Evaluation of the anti-osteoporotic effect of <i>Ginkgo biloba</i> L. in Wistar rats with glucocorticoid-induced-osteoporosis by bone densitometry using dual-energy x-ray absorptiometry (DEXA) and mechanical testing

LUCINDA, LEDA M.F.; AARESTRUP, BEATRIZ J.V.; REBOREDO, MAYCON M.; PAINS, THAIS D.A.; CHAVES, RAPHAEL Z.; REIS, JOÃO E.P.; LOUZADA, MÁRIO J.Q.; GUERRA, MARTHA O.

doi:10.1590/0001-3765201720160479

ABSTRACT

Evaluate the effect of the extract of Ginkgo biloba in the bone alkaline phosphatase, bone mineral density, in the mechanical properties of the tibia in rats with glucocorticoid-induced-osteoporosis. After osteoporosis induction, the rats were divided into five groups: Osteoporosis; EGb1 (28 mg/Kg); EGb2 (56 mg/Kg); alendronate (0.2 mg/animal) and control. The animals were treated during 20 and 30 days. The control group was compared with the osteoporosis’s (Student’s t-test), while the other were analyzed by ANOVA test followed by Tukey/Dunnett’T3 (p<0.05). In the osteoporosis group the bone alkaline phosphatase, bone mineral density, the bone stiffness, the maximum load and the resilience were reduced. The bone alkaline phosphatase values increased in the EGb1 and EGb2 groups (30 days). In addition, in the EGb2 and alendronate groups (20 and 30 days) the bone mineral density increased. The extract of Ginkgo biloba restored bone alkaline phosphatase and bone mineral density using dual-energy x-ray absorptiometry.

Key words:
bone density; DEXA scan; Ginkgo biloba; osteoporosis

INTRODUCTION

The low bone mass is associated with genetic, nutritional and lifestyle factors, as well as estrogen levels and the use of some drugs (Johnell 1996JOHNELL O. 1996. Advences in osteoporosis: better identification of risk factors can reduce morbity and mortality. J Intern Med 239: 229-304.). Among these drugs, glucocorticoids have potent anti-inflamatory effects and were used for decades in the treatment of chronic diseases, as well as in posttransplantation immunotherapy (McLaughlin et al. 2002). The current use of oral corticosteroids is associated with serious side effects, including osteoporosis and consequently an increase in fractures (Henneicke et al. 2011HENNEICKE H ET AL. 2011. Corticosterone selectively targets endocortical surfaces by an osteoblast-dependent mechanism. Bone 49: 733-742.). Despite the clinical recognition that glucocorticoids can cause bone loss, many patients receiving long-term glucocorticoid therapy are not evaluated for their skeletal health and do not receive specific prophylaxis or treatment (Cruse et al. 2006CRUSE LM, VALERIANO J, VASEY FB AND CARTER JD. 2006. Prevalence of evaluation and treatment of glucocorticoid-induced osteoporosis in men. J Clin Rheumatol 12: 221-225., Feldstein et al. 2005FELDSTEIN AC, ELMER PJ, NICHOLS GA AND HERSON M. 2005. Practice patterns in patients at risk for glucocorticoid-induced osteoporosis. Osteoporos Int 16: 2168-2174.).

Glucocorticoids act directly on bone cells and one of their principal actions is to reduce osteoblasts function and number by apoptosis (Chang et al. 2009, Hock et al. 2001HOCK JM, KRISHNAN V, ONYIA JE, BIDWELL JP, MILAS J AND STANISLAUS D. 2001. Osteoblast Apoptosis and Bone Turnover. J Bone Miner Res 16: 975-984.). The Bax expression by ostoblasts increase in the glucocorticoid-induced osteoporosis (GIO) as showed by Lucinda et al. (2013LUCINDA LM, VIEIRA BJ, PETERS VM, REIS JEP, OLIVEIRA RSMF AND GUERRA M DE O. 2013. The effect of the Ginkgo biloba extract in the expression of Bax, Bcl-2 and bone mineral content of Wistar rats with glucocorticoid-induced osteoporosis. Phytother Res 27: 515-520.). It`s well known that apoptosis is regulated by an intrinsic process involving activation of genes that can promote cell death (Bras et al. 2005BRAS M, QUEENAN B AND SUSIN S. 2005. Programmed cell death via mitochondria: different modes of dying. Biochemistry 70: 231-239.). Likewise, the Bcl-2 gene family encodes a large number of proteins, including Bax, a pro-apoptotic protein member of the Bcl-2 gene family that participates in programmed cell death (Verborgt et al. 2002VERBORGT O, TATTON NA, MAJESKA RJ AND SCHAFFLER MB. 2002. Spatial distribution of Bax and Bcl-2 in osteocytes after bone fatigue: Complementary roles in bone remodeling regulation. J Bone Miner Res 17: 907-914.).

The biochemical markers are also important in the management of osteoporosis, one of them being the bone alkaline phosphatase (BAP) which is a specific enzyme released from osteoblasts into the blood during the process of bone formation and believed to be indicative of the bone mineralization process (Brown et al. 2009BROWN JP ET AL. 2009. Bone turnover markers in the management of postmenopausal osteoporosis. Clin Biochem 42: 929-942.).

Biphosphonates are widely used in the prevention or in the treatment of osteoporosis (Russell 2006RUSSELL RG. 2006. Bisphosphonates: from bench to bedside. Ann NY Acad Sci 1068: 367-401.), however, some side effects like gastrointestinal intolerance (Szejnfeld 2000SZEJNFELD VL. 2000. Clinical manifestations. Osteoporosis: diagnostic and treatment. 1st ed., São Paulo: Sarvier, 406 p.) and osteonecrosis of the jaw have been reported (Hoff et al. 2008HOFF AO ET AL. 2008. Frequency and risk factors associated with osteonecrosis of the jaw in cancer patients treated with intravenous bisphosphonates. J Bone Miner Res 23: 826-836., Pozzi et al. 2007POZZI S ET AL. 2007. Bisphosphonate associated osteonecrosis of the jaw: a review of 35 cases and an evaluation of its frequence in multiple myeloma patients. Leuk Lynphoma 48: 1852-1854.); thus, the necessity to search for new approaches to the current therapies. Phytoestrogens showed significant results in the treatment of osteoporosis (Bawa 2010BAWA S. 2010. The significance of soy protein and soy bioactive compounds in the prophylaxis and treatment of osteoporosis. J Osteoporos 8: 1-8.). Similarly, Trivedi et al. (2009TRIVEDI R, KUMAR A, GUPTA V, KUMAR S, NAGAR GK, ROMERO JR, DWIVEDI AK AND CHATTOPADHYAY N. 2009. Effects of Egb 761 on bone mineral density, bone microstructure, and osteoblast function: Possible roles of quercetin and kaempferol. Mol Cell Endocrinol 302: 86-91.) suggest that the phytoestrogens components of EGb, kaempferol and quercetin, are involved in the beneficial outcomes on bone.

