© 2015 Polish Urological Association. All Rights Reserved.Introduction Prostate cancer is a large clinical burden across Europe. It is, in fact, the most common cancer in males, accounting for more than 92,300 deaths annually throughout the continent. Prostate cancer is androgen-sensitive; thus an androgen deprivation therapy (ADT) is often used for treatment by reducing androgen to castrate levels. Several ADT agents have achieved benefits with effective palliation, but, unfortunately, severe adverse events are frequent. Contemporary ADT (Luteinising Hormone Releasing Hormone agonist - LHRHa injections) can result in side effects that include osteoporosis and fractures, compromising quality of life and survival.  Methods In this review we analysed the associated bone toxicity consequent upon contemporary ADT and based on the literature and our own experience we present future perspectives that seek to mitigate this associated toxicity both by development of novel therapies and by better identification and prediction of fracture risk. Results Preliminary results indicate that parenteral oestrogen can mitigate associated osteoporotic risk and that CT scans could provide a more accurate indicator of overall bone quality and hence fracture risk.  Conclusions As healthcare costs increase globally, cheap and effective alternatives that achieve ADT, but mitigate or avoid such bone toxicities, will be needed. More so, innovative techniques to improve both the measurement and the extent of this toxicity, by assessing bone health and prediction of fracture risk, are also required

Abel, PD

Abel, RL

Edwards, S

Honeyfield, L

Price, P

Shah, SI

Wilson, HC

Central European Journal of Urology

PubMed

Hannah C.P. Wilson

Syed I.A. Shah

Paul D. Abel

Patricia Price

Lesley Honeyfield

Steve Edwards

Richard L. Abel

Crossref

Contemporary hormone therapy with LHRH agonists for prostate cancer: avoiding osteoporosis and fracture

