment to shape modeling and in relation to the high heritability of osteoporosis now that a plethora of genes have been associated with low BMD and osteoporotic fracture. This review highlights the current therapeutics in clinical use (including bisphosphonates, anti-RANKL [receptor activator of NF-κB ligand], intermittent low dose parathyroid hormone, and strontium ranelate) and some of those in development (anti-sclerostin antibodies and cathepsin K inhibitors). By highlighting the intimate relationship between the activities of bone forming (osteoblasts) and bone-resorbing (osteoclasts) cells, we include an overview and comparison of the molecular mechanisms exploited in each therapy.

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