Ginkgo biloba L. (family Ginkgoaceae) is a plant currently used by the population in different therapeutical approaches. The main compounds of this plant comprise 6% of terpenoids (ginkgolides and bilobilides), less than 5 ppm of ginkgolic acid, and 24% of phytoestrogens (Kaempferol, ishorhamnetin and quercetin) (Oh and Chung 2004OH SM AND CHUNG KH. 2004. Estrogenic activities of Ginkgo biloba extracts. Life Sci 74: 1325-1335., Van Beek 2002). Notwithstanding the fact that there is lack of pre-clinical studies as well as absence of clinical ones using Ginkgo biloba in the treatment of osteoporosis, the few existing pre-clinical studies have showed promising results in the management of osteoporosis (Lucinda et al. 2010aLUCINDA LM, DE OLIVEIRA TT, SALVADOR PA, PETERS VM, REIS JE AND GUERRA M DE O. 2010a. Radiographic evidences of mandibular osteoporosis improvement in Wistar rats treated with Ginkgo biloba. Phytother Res 24: 264-267., b, Oh et al. 2008, Trivedi et al. 2009TRIVEDI R, KUMAR A, GUPTA V, KUMAR S, NAGAR GK, ROMERO JR, DWIVEDI AK AND CHATTOPADHYAY N. 2009. Effects of Egb 761 on bone mineral density, bone microstructure, and osteoblast function: Possible roles of quercetin and kaempferol. Mol Cell Endocrinol 302: 86-91.).

Among the major effects of Ginkgo biloba extract (EGb) that could be important in the treatment of osteoporosis, the antiapoptotic properties of this extract have been reported by some authors (Smith et al. 2002SMITH JV, BURDICK AJ, GOLIK P, KHAN I, WALLACE D AND LUO Y. 2002. Antiapoptotic properties of Ginkgo biloba extract EGb761 in differentiated PC12 cells. Cell Mol Biol 48: 699-707., Smith and Luo 2004, Lucinda et al. 2013LUCINDA LM, VIEIRA BJ, PETERS VM, REIS JEP, OLIVEIRA RSMF AND GUERRA M DE O. 2013. The effect of the Ginkgo biloba extract in the expression of Bax, Bcl-2 and bone mineral content of Wistar rats with glucocorticoid-induced osteoporosis. Phytother Res 27: 515-520.). Specifically, Brayboy et al. (2001BRAYBOY JR, CHEN XW, LEE YS AND ANDERSON JJB. 2001. The protective effects of Ginkgo biloba extract (EGb 761) against free radical damage osteoblast-like bone cells (MC3T3-E1) and the proliferative effects of EGb 761 on these cells. Nutr Res 21: 275-285.) reported that EGb was effective in protecting the osteoblasts from death when they were exposed to the action of free radicals in vitro.

Consequently, Ginkgo biloba was effective in stimulating osteoblast differentiation and increase in the bone formation (Brayboy et al. 2001BRAYBOY JR, CHEN XW, LEE YS AND ANDERSON JJB. 2001. The protective effects of Ginkgo biloba extract (EGb 761) against free radical damage osteoblast-like bone cells (MC3T3-E1) and the proliferative effects of EGb 761 on these cells. Nutr Res 21: 275-285., Oh et al. 2008OH SM, KIM HR AND CHUNG KH. 2008. Effects of Ginkgo biloba on in vitro osteoblasts cells and ovariectomized rat osteoclasts cells. Arch Pharm Res 31: 216-224.). In our previous studies the EGb improved periodontal bone support and the percentual of alveolar bone in the mandible and also in the mandible it improved the expression of Bcl-2 and decreased the expression of Bax by osteoblasts. Additionally, the EGb improved the trabecular bone in femur of rats with glucocorticoid-induced osteoporosis (Lucinda et al. 2010aLUCINDA LM, DE OLIVEIRA TT, SALVADOR PA, PETERS VM, REIS JE AND GUERRA M DE O. 2010a. Radiographic evidences of mandibular osteoporosis improvement in Wistar rats treated with Ginkgo biloba. Phytother Res 24: 264-267., b, 2013). Similarly, Trivedi et al. (2009TRIVEDI R, KUMAR A, GUPTA V, KUMAR S, NAGAR GK, ROMERO JR, DWIVEDI AK AND CHATTOPADHYAY N. 2009. Effects of Egb 761 on bone mineral density, bone microstructure, and osteoblast function: Possible roles of quercetin and kaempferol. Mol Cell Endocrinol 302: 86-91.) reported that EGb improved bone mineral density (BMD) in ovariectomized rats.

Based on our previous results, the present study was designed to evaluate the effect of EGb in the biochemical marker BAP, in the BMD using dual-energy x-ray absorptiometry (DEXA) and in the mechanical properties of the tibia of Wistar rats with GIO.

MATERIALS AND METHODS

The methodology of this work was approved by the Ethical Committee on Animal Experimentation (protocol number 026/2009- CEEA, Federal University of Juiz de Fora, MG, Brazil), which follows the international principles in ethics for animal experimentation.

PLANT MATERIAL

The aqueous EGb was supplied by JR Pharma (Lot no. 20091112). The EGb used was composed of 28.2% ginkgoflavonglicosides: 8.3% of terpenolactones; 15% of quercetin glycosides; 10.9% of kaempferol glycosides; 2.3% of ishorhamnetin glycosides and less than 5 ppm of ginkgolic acids.

SODIUM ALENDRONATE

The solution of sodium alendronate was supplied by JR Pharma (India- lot no AS/004/08/2008-050309A). Alendronate of sodium in the present study was used to evaluate the efficacy of EGb. This drug is currently indicated for the treatment of glucocorticoid-induced osteoporosis and acts directly in the osteoclasts activity improving their apoptosis.