Wilson H, Shah I, Abel P, Price P, Honeyfield L, Edwards S,

Spiral - Imperial College Digital Repository

165Central European Journal of UrologyR E V I E W   P A P E R UROLOGICAL ONCOLOGYContemporary hormone therapy with LHRH agonists  for prostate cancer: avoiding osteoporosis and fractureHannah C.P. Wilson, Syed I.A. Shah, Paul D. Abel, Patricia Price, Lesley Honeyfield, Steve Edwards, Richard L. AbelDepartment of Surgery and Cancer, Imperial College, LondonArticle historySubmitted: Nov. 26, 2014 Accepted: Feb. 1, 2015 Published on-line:  April 20, 2015Introduction Prostate cancer is a large clinical burden across Europe. It is, in fact, the most common can-cer in males, accounting for more than 92,300 deaths annually throughout the continent. Prostate cancer is androgen-sensitive; thus an androgen deprivation therapy (ADT) is often used for treatment by reducing  androgen to castrate levels. Several ADT agents have achieved benefits with effective palliation, but, unfortunately, severe adverse events are frequent. Contemporary ADT (Luteinising Hormone Releasing Hormone agonist - LHRHa injections) can result in side effects that include osteoporosis and fractures, compromising quality of life and survival. Methods In this review we analysed the associated bone toxicity consequent upon contemporary ADT  and based on the literature and our own experience we present future perspectives that seek to mitigate this associated toxicity both by development of novel therapies and by better identification and prediction of fracture risk.Results Preliminary results indicate that parenteral oestrogen can mitigate associated osteoporotic risk and that CT scans could provide a more accurate indicator of overall bone quality and hence fracture risk. Conclusions As healthcare costs increase globally, cheap and effective alternatives that achieve ADT, but mitigate or avoid such bone toxicities, will be needed. More so, innovative techniques to improve both the measurement and the extent of this toxicity, by assessing bone health and prediction of fracture risk, are also required.Corresponding authorHannah WilsonImperial College LondonCharing Cross HospitalFulham Palace RoadW6 8RF London, UK phone: 07 881 765 605hcw112@ic.ac.ukKey Words: prostate cancer ‹› androgen deprivation therapy ‹› luteinising hormone releasing hormone agonist ‹› osteoporosis ‹› fracture imagingCent European J Urol 2015; 68: 165-168 doi: 10.5173/ceju.2015.513INTRODUCTIONThe discovery by Huggins in the 1940s that pros-tate cancer is androgen-sensitive led to the devel-opment of therapies, with differing mechanisms of action, to achieve castrate levels of androgen (ADT). Unfortunately, these agents often also had major unwanted side effects, such as osteoporosis and fractures, with ADT achieved with contem-porary LHRH agonists (LHRHa) [1]. As both the clinical and financial burden surrounding prostate cancer grows [2], cheap and effective alternatives that achieve ADT but mitigate such bone toxicities are required. Mechanisms of action and toxicity  with contemporary hormonal treatment  of prostate cancerProstate cancer cell growth is usually androgen-de-pendent [3], through stimulation of androgen recep-tors for growth and proliferation [4]. ADT in men, ei-ther medically (LHRHa) or by surgical orchiectomy, suppresses serum concentrations of both androgens and oestrogen to less than 5% and 20% of normal val-ues respectively (oestradiol is synthesised in males by the aromatisation of testosterone) [5]. These very low sex hormone levels result in potentially major toxicities, including hot flushes, sarcopenia, erectile Citation: Wilson HCP, Shah SIA, Abel PD, Price P, Honeyfield L, Edwards S, Abel RL. Contemporary hormone therapy with LHRH agonists for prostate cancer: avoiding osteoporosis and fracture. Cent European J Urol. 2015; 68: 165-168.Central European Journal of Urology166dysfunction and osteoporosis (the latter and related fragility fracture risk specifically are most likely a consequence of oestrogen deficiency) [6].Osteoporosis, fracture risk and ADTSusceptibility to bone fractures arises following an imbalance in the activity of cells involved in bone turnover, namely osteoblasts and osteoclasts [7]. This results in reduced bone formation with increased bone resorption. As such, bone mineral density (BMD) is reduced and susceptibility to bone fracture increases. Following initiation of ADT, accelerated bone resorption ensues, leading to both a reduced bone mass, as well as structural changes with perfo-ration of trabeculae [8] accounting, therefore, for the greater risk of developing osteoporosis [9]. Shahin-ian et al. demonstrated a direct link between ADT and  fracture risk [10], whilst Shao et al. confirmed this and reported it to be directly proportional to the number of LHRHa doses received [11]. Importantly, Shao et al. reported that if a fracture occurred, it was associated with an overall 40% higher relative risk of mortality compared to if no fracture occurred (mortality was 6.27% higher within 6 months and 9.87% within 12 months of experiencing a fracture). There is, therefore, an unmet need for new and ef-fective alternative interventions that achieve ADT, but avoid bone toxicities and the related morbidity, mortality and cost.Alternative therapies: revisiting the pastOral oestrogen (diethylstilbestrol – DES) was origi-nally one of the main therapeutic options for treat-ing prostate cancer. While many studies confirmed its efficacy of androgen suppression, and even im-proved overall survival, thorough analyses revealed it was associated with life-threatening cardiovas-cular toxicity [12]. Importantly, these early studies were conducted using a relatively high dose of DES (5 mg) and further work has elucidated that a lower dose, either 3 mg or 1 mg may avoid or reduce such cardiovascular toxicity [13, 14]. This is now known to be due directly to the hepatic first-pass of oes-trogen, which results in induction of pro-coagulant proteins increasing the risk of thromboembolism and cardiovascular events. More recently, there is evidence that parenteral administration of oestro-gen (either by intramuscular injection or transcu-taneously) is able to circumvent this cardiovascular toxicity [15, 16]. Furthermore, the administration of parenteral (exogenous) oestrogen returns serum (endogenous) oestrogen to levels that may miti-gate contemporary ADT toxicities that are caused by endogenous oestrogen depletion. Such mitiga-tions of toxicities include osteoporosis, by improving the BMD [17].New and encouraging preliminary data reveals oes-trogen to be a cheap and safe option. Moreover with outcomes at least equivocal to contemporary ADT, the question of why oestrogen in parenteral form has yet to reclaim a role in prostate cancer therapy, re-mains a mystery. The ongoing UK National PATCH (Prostate Adenocarcinoma TransCutaneous Hor-mones) randomised clinical trial comparing transder-mal oestradiol with LHRHa in locally advanced and metastatic prostate cancer has shown preliminary data to support the potential offered by oestrogen to deliver ADT and mitigate associated bone toxicity, as well as other adverse events of LHRHa ADT [18]. PATCH, which includes a total of 686 men, compares oestrogen patches (EP; FemSeven 100 µg/24 hr, 4 patches changed twice-weekly reducing to 3 after 4 weeks) versus LHRHa for locally advanced or met-astatic prostate cancer (allocation ratio 2:1 before 21/2/2011, 1:1 after).  Early Phase II data showed equivalence of safety and efficacy between trial arms [15]. A recent PATCH sub-study evaluating bone health further highlighted the osteoprotective potential of transdermal oestrogen whilst avoiding the associated cardiovascular toxicity of oral oes-trogen. Compared to baseline, lumbar spine BMD declined following LHRHa treatment at both year 1 and year 2 (-2.11% and -6.09% respectively), while it increased with oestrogen patch treatment at year 1 (+6.43%) and was maintained at year 2 (+4.58). These early results encourage the hypothesis that exogenous oestrogen suppresses testosterone to cas-trate levels whilst appearing to improve BMD values (Table 1) [17].Predicting fracture risk: is the current gold standard accurate enough?The current gold standard for measuring osteoporot-ic risk is assessment of BMD [19], This is assessed *Comparing armsTable 1. Early data from the bone sub-study of the PATCH trial: Changes in lumbar spine bone mineral density at 1 and 2 years from baseline (Langley et al. 2014 [17])Mean percentage change p-valueLHRHa arm Transdermal oestrogen armYear 1 -2.11% (n=21) +6.43%, (n=39) <0.001*Year 2 -6.09%, n=10 +4.58%, n=20 <0.001*167Central European Journal of Urologyusing Dual Energy X-ray Absorptiometry (DEXA) and the diagnostic tool: Fracture Risk Assess-ment Tool (FRAX) [20]. FRAX integrates the BMD of the femoral neck along with multiple clinical risk factors to calculate both the 10-year probability of a hip fracture and a major osteoporotic fracture [21]. Whilst originally it was thought that bone strength was almost entirely explained by density, clinical observations did not support the data [22]. It was subsequently found that densitometry failed to take into account the importance of cortical geom-etry and trabecular architecture for bone strength. In fact, BMD only accounts for about 40–50% of the in vitro compressive strength of bone, whilst struc-ture contributes as much as 30–40% of the remainder [23]. Following these discoveries, a new understand-ing of bone strength-termed bone quality, operation-ally defined as the structural and mechanical basis of bone strength, was developed [24]. Bone quality is an amalgamation of all the factors that determine how well a skeleton can resist frac-turing, including the micro-architecture, accumu-lated microscopic damage, quality of collagen, size of mineral crystals and the rate of bone turnover [19]. The current challenge is to find a suitable and non-invasive method of measuring bone quality in clinical practice, which can predict the risk of bone fracture in individual patients. Whilst advanced technologies such as computerised tomography (CT) and magnet-ic resonance imaging (MRI) have been considered, it is difficult to balance factors such as radiation risk to the patient, technical matters including image resolution and the inescapable costs of healthcare.CONCLUSIONSThere is an unmet need to improve management of patients requiring treatments that may diminish bone quality, as well as instruments that will pre-dict this, and hence osteoporotic and fracture risk to patients. This is particularly important for those al-ready at an increased risk