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Volume 7

Journal of Infectious Diseases & Therapy

Infectious Diseases & Endocrinology 2019

February 27-28, 2019

February 27-28, 2019 Tokyo, Japan

Infectious Diseases, Diabetes and Endocrinology

Global Experts Meeting on

J Infect Dis Ther 2019, Volume 7

DOI: 10.4172/2332-0877-C2-063

Osteoporosis: Update and emerging therapies

Mohammad Saifuddin

Dhaka Medical College and Hospital, Bangladesh

steoporosis is a growing major public health prob¬lem with impacts on quality and quantity of life that cross medical,

social and economic lines. National Osteoporosis Foundation (NOF) estimates that 10.2 million Americans have

osteoporosis and that an additional 43.4 million have low bone mass. More than 2 million osteoporosis-related fractures occur

annually in the U.S.A. and more than 70% of these occur in women. Despite the availability of cost effective and well-tolerated

treatments to reduce fracture risk, only 23% of women age 67 or older who have an osteoporosis-related fracture receive either

a bone mineral density test or a prescription for a drug to treat osteoporosis in the six months after the fracture. Lifelong

adequate calcium and vitamin D intake is necessary for the acquisition of peak bone mass and subsequent maintenance of bone

health. Current FDA-approved pharmacologic options for the prevention and/or treatment of postmenopausal osteoporosis

include, in alphabetical order: Bisphosphonates (alendronate, alendronate plus D, ibandronate, risedronate and zoledronic

acid), calcitonin, estrogens (estrogen and/or hormone therapy), estrogen agonist/antagonist (raloxifene), tissue-selective

estrogen complex (conjugated estrogens/bazedoxifene), parathyroid hormone (PTH[1-34], teriparatide) and the RANKL

inhibitor denosumab. Sequential treatment with anabolic therapy followed by an anti-resorptive agent is generally preferred.

Combination therapy with teriparatide and an anti-resorptive can be considered in a few clinical settings in patients with very

severe osteoporosis such as spine and hip fractures. There are few indications for combining two anti-resorptive treatments,

but such options could be considered in the short-term in women who are experiencing active bone loss while on low dose

HRT for menopausal symptoms or raloxifene for breast cancer prevention. Evidence of efficacy beyond five years is limited,

whereas rare safety concerns such as ONJ and atypical femur fractures become more common beyond five years. Since there

is no extensive evidence base to guide treatment duration decisions, duration decisions need to be individualized. After the

initial three to five-year treatment period, a comprehensive risk assessment should be performed. This should include interval

clinical history, particular with respect to intercurrent fracture history and new chronic diseases or medications, as well as

height measurement, BMD testing and vertebral imaging if there has been any documented height loss during the treatment

period. It is reasonable to discontinue bisphosphonates after three to five years in people who appear to be at modest risk of

fracture after the initial treatment period. In contrast, for those who appear to be at high risk for fracture, continued treatment

with a bisphosphonate or an alternative therapy should be considered.