ANIMALS

Female Wistar rats (50 days old and weighing approximately 100-150 g) were obtained from the vivarium of the Federal University of Juiz de Fora, where they were born and bred. Groups of three animals were housed in clear plastic cages with stainless steel wire lids and pinewood shavings as bedding and kept in an animal room with controlled environmental conditions (12-h light/12-h dark cycle, temperature 22 ºC) on closed ventilated shelves. The animals were fed on rat chow pellets (an average of 25 g daily) and received water ad libitum.

OSTEOPOROSIS INDUCTION

The osteoporosis induction was done in the 50 day-old rats through the intramuscular administration of dexamethasone disodium phosphate (Decadron ® 4 mg/ml) at the dose level of 7 mg/Kg of body weight, once a week, during five weeks in all groups, except in the control group (Lucinda et al. 2010aLUCINDA LM, DE OLIVEIRA TT, SALVADOR PA, PETERS VM, REIS JE AND GUERRA M DE O. 2010a. Radiographic evidences of mandibular osteoporosis improvement in Wistar rats treated with Ginkgo biloba. Phytother Res 24: 264-267., b, 2013).

BIOASSAY

In this experiment, after the end of osteoporosis induction, 60 animals, 85 day-old, were selected at random and divided evenly into five groups (n=6): Osteoporosis group (dexamethasone only); EGb1 group (Extract of Ginkgo biloba 28 mg/Kg); EGb2 group (Extract of Ginkgo biloba 56 mg/Kg); Alendronate group (sodium alendronate 0.2 mg/animal/day) and Control group. The Control group was submitted to neither osteoporosis induction nor any treatment. The Alendronate, EGb1 and EGb2 groups were treated intragastrically, once a day, during 20 days (n=30) and 30 days (n=30), after the osteoporosis induction. The choice of EGb doses was based on previous studies (Lucinda et al. 2010aLUCINDA LM, DE OLIVEIRA TT, SALVADOR PA, PETERS VM, REIS JE AND GUERRA M DE O. 2010a. Radiographic evidences of mandibular osteoporosis improvement in Wistar rats treated with Ginkgo biloba. Phytother Res 24: 264-267., b, 2013). The 105 day-old animals were euthanized on the 21^st (n=30) and the 115 day -old animals on the 31^st (n=30) days. First they were anaesthetized intraperitoneally with Xylazine and Ketamine in doses of 180 mg/Kg and 10 mg/kg respectively, the blood samples (5 ml) collection was performed by cardiac puncture. Following blood collection the animals were euthanized by total exsanguination. The blood samples were centrifuged at 3000 rpm for 10 min and the serum was stored at -80 ºC during three months. Serum bone specific alkaline phosphatase (BAP) was measured using Access Ostase assay (Beckman access, Beckman Coulter Inc. Fullerton, CA, USA) (Gao et al. 2011GAO SG, LI KH, XU M, JIANG W, SHEN H, LUO W, XU WS, TIAN J AND LEI GH. 2011. Bone turnover in passive smoking female rat: relationship to change in bone mineral density. BMC Musculoskelet Disord 12: 131.). The right tibias were removed and stored at -20 ºC for 30 days until the analysis, afterward they were thawed at room temperature for four hours. Finally, the tibias were placed centrally in their anatomical position on the scanner table.

BONE MINERAL DENSITY (BMD) ANALYSIS

The BMD of the tibia was measured using DPX-ALPHA LUNAR^TM1 by bone densitometry using dual-energy x-ray absorptiometry (DEXA). The analyses were performed using the software for small animals and bones were evaluated individually (Estanislau et al. 2010ESTANISLAU CA, RAHAL SC, MULLER SS, LOUZADA MJQ AND ARAÚJO FAP. 2010. Evaluation of femur of orchiectomized guinea pigs by bone densitometry using dual-energy x-ray absorptiometry (DXA) and mechanical testing. Vet and Zootec 17: 104-112.).

BIOMECHANICAL PARAMETERS

The isolated right tibias were assessed for the three-point-bending test using the universal machine EMIC, model DL 3000. Universal machine was fitted with a load cell of 2000 N capacity at a loading rate of 5 mm/min. The graphic register enabled assays according to parameters and unities previously defined.

In the bending test of the right tibia diaphysis, the distance between two points of the support was standardized at two thirds of the specimen and load application was equidistant from each end. Tests were performed considering the following structural-mechanical properties: resilience (mJ) which was defined as the energy that the specimen admits in the elastic phase; maximum load (N) and stiffness (10³ N/m) which was defined as the relationship between load and deformation indicating the rigidity of the structure (Estanislau et al. 2010ESTANISLAU CA, RAHAL SC, MULLER SS, LOUZADA MJQ AND ARAÚJO FAP. 2010. Evaluation of femur of orchiectomized guinea pigs by bone densitometry using dual-energy x-ray absorptiometry (DXA) and mechanical testing. Vet and Zootec 17: 104-112.).

STATISTICAL ANALYSIS

The data were expressed by (mean± standard deviation) and were analyzed for statistical significance using one-way analysis of variance (ANOVA), followed by Tukey/Dunnett’T3 post-hoc test except for the control group. The control group was compared with the osteoporosis group using the Student’s t-test. p<0.05 was considered significant.

RESULTS

The values of BAP in the present study were significantly reduced in the osteoporosis group and in the EGb1, EGb2 groups (thirty days) the levels of BAP increased significantly (figure 1).

Figure 1
The levels of bone alkaline phosphatase (BAP). a - 20 days of treatment. b - 30 days of treatment. *p<0.05 when the control group was compared to the osteoporosis group (Student`s t-test). **p<0.05 when all groups, except the control, were compared to the osteoporosis group (Dunnett T3 test).

Figure 2 shows that the osteoporosis group had a significant lower BMD than the control group. The EGb2 and alendronate groups at the end of 20 and 30 days significantly recovered the BMD. The results of three-point bending test are reported in figures 3, 4 and 5. The osteoporosis group revealed a significant reduction of the bone stiffness, maximum load and resilience values when compared to the control group.

Figure 2
Bone mineral density (BMD) using dual-energy x-ray absorptiometry. a - 20 days of treatment. b - 30 days of treatment. a - *p<0.05 when the control group was compared to the osteoporosis group (Mann- Whitney test). a -**p<0.05 when all groups, except the control, were compared to the osteoporosis group (Tukey test). b - *p<0.05 when the control group was compared to the osteoporosis group (Student`s t-test). b **p<0.05 when all groups, except the control, were compared to the osteoporosis group (Dunnett T3 test).

Figure 3
Mechanical properties of the three-point bending test- Maximum load. a - 20 days of treatment. b - 30 days of treatment. *p<0.05 when the control group was compared to the osteoporosis group (Student`s t-test).