of bone loss, including the elderly or prostate cancer patients undergoing ADT. Patients enrolled on the PATCH trial offer a unique opportunity to study these bone quality changes by comparing directly between prostate cancer ther-apies that either decrease (LHRHa) or increase (oes-trogen) bone quality, and thus to assess the methods by which these changes may be more easily moni-tored and speedily diagnosed. CONFLICT OF INTEREST Professor Paul Abel as editorial member at Central European Jour-nal of Urology.ACKNOWLEDGMENTSDr. S. I. A. Shah’s work is supported by the Commonwealth Scholarship Commission, United Kingdom1. Ross RW, Small EJ. Osteoporosis in men treated with androgen deprivation therapy for prostate cancer. J Urol. 2002; 167: 1952-1956.2. Prostate cancer statistics: Cancer Research http://www.cancerresearchuk.org/cancer-info/cancerstats/types/prostate/incidence/uk-prostate-cancer-incidence-statistics#geog3. Gomella LG. Effective testosterone suppression for prostate cancer: is there a best castration therapy? Rev Urol. 2009; 11: 52-60.4. Tan ME, Li J, Xu HE, Melcher K, Yong EL. Androgen receptor: structure, role  in prostate cancer and drug discovery.  Acta Pharmacol Sin. 2015; 36: 3-23.5. Garnick MB. Leuprolide versus diethylstilbestrol for previously untreated stage D2 prostate cancer. Results  of a prospectively randomized trial. Urology. 1986; suppl 1: 21-28.6. Freedland SJ, Eastham J, Shore N. Androgen deprivation therapy and estrogen deficiency induced adverse effects in the treatment of prostate  cancer. Prostate Cancer Prostatic Dis.  2009; 12: 333-338.7. Frenkel B, Hong A, Baniwal SK, al. Regulation of adult bone turnover by sex steroids. J Cell Physiol. 2010; 224: 305-310.8. Singh M, Nagrath AR, Maini PS. Changes  in trabecular pattern of the upper end  of the femur as an index of osteoporosis.  J Bone Joint Surg Am. 1970; 52: 457-467.9. Kiratli BJ, Srinivas S, Perkash I, Terris MK. Progressive decrease in bone density over 10 years of androgen deprivation therapy in patients with prostate cancer. Urology. 2001; 57: 127-132.10. Shahinian VB, Kuo YF, Freeman JL, Goodwin JS. Risk of fracture after androgen deprivation for prostate cancer. N Engl J Med. 2005; 352: 154-164.11. Shao YH, Moore DF, Shih W, Lin Y, Jang TL,  Lu-Yao GL. Fracture after androgen deprivation therapy among men  with a high baseline risk of skeletal complications. BJU Int. 2013; 111:  745-752.12. Byar DP. Proceedings: The Veterans Administration Cooperative Urological Research Group's studies of cancer of the prostate. Cancer. 1973; 32: 1126-1130.13. Poulsen MH, Frost M, Abrahamsen B, Brixen K, Walter S. Osteoporosis and prostate cancer: a cross-sectional study  of Danish men with prostate cancer before androgen deprivation therapy. Scand J Urol. 2014; 48: 350-355.14. Turo R, Smolski M, Esler R, et al. Diethylstilboestrol for the treatment  of prostate cancer: past, present and future. Scand J Urol. 2014; 48: 4-1415. Langley RE, Godsland IF, Kynaston H, et al. Early hormonal data from a multicentre ReferencesCentral European Journal of Urology168phase II trial using transdermal oestrogen patches as first-line hormonal therapy  in patients with locally advanced  or metastatic prostate cancer. BJU Int. 2008; 102: 442-445.16. Hedlund PO, Damber JE, Hagerman I,  et al. Parenteral estrogen versus combined androgen deprivation in the treatment  of metastatic prostatic cancer: part 2.  Final evaluation of the Scandinavian Prostatic Cancer Group (SPCG) Study  No. 5. Scand J Urol Nephrol. 2008; 42: 220-229.17. Langley RE, Duong T, Jovic G, et al.  Bone density in men receiving androgen deprivation therapy for prostate  cancer, a randomised comparison  between transdermal estrogen and luteinising hormone-releasing hormone agonists. J Clin Oncol 2014; 32: suppl 5: abstr 5067.18. Langley RE, Cafferty FH, Alhasso AA, et al.  Cardiovascular outcomes in patients  with locally advanced and metastatic prostate cancer treated with luteinising-hormone-releasing-hormone agonists  or transdermal oestrogen: the randomised, phase 2 MRC PATCH trial (PR09). Lancet Oncol. 2013; 14: 306-316.19.  Licata AA. Bone density vs bone quality: what's a clinician to do? Cleve Clin J Med. 2009; 76: 331-336.20. Fujiwara S, Nakamura T, Orimo H, et al.  Development and application  of a Japanese model of the WHO  fracture risk assessment tool (FRAX). Osteoporos Int. 2008; 19: 429-435.21. Kanis JA, Johnell O, Oden A, Johansson H, McCloskey E. FRAX and the assessment  of fracture probability in men and women from the UK. Osteoporos Int. 2008; 19: 385-397.22. Licata AA. Bone density, bone quality, and FRAX: changing concepts in osteoporosis management. Am Journal Obstet Gynecol. 2013; 208: 92-96.23. Ulrich D, van Rietbergen B, Laib A, Ruegsegger P. The ability of three-dimensional structural indices to reflect mechanical aspects of trabecular bone. Bone. 1999; 25: 55-60.24. Abel RL, Prime M, Jin A, Cobb JP, Bhattacharya R. 3D Imaging Bone  Quality: Bench to Bedside. Hard Tissue. 2013; 10; 2: 42. 

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Contemporary hormone therapy with LHRH agonists for prostate cancer: avoiding osteoporosis and fracture.

Contemporary hormone therapy with LHRH agonists for prostate cancer: avoiding osteoporosis and fracture.

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