Treatments for Osteoporosis Expected Benefits, Potential Harms and Drug Holidays. Suzanne Morin MD FRCP FACP McGill University May 2014

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Treatments for Osteoporosis Expected Benefits, Potential Harms and Drug Holidays Suzanne Morin MD FRCP FACP McGill University May 2014

Learning Objectives Overview of osteoporosis management Outline efficacy and risks of bisphosphonates Discuss indications for drug holiday and how to monitor patients during that time

Bone Strength Biomechanical, biological and genetic factors Bone Quality + Bone Density + Bone Geometry Bone mineral content Bone turnover Activation Frequency Damage accumulation Quality of collagen Bone diameter Cortical thickness Bone Strength Adapted from R.Rizzoli 2005

Fracture Risk Assessment: Importance of Using Tools

Fracture Risk Assessment tools CAROC* Risk Factors: Sex Age BMD Fragility fracture after 40 Systemic glucocorticoid use ( 3 months) Additional Risk Factors: Low BMI FRAX ǂ Parental history of fracture (especially hip) Current smoking Alcohol intake 3 units/day Rheumatoid arthritis, or other secondary causes of osteoporosis Calibrated with Canadian data and validated in Canadians *Canadian Association of Radiologists and Osteoporosis Canada, 2010 3 months in the prior year of a prednisone equivalent dose 7.5mg daily ǂ Fracture Risk Assessment Tool of the World Health Organization Papaioannou A, et al CMAJ 2010.

Fracture Risk Assessment CAROC Assessment Tool Stratification Femoral neck T-score Women (treatment naive) 0.0-0.5-1.0-1.5-2.0-2.5-3.0-3.5-4.0 Fragility fracture after age 40 Individuals Low risk (<10%) with a T-score for the lumbar High risk (> 20%) 50 55 60 65 70 75 80 85 Age (years) Increases to the next risk category spine or total hip 2.5 should be Moderate risk (10-20%) considered to have at least moderate risk Prolonged corticosteroid therapy* Hip / vertebral fracture High risk (> 20%) > 1 non-vertebral fragility fracture * At least three months cumulative use during the preceding year at a prednisone-equivalent dose 7.5 mg daily Papaioannou A, et al CMAJ 2010.

How do we Choose Pharmacological therapy? First Line Therapies with Evidence for Fracture Prevention in Postmenopausal Women* Type of Fracture Vertebral Antiresorptive Therapy Patient Preference Bisphosphonates Denosumab Raloxifene Estrogen** (Hormone Alendronate Risedronate Safety Zoledronic Profile therapy) Acid Compliance- Adherence to therapy Provincial Reimbursement Plan Bone Formation Therapy Teriparatide Hip ---- --- Non- Vertebral + ---- + In clinical trials, non-vertebral fractures are a composite endpoint including hip, femur, pelvis, tibia, humerus, radius, and clavicle. * For postmenopausal women, indicates first line therapies and Grade A recommendation. For men requiring treatment, alendronate, risedronate, and zoledronic acid can be used as first line therapies for prevention of fractures [Grade D]. ** Estrogen or hormone therapy can be used as first line therapy in women with menopausal symptoms. 8

Bisphosphonates Anti-Fracture efficacy and cost-effectiveness documented 1 1 st line agents for treatment of patients at high risk for fragility fracture 150 million prescriptions dispensed between 2005 and 2009 in USA 2 1 McClung M et al. Am J Med 2013; 126: 13-20 2 Whitaker M et al. New Engl J Med 2012; 366: 2048-51

Bisphosphonates Inhibit osteoclastic activity and reduce bone remodeling -> increase BMD, lower fracture risk Prolonged residence in the skeleton Concerns have been raised: Over-suppression of bone turnover Microdamage accumulation and microcrack progression Over-mineralization and greater homogeneity of crystalline maturity Advanced glycation end-products loaded collagen Ettinger B et al. 2013 Bone epub Feb 2013

Bisphosphonates: good and bad? Osteonecrosis of the jaw Atypical femur fractures Atrial fibrillation Kidney injury Oesophageal cancer

Osteonecrosis of the Jaw Presence of exposed bone in the maxillofacial region that does not heal within 8 weeks of In the absence of radiation therapy Incidence between 1 in 10,000 to 1 in 100,000 patient-treatment-years. Higher in oncology population Recommendations for elective or urgent dental procedures: www.osteoporosis.ca/multimedia/pdf/hp/recommen dations_pamphlet_eng.pdf

Atypical Femur Fractures Case reports Case series RCT re-analyses Cohort studies Case-control studies Meta-Analysis Insufficiency fracture Associated with bisphosphonate use Infrequent Feldstein A et al. J Bone Miner Res. 2012; 27: 977-86 Gedmintas L et al. J Bone Miner Res. 2013 28:1729-37 Shane E et al J Bone Miner Res. Epub 2013 May 28

Incidence of AFF Incidence estimated to be 1 1.78/100,000 p-years with exposure of < 2 years 113/ 100,000 p-years with exposure 8 to 10 years Meta-analysis shows increased risk of subtrochanteric, diaphyseal and atypical fractures with bisphosphonate use 1 Dell RM et al. J Bone Miner Res 2012; 27: 2544-50

Atypical Femur Fractures

Long-term Adverse Events associated with Bisphosphophate Use Papaioannou A et al Canadian Medical Association Journal 2010;182(17):1864-1873. Shane E et al J Bone Miner Res. May 28 2013. Koshla S et al. J.Bone Miner.Res. 2007;22:1479-1491. 16

How long should we keep patients on therapy? Usually limited to bisphosphonate therapy Concerns arise because: Prolonged residence of bisphosphonates in bone Over-suppression of bone remodeling Patient s risk for fracture Affinity of bisphosphonate for bone

Concept of Drug Holiday Alendronate data Risedronate Zoledronic Acid data NO data on drug holiday with raloxifene or denosumab but, we know that if you stop these medications, there is no residual effect of therapy on bone remodeling

Duration of Bisphosphonate Therapy and Drug Holiday What do we Monitor during a Drug Holiday? -Treat to Target- Monitor Fracture Risk Bone Turnover Markers Inquire about Fractures Bone Mineral Density 20

FRAX- Treatment Target? Leslie WD, Majumdar SR, Morin SN et al ASBMR 2013, Baltimore, MD

What are the Therapeutic Options After a Drug Holiday Remember to assess the risk for fractures with CAROC or FRAX Always consider patient s preference Resume bisphosphonate Change class: Denosumab Consider to change over to anabolic agent (teriparatide) but, restriction of reimbursement by Provincial Drug Plan 22

Key Messages Use fracture assessment tools Avoid basing your treatment decisions on BMD alone Use anti-osteoporosis medications only in patients at moderate and high risk for fractures Monitor adherence, tolerability, fractures, BMD and?bone turnover markers Consider a drug holiday in patients at low and moderate risk after 5 to 7 years of treatment with bisphosphonates

Questions? Osteoporosis Canada www.osteoporosis.ca suzanne.morin@mcgill.ca http://blogs.mcgill.ca/calcium/