Figure 4
Mechanical properties of the three-point bending test-bone stiffness. a - 20 days of treatment. b - 30 days of treatment. *p<0.05 when the control group was compared to the osteoporosis group (Student`s t-test).

Figure 5
Mechanical properties of the three-point bending test- resilience. a - 20 days of treatment. b - 30 days of treatment. *p<0.05 when the control group was compared to the osteoporosis group (Student`s t-test).

DISCUSSION

To our knowledge, a few pre-clinical studies have been conducted to evaluate the effects of EGb in osteoporosis; the majority of them, however, employed as a model for osteoporosis induction, ovariectomized rats. We are the first group that evaluated the effects of EGb in the GIO. The aim of this study was to assess the effect of the treatment with EGb in recovering the osteoporosis induction by glucocorticoids trough mechanical tests and BMD using DEXA.

Our previous results were basically based on bone biopsy following by histomorphometric and immunohistochemestry analysis, in the present study the BMD was evaluated by DEXA that is the gold standard method for the clinical evaluation of osteoporosis.

We observed that the use of glucocorticoids reduced the BAP, BMD, the maximum load, resilience and stiffness. The treatment with EGb was effective in recovering the levels of BAP, BMD, suggesting that the extract increased bone mass in those animals, probably reducing the apoptosis of osteoblasts as showed in our previous studies (Lucinda et al. 2013LUCINDA LM, VIEIRA BJ, PETERS VM, REIS JEP, OLIVEIRA RSMF AND GUERRA M DE O. 2013. The effect of the Ginkgo biloba extract in the expression of Bax, Bcl-2 and bone mineral content of Wistar rats with glucocorticoid-induced osteoporosis. Phytother Res 27: 515-520.).

Glucocorticoid is typically associated with decreased BMD, number of osteoblasts, bone formation rate (Chang et al. 2009, Manolagas and Weinstein 1999MANOLAGAS SC AND WEINSTEIN RS. 1999. New developments in the pathogenesis and treatment of steroid-induced osteoporosis. J Bone Miner Res 14: 1061-1066., Weinstein et al. 1998) trabecular bone (Jee and Yao 2001JEE WSS AND YAO W. 2001. Overview: animal models of osteopenia and osteoporosis. J Musculoskel Neuron Interact 1: 193-207., Lucinda et al. 2010bLUCINDA LM, VIEIRA BJ, OLIVEIRA TT, SÁ RC, PETERS VM, REIS JE AND GUERRA M DE O. 2010b. Evidences of osteoporosis improvement in Wistar rats treated with Ginkgo biloba extract: a histomorphometric study of mandible and femur. Phytother Res 81: 982-987.) and biomechanical parameters (Wang et al. 2005WANG FS, LIN CL, CHEN YJ, WANG CJ, YANG KD, HUANG YT, SUN YC AND HUANG HC. 2005. Secreted Frizzled-Related Protein 1 Modulates Glucocorticoid Attenuation of Osteogenic Activities and Bone Mass. Endocrinology 146: 2415-2423.).

Biochemical markers, such as BAP, reflect the bone destruction in conditions that affect bone metabolism (Melton et al. 1997). The values of BAP in the present study were significantly reduced in the osteoporosis group (figure 1) showing an alteration in the process of bone formation and bone mineralization.

A relevant finding was that the EGb increased significantly the levels of BAP (figure 1), and such increase is a response to an anabolic therapy (Miyauchi et al. 2008MIYAUCHI A, MATSUMOTO T, SHIGETA H, TSUJIMOTO M, THIEBAUD D AND NAKAMURA T. 2008. Effect of teriparatide on bone mineral density and biochemical markers in Japanese women with postmenopausal osteoporosis: a 6-month dose-response study. J Bone Miner Metab 26: 624-634.) that is directly linked with osteoblastic activity (Duque and Rivas 2007DUQUE G AND RIVAS D. 2007. Alendronate has an anabolic effect on bone through the differentiation of mesenchymal stem cells. J Bone Miner Res 22: 1603-1611.). In accordance with the present study results, studies in vitro showed that Ginkgo biloba (100µg/ml) increased alkaline phosphatase levels in 147.2% when compared to the culture of control cells. Similarly, the EGb components, kaempferol and quercetin, were also shown to stimulate alkaline phosphatase activity in cultures of human osteoblastic cells (Oh et al. 2008OH SM, KIM HR AND CHUNG KH. 2008. Effects of Ginkgo biloba on in vitro osteoblasts cells and ovariectomized rat osteoclasts cells. Arch Pharm Res 31: 216-224., Prouillet et al. 2004PROUILLET C, MAZIÈRE J, MAZIÈRE C, WATTEL A, BRAZIER M AND KAMEL S. 2004. Stimulatory effect of naturally occurring flavonols quercetin and kaempferol on alkaline phosphatase activity in MG-63 human osteoblasts through ERK and estrogen receptor pathway. Biochem Pharmacol 67: 1307-1313.).

In the current, study we evaluated the whole right tibias with DEXA, which is currently the method of first choice for measuring BMD (Ralston 2005RALSTON SH. 2005. Bone densitometry and bone biopsy. Best Pract Res Clin Rheumatol 19: 487-501.). The higher dose of EGb was effective in recovering the BMD of the tibia as well as the alendronate, a drug that is widely used in the treatment of osteoporosis. Trivedi et al. (2009TRIVEDI R, KUMAR A, GUPTA V, KUMAR S, NAGAR GK, ROMERO JR, DWIVEDI AK AND CHATTOPADHYAY N. 2009. Effects of Egb 761 on bone mineral density, bone microstructure, and osteoblast function: Possible roles of quercetin and kaempferol. Mol Cell Endocrinol 302: 86-91.) reported an increase of the BMD in ovariectomized rats treated with EGb. The authors based their results in the improvement of the osteoblasts function and number, which was confirmed by the increase in the osteogenic genes and osteocalcin. We also believe that the EGb has an important role in increasing osteoblast function and number, once in our previous results the extract reduced the pro apoptotic protein suggesting a decrease in the osteoblasts death (Lucinda et al. 2013LUCINDA LM, VIEIRA BJ, PETERS VM, REIS JEP, OLIVEIRA RSMF AND GUERRA M DE O. 2013. The effect of the Ginkgo biloba extract in the expression of Bax, Bcl-2 and bone mineral content of Wistar rats with glucocorticoid-induced osteoporosis. Phytother Res 27: 515-520.).

Bone fragility can be defined by biomechanical parameters and it is influenced by several components including bone turnover, microarchiteture, mineralization, microdamage, collagen crosslink and mineral crystal structure (Friedman 2006FRIEDMAN AW. 2006. Important determinants of bone strength: beyound bone mineral density. J Clin Rheumatol 12: 70-77., Turner 2002TURNER CH. 2002. Biomechanics of bone: determinants of skeletal fragility and bone quality. Osteoporos Int 13: 97-104.). Glucocorticoids have been associated with rapid and significant bone loss as well as increased risk in bone fractures. In the present study the GIO showed not only a significant reduction in BMD but also reduction in the biomechanical parameters of bone like the bone stiffness, maximum load and resilience.

Despite the fact that EGb and alendronate increased the BMD, no significant improvement in the biomechanical parameters of the tibia occurred. Sliwiński et al. (2004SLIWIŃSKI L, JANIEC W, PYTLIK M, FOLWARCZNA J, KACZMARCZYK-SEDLAK I, PYTLIK W, CEGIEŁA U AND NOWIŃSKA B. 2004. Effect of administration of alendronate sodium and retinol on the mechanical properties of the femur in ovariectomized rats. Pol J Pharmacol 56: 817-824.) showed an increase in the mineral content of femoral diaphysis in the treatment with alendronate; nevertheless, it had a less significant effect on mechanical properties of the femoral diaphysis. In addition, they reported that the femoral neck, which is an area with the predominance of trabecular bone, had a significant increase of load when it was compared to the ovariectomized rats. These results may be indicative of a bigger influence of alendronate and EGb on the trabecular bone despite the cortical bone present in the diaphysis of long bones, and also lack of correlation between bone density and risk of fractures, as postulated by some researchers (Ferretti et al. 1993FERRETTI JL, CAPOZZA RF, MONDELO N AND ZANCHETTA JR. 1993. Interrelationships between densitometric, geometric, and mechanical properties of rat femora: Inferences concerning mechanical regulation of bone modeling. J Bone Miner Res 8: 1389-1396.).

Although the measurement of BMD is one of the most important tools in the diagnosis of osteoporosis it has become increasingly clear that it cannot reflect all components of bone strength. Several osteoporosis therapies, such as biphosphonates, have shown improvement in BMD; however, those changes provide only information about the quantity of bone loss or its gain and cannot fully account for changes in mechanical properties which include the architectural changes occurring in bone (Cummings et al. 2002CUMMINGS SR, KARPF DB, HARRIS F, GENANT HK, ENSRUD K, LACROIX AZ AND BLACK DM. 2002. Improvement in spine bone density and reduction in risk of vertebral fractures during treatment with antiresorptive drugs. Am J Med 112: 281-289., Watts et al. 2004WATTS NB, COOPER C, LINDSAY R, EASTELL R, MANHART MD, BARTON IP, VAN STAA TP AND ADACHI JD. 2004. Relationship between changes in bone mineral density and vertebral fracture risk associated with risedronate: greater increases in bone mineral density do not relate to greater decreases in fracture risk. Clin Densitom 7: 255-261.). For example, the increase in BMD in patients treated with risedronate was found to be independent of fracture incidence (Watts et al. 2004).

Likewise, our data showed that EGb and alendronate did not affect the biomechanical properties, apart from the BMD improvement. To our knowledge, the present study is the first one to evaluate the effect of EGb in the biomechanical parameters of tibial diaphysis and the results suggest that the EGb increase the biomechanical parameters but not in a significant way. We may speculate that the period of treatment and the dose of EGb could not be enough to recover the cortical bone of the tibia, despite the promising results with alveolar bone (Lucinda et al. 2010aLUCINDA LM, DE OLIVEIRA TT, SALVADOR PA, PETERS VM, REIS JE AND GUERRA M DE O. 2010a. Radiographic evidences of mandibular osteoporosis improvement in Wistar rats treated with Ginkgo biloba. Phytother Res 24: 264-267., b). However, Trivedi et al. (2009TRIVEDI R, KUMAR A, GUPTA V, KUMAR S, NAGAR GK, ROMERO JR, DWIVEDI AK AND CHATTOPADHYAY N. 2009. Effects of Egb 761 on bone mineral density, bone microstructure, and osteoblast function: Possible roles of quercetin and kaempferol. Mol Cell Endocrinol 302: 86-91.) reported an increase in tibial cortical bone of ovariectomized rats with EGb in a higher dose (100mg/kg/day) and with a longer period of treatment (five weeks of treatment).

In summary, the treatment with GIO reduced BMD and the biomechanical parameters of bone like the bone stiffness, maximum load and resilience. We showed that EGb restored BMD evaluated by DEXA, however no improvement in the biomechanical parameters of the tibia occurred (Lucinda et al. 2013LUCINDA LM, VIEIRA BJ, PETERS VM, REIS JEP, OLIVEIRA RSMF AND GUERRA M DE O. 2013. The effect of the Ginkgo biloba extract in the expression of Bax, Bcl-2 and bone mineral content of Wistar rats with glucocorticoid-induced osteoporosis. Phytother Res 27: 515-520.).

ACKNOWLEDGMENTS

This work was financed by Fundação de Amparo à Pesquisa do Estado de Minas Gerais (FAPEMIG) (APQ-00154-11 and 173/08). We would like to thank Cassiana M. Boya for the English review of the manuscript.

REFERENCES

BAWA S. 2010. The significance of soy protein and soy bioactive compounds in the prophylaxis and treatment of osteoporosis. J Osteoporos 8: 1-8.
BRAS M, QUEENAN B AND SUSIN S. 2005. Programmed cell death via mitochondria: different modes of dying. Biochemistry 70: 231-239.
BRAYBOY JR, CHEN XW, LEE YS AND ANDERSON JJB. 2001. The protective effects of Ginkgo biloba extract (EGb 761) against free radical damage osteoblast-like bone cells (MC3T3-E1) and the proliferative effects of EGb 761 on these cells. Nutr Res 21: 275-285.
BROWN JP ET AL. 2009. Bone turnover markers in the management of postmenopausal osteoporosis. Clin Biochem 42: 929-942.
CHANG JK, LI CJ, LIAO HJ, WANG CK, WANG GJ AND HO ML. 2009. Anti-inflammatory drugs suppress proliferation and induce apoptosis through altering expressions of cell cycle regulators and pro-apoptotic factors in cultured human osteoblasts. Toxicology 258: 148-156.
CRUSE LM, VALERIANO J, VASEY FB AND CARTER JD. 2006. Prevalence of evaluation and treatment of glucocorticoid-induced osteoporosis in men. J Clin Rheumatol 12: 221-225.
CUMMINGS SR, KARPF DB, HARRIS F, GENANT HK, ENSRUD K, LACROIX AZ AND BLACK DM. 2002. Improvement in spine bone density and reduction in risk of vertebral fractures during treatment with antiresorptive drugs. Am J Med 112: 281-289.
DUQUE G AND RIVAS D. 2007. Alendronate has an anabolic effect on bone through the differentiation of mesenchymal stem cells. J Bone Miner Res 22: 1603-1611.
ESTANISLAU CA, RAHAL SC, MULLER SS, LOUZADA MJQ AND ARAÚJO FAP. 2010. Evaluation of femur of orchiectomized guinea pigs by bone densitometry using dual-energy x-ray absorptiometry (DXA) and mechanical testing. Vet and Zootec 17: 104-112.
FELDSTEIN AC, ELMER PJ, NICHOLS GA AND HERSON M. 2005. Practice patterns in patients at risk for glucocorticoid-induced osteoporosis. Osteoporos Int 16: 2168-2174.
FERRETTI JL, CAPOZZA RF, MONDELO N AND ZANCHETTA JR. 1993. Interrelationships between densitometric, geometric, and mechanical properties of rat femora: Inferences concerning mechanical regulation of bone modeling. J Bone Miner Res 8: 1389-1396.
FRIEDMAN AW. 2006. Important determinants of bone strength: beyound bone mineral density. J Clin Rheumatol 12: 70-77.
GAO SG, LI KH, XU M, JIANG W, SHEN H, LUO W, XU WS, TIAN J AND LEI GH. 2011. Bone turnover in passive smoking female rat: relationship to change in bone mineral density. BMC Musculoskelet Disord 12: 131.
HENNEICKE H ET AL. 2011. Corticosterone selectively targets endocortical surfaces by an osteoblast-dependent mechanism. Bone 49: 733-742.
HOCK JM, KRISHNAN V, ONYIA JE, BIDWELL JP, MILAS J AND STANISLAUS D. 2001. Osteoblast Apoptosis and Bone Turnover. J Bone Miner Res 16: 975-984.
HOFF AO ET AL. 2008. Frequency and risk factors associated with osteonecrosis of the jaw in cancer patients treated with intravenous bisphosphonates. J Bone Miner Res 23: 826-836.
JEE WSS AND YAO W. 2001. Overview: animal models of osteopenia and osteoporosis. J Musculoskel Neuron Interact 1: 193-207.
JOHNELL O. 1996. Advences in osteoporosis: better identification of risk factors can reduce morbity and mortality. J Intern Med 239: 229-304.
LUCINDA LM, DE OLIVEIRA TT, SALVADOR PA, PETERS VM, REIS JE AND GUERRA M DE O. 2010a. Radiographic evidences of mandibular osteoporosis improvement in Wistar rats treated with Ginkgo biloba. Phytother Res 24: 264-267.
LUCINDA LM, VIEIRA BJ, OLIVEIRA TT, SÁ RC, PETERS VM, REIS JE AND GUERRA M DE O. 2010b. Evidences of osteoporosis improvement in Wistar rats treated with Ginkgo biloba extract: a histomorphometric study of mandible and femur. Phytother Res 81: 982-987.
LUCINDA LM, VIEIRA BJ, PETERS VM, REIS JEP, OLIVEIRA RSMF AND GUERRA M DE O. 2013. The effect of the Ginkgo biloba extract in the expression of Bax, Bcl-2 and bone mineral content of Wistar rats with glucocorticoid-induced osteoporosis. Phytother Res 27: 515-520.
MANOLAGAS SC AND WEINSTEIN RS. 1999. New developments in the pathogenesis and treatment of steroid-induced osteoporosis. J Bone Miner Res 14: 1061-1066.
MCLAUGHLIN F, MACKINTOSH J, HAYES BP, MCLAREN A, UINGS IJ, SALMON P, HUMPHREYS J, MELDRUM E AND FARROW SN. 2002. Glucocorticoid-induced osteopenia in the mouse as assessedby histomorphometry, microcomputed tomography, and biochemical markers. Bone 30: 924-930.
MELTON LJ 3RD, KHOSLA S, ATKINSON EJ, O’FALLON WM AND RIGGS BL. 1997. Relationship of bone turnover to bone density and fractures. J Bone Miner Res 12: 1083-1091.
MIYAUCHI A, MATSUMOTO T, SHIGETA H, TSUJIMOTO M, THIEBAUD D AND NAKAMURA T. 2008. Effect of teriparatide on bone mineral density and biochemical markers in Japanese women with postmenopausal osteoporosis: a 6-month dose-response study. J Bone Miner Metab 26: 624-634.
OH SM AND CHUNG KH. 2004. Estrogenic activities of Ginkgo biloba extracts. Life Sci 74: 1325-1335.
OH SM, KIM HR AND CHUNG KH. 2008. Effects of Ginkgo biloba on in vitro osteoblasts cells and ovariectomized rat osteoclasts cells. Arch Pharm Res 31: 216-224.
POZZI S ET AL. 2007. Bisphosphonate associated osteonecrosis of the jaw: a review of 35 cases and an evaluation of its frequence in multiple myeloma patients. Leuk Lynphoma 48: 1852-1854.
PROUILLET C, MAZIÈRE J, MAZIÈRE C, WATTEL A, BRAZIER M AND KAMEL S. 2004. Stimulatory effect of naturally occurring flavonols quercetin and kaempferol on alkaline phosphatase activity in MG-63 human osteoblasts through ERK and estrogen receptor pathway. Biochem Pharmacol 67: 1307-1313.
RALSTON SH. 2005. Bone densitometry and bone biopsy. Best Pract Res Clin Rheumatol 19: 487-501.
RUSSELL RG. 2006. Bisphosphonates: from bench to bedside. Ann NY Acad Sci 1068: 367-401.
SLIWIŃSKI L, JANIEC W, PYTLIK M, FOLWARCZNA J, KACZMARCZYK-SEDLAK I, PYTLIK W, CEGIEŁA U AND NOWIŃSKA B. 2004. Effect of administration of alendronate sodium and retinol on the mechanical properties of the femur in ovariectomized rats. Pol J Pharmacol 56: 817-824.
SMITH JV, BURDICK AJ, GOLIK P, KHAN I, WALLACE D AND LUO Y. 2002. Antiapoptotic properties of Ginkgo biloba extract EGb761 in differentiated PC12 cells. Cell Mol Biol 48: 699-707.
SMITH JV AND LUO Y. 2004. Studies on molecular mechanisms of Ginkgo biloba extract. Appl Microbiol Biotechnol 64: 465-472.
SZEJNFELD VL. 2000. Clinical manifestations. Osteoporosis: diagnostic and treatment. 1st ed., São Paulo: Sarvier, 406 p.
TRIVEDI R, KUMAR A, GUPTA V, KUMAR S, NAGAR GK, ROMERO JR, DWIVEDI AK AND CHATTOPADHYAY N. 2009. Effects of Egb 761 on bone mineral density, bone microstructure, and osteoblast function: Possible roles of quercetin and kaempferol. Mol Cell Endocrinol 302: 86-91.
TURNER CH. 2002. Biomechanics of bone: determinants of skeletal fragility and bone quality. Osteoporos Int 13: 97-104.
VAN BEEK TA. 2002. Chemical analysis of Ginkgo biloba leaves and extracts. J Chromatogr A 967: 21-55.
VERBORGT O, TATTON NA, MAJESKA RJ AND SCHAFFLER MB. 2002. Spatial distribution of Bax and Bcl-2 in osteocytes after bone fatigue: Complementary roles in bone remodeling regulation. J Bone Miner Res 17: 907-914.
WANG FS, LIN CL, CHEN YJ, WANG CJ, YANG KD, HUANG YT, SUN YC AND HUANG HC. 2005. Secreted Frizzled-Related Protein 1 Modulates Glucocorticoid Attenuation of Osteogenic Activities and Bone Mass. Endocrinology 146: 2415-2423.
WATTS NB, COOPER C, LINDSAY R, EASTELL R, MANHART MD, BARTON IP, VAN STAA TP AND ADACHI JD. 2004. Relationship between changes in bone mineral density and vertebral fracture risk associated with risedronate: greater increases in bone mineral density do not relate to greater decreases in fracture risk. Clin Densitom 7: 255-261.
WEINSTEIN RS, JILKA RL, PARFITT AM AND MANOLAGAS SC. 1998. Inhibition of osteoblastogenesis and promotion of apoptosis of osteoblasts and osteoclasts by glucocorticoids: Potential mechanisms of their deleterious effects on bone. J Clin Invest 102: 274-282.

Publication Dates

Publication in this collection
16 Oct 2017
Date of issue
Oct-Dec 2017

History

Received
29 July 2016
Accepted
01 Jan 2017

This is an open-access article distributed under the terms of the Creative Commons Attribution License

[1] BAWA S. 2010. The significance of soy protein and soy bioactive compounds in the prophylaxis and treatment of osteoporosis. J Osteoporos 8: 1-8.

[2] BRAS M, QUEENAN B AND SUSIN S. 2005. Programmed cell death via mitochondria: different modes of dying. Biochemistry 70: 231-239.

[3] BRAYBOY JR, CHEN XW, LEE YS AND ANDERSON JJB. 2001. The protective effects of Ginkgo biloba extract (EGb 761) against free radical damage osteoblast-like bone cells (MC3T3-E1) and the proliferative effects of EGb 761 on these cells. Nutr Res 21: 275-285.

[4] BROWN JP ET AL. 2009. Bone turnover markers in the management of postmenopausal osteoporosis. Clin Biochem 42: 929-942.

[5] CHANG JK, LI CJ, LIAO HJ, WANG CK, WANG GJ AND HO ML. 2009. Anti-inflammatory drugs suppress proliferation and induce apoptosis through altering expressions of cell cycle regulators and pro-apoptotic factors in cultured human osteoblasts. Toxicology 258: 148-156.

[6] CRUSE LM, VALERIANO J, VASEY FB AND CARTER JD. 2006. Prevalence of evaluation and treatment of glucocorticoid-induced osteoporosis in men. J Clin Rheumatol 12: 221-225.

[7] CUMMINGS SR, KARPF DB, HARRIS F, GENANT HK, ENSRUD K, LACROIX AZ AND BLACK DM. 2002. Improvement in spine bone density and reduction in risk of vertebral fractures during treatment with antiresorptive drugs. Am J Med 112: 281-289.

[8] DUQUE G AND RIVAS D. 2007. Alendronate has an anabolic effect on bone through the differentiation of mesenchymal stem cells. J Bone Miner Res 22: 1603-1611.

[9] ESTANISLAU CA, RAHAL SC, MULLER SS, LOUZADA MJQ AND ARAÚJO FAP. 2010. Evaluation of femur of orchiectomized guinea pigs by bone densitometry using dual-energy x-ray absorptiometry (DXA) and mechanical testing. Vet and Zootec 17: 104-112.

[10] FELDSTEIN AC, ELMER PJ, NICHOLS GA AND HERSON M. 2005. Practice patterns in patients at risk for glucocorticoid-induced osteoporosis. Osteoporos Int 16: 2168-2174.

[11] FERRETTI JL, CAPOZZA RF, MONDELO N AND ZANCHETTA JR. 1993. Interrelationships between densitometric, geometric, and mechanical properties of rat femora: Inferences concerning mechanical regulation of bone modeling. J Bone Miner Res 8: 1389-1396.

[12] FRIEDMAN AW. 2006. Important determinants of bone strength: beyound bone mineral density. J Clin Rheumatol 12: 70-77.

[13] GAO SG, LI KH, XU M, JIANG W, SHEN H, LUO W, XU WS, TIAN J AND LEI GH. 2011. Bone turnover in passive smoking female rat: relationship to change in bone mineral density. BMC Musculoskelet Disord 12: 131.

[14] HENNEICKE H ET AL. 2011. Corticosterone selectively targets endocortical surfaces by an osteoblast-dependent mechanism. Bone 49: 733-742.

[15] HOCK JM, KRISHNAN V, ONYIA JE, BIDWELL JP, MILAS J AND STANISLAUS D. 2001. Osteoblast Apoptosis and Bone Turnover. J Bone Miner Res 16: 975-984.

[16] HOFF AO ET AL. 2008. Frequency and risk factors associated with osteonecrosis of the jaw in cancer patients treated with intravenous bisphosphonates. J Bone Miner Res 23: 826-836.

[17] JEE WSS AND YAO W. 2001. Overview: animal models of osteopenia and osteoporosis. J Musculoskel Neuron Interact 1: 193-207.

[18] JOHNELL O. 1996. Advences in osteoporosis: better identification of risk factors can reduce morbity and mortality. J Intern Med 239: 229-304.

[19] LUCINDA LM, DE OLIVEIRA TT, SALVADOR PA, PETERS VM, REIS JE AND GUERRA M DE O. 2010a. Radiographic evidences of mandibular osteoporosis improvement in Wistar rats treated with Ginkgo biloba. Phytother Res 24: 264-267.

[20] LUCINDA LM, VIEIRA BJ, OLIVEIRA TT, SÁ RC, PETERS VM, REIS JE AND GUERRA M DE O. 2010b. Evidences of osteoporosis improvement in Wistar rats treated with Ginkgo biloba extract: a histomorphometric study of mandible and femur. Phytother Res 81: 982-987.

[21] LUCINDA LM, VIEIRA BJ, PETERS VM, REIS JEP, OLIVEIRA RSMF AND GUERRA M DE O. 2013. The effect of the Ginkgo biloba extract in the expression of Bax, Bcl-2 and bone mineral content of Wistar rats with glucocorticoid-induced osteoporosis. Phytother Res 27: 515-520.

[22] MANOLAGAS SC AND WEINSTEIN RS. 1999. New developments in the pathogenesis and treatment of steroid-induced osteoporosis. J Bone Miner Res 14: 1061-1066.

[23] MCLAUGHLIN F, MACKINTOSH J, HAYES BP, MCLAREN A, UINGS IJ, SALMON P, HUMPHREYS J, MELDRUM E AND FARROW SN. 2002. Glucocorticoid-induced osteopenia in the mouse as assessedby histomorphometry, microcomputed tomography, and biochemical markers. Bone 30: 924-930.

[24] MELTON LJ 3RD, KHOSLA S, ATKINSON EJ, O’FALLON WM AND RIGGS BL. 1997. Relationship of bone turnover to bone density and fractures. J Bone Miner Res 12: 1083-1091.

[25] MIYAUCHI A, MATSUMOTO T, SHIGETA H, TSUJIMOTO M, THIEBAUD D AND NAKAMURA T. 2008. Effect of teriparatide on bone mineral density and biochemical markers in Japanese women with postmenopausal osteoporosis: a 6-month dose-response study. J Bone Miner Metab 26: 624-634.

[26] OH SM AND CHUNG KH. 2004. Estrogenic activities of Ginkgo biloba extracts. Life Sci 74: 1325-1335.

[27] OH SM, KIM HR AND CHUNG KH. 2008. Effects of Ginkgo biloba on in vitro osteoblasts cells and ovariectomized rat osteoclasts cells. Arch Pharm Res 31: 216-224.

[28] POZZI S ET AL. 2007. Bisphosphonate associated osteonecrosis of the jaw: a review of 35 cases and an evaluation of its frequence in multiple myeloma patients. Leuk Lynphoma 48: 1852-1854.

[29] PROUILLET C, MAZIÈRE J, MAZIÈRE C, WATTEL A, BRAZIER M AND KAMEL S. 2004. Stimulatory effect of naturally occurring flavonols quercetin and kaempferol on alkaline phosphatase activity in MG-63 human osteoblasts through ERK and estrogen receptor pathway. Biochem Pharmacol 67: 1307-1313.

[30] RALSTON SH. 2005. Bone densitometry and bone biopsy. Best Pract Res Clin Rheumatol 19: 487-501.

[31] RUSSELL RG. 2006. Bisphosphonates: from bench to bedside. Ann NY Acad Sci 1068: 367-401.

[32] SLIWIŃSKI L, JANIEC W, PYTLIK M, FOLWARCZNA J, KACZMARCZYK-SEDLAK I, PYTLIK W, CEGIEŁA U AND NOWIŃSKA B. 2004. Effect of administration of alendronate sodium and retinol on the mechanical properties of the femur in ovariectomized rats. Pol J Pharmacol 56: 817-824.

[33] SMITH JV, BURDICK AJ, GOLIK P, KHAN I, WALLACE D AND LUO Y. 2002. Antiapoptotic properties of Ginkgo biloba extract EGb761 in differentiated PC12 cells. Cell Mol Biol 48: 699-707.

[34] SMITH JV AND LUO Y. 2004. Studies on molecular mechanisms of Ginkgo biloba extract. Appl Microbiol Biotechnol 64: 465-472.

[35] SZEJNFELD VL. 2000. Clinical manifestations. Osteoporosis: diagnostic and treatment. 1st ed., São Paulo: Sarvier, 406 p.

[36] TRIVEDI R, KUMAR A, GUPTA V, KUMAR S, NAGAR GK, ROMERO JR, DWIVEDI AK AND CHATTOPADHYAY N. 2009. Effects of Egb 761 on bone mineral density, bone microstructure, and osteoblast function: Possible roles of quercetin and kaempferol. Mol Cell Endocrinol 302: 86-91.

[37] TURNER CH. 2002. Biomechanics of bone: determinants of skeletal fragility and bone quality. Osteoporos Int 13: 97-104.

[38] VAN BEEK TA. 2002. Chemical analysis of Ginkgo biloba leaves and extracts. J Chromatogr A 967: 21-55.

[39] VERBORGT O, TATTON NA, MAJESKA RJ AND SCHAFFLER MB. 2002. Spatial distribution of Bax and Bcl-2 in osteocytes after bone fatigue: Complementary roles in bone remodeling regulation. J Bone Miner Res 17: 907-914.

[40] WANG FS, LIN CL, CHEN YJ, WANG CJ, YANG KD, HUANG YT, SUN YC AND HUANG HC. 2005. Secreted Frizzled-Related Protein 1 Modulates Glucocorticoid Attenuation of Osteogenic Activities and Bone Mass. Endocrinology 146: 2415-2423.

[41] WATTS NB, COOPER C, LINDSAY R, EASTELL R, MANHART MD, BARTON IP, VAN STAA TP AND ADACHI JD. 2004. Relationship between changes in bone mineral density and vertebral fracture risk associated with risedronate: greater increases in bone mineral density do not relate to greater decreases in fracture risk. Clin Densitom 7: 255-261.

[42] WEINSTEIN RS, JILKA RL, PARFITT AM AND MANOLAGAS SC. 1998. Inhibition of osteoblastogenesis and promotion of apoptosis of osteoblasts and osteoclasts by glucocorticoids: Potential mechanisms of their deleterious effects on bone. J Clin Invest 102: 274-282.

Brasil