Download pdf - Treatment with eldecalcitol (ED-71) and raloxifene ... · Product Research Dept., Chugai Pharmaceutical Co., Ltd., Gotemba, Japan Backgrounds •Eldecalcitol (ED‐71; ELD), a 2β‐hydroxypropyloxy

Treatment with eldecalcitol (ED-71) and raloxifene combined increases cancellous and cortical bone strength in ovariectomized rats.

S d ki S k i S t hi T k d A k Shi i hi N b K ik M hik Mih d K i hi E dSadaoki Sakai, Satoshi Takeda, Ayako Shiraishi, Nobuo Koike, Masahiko Mihara and Koichi EndoProduct Research Dept., Chugai Pharmaceutical Co., Ltd., Gotemba, Japan

Backgrounds•Eldecalcitol (ED‐71; ELD), a 2β‐hydroxypropyloxy derivative of 1α,25(OH)2D3, was approved for treatment of osteoporosis in Japan in 2011.•ELD significantly reduced the incidence of vertebral and wrist fractures compared with alfacalcidol, a prodrug of 1α,25(OH)2D3, in a 3‐year clinical study [1].

ObjectiveTo compare the effects of combining ELD and RAL against each monotherapy in osteoporotic rats.

Summary

The combination treatment with ELD and RAL•ELD inhibited osteoclastic bone resorption and increased bone mass more potently than alfacalcidol in ovariectomized (OVX) rats [2].•Raloxifene (RAL), a selective estrogen receptor modulator, is globally approved for the treatment and prevention of postmenopausal osteoporosis.•There are no reports describing the efficacy of combination treatment of ELD with RAL in osteoporosis patients or in animal models.

[1] Matsumoto T et al. Bone 49: 605 (2011) [2] Uchiyama Y et al. Bone 30: 582 (2002)

Results

The combination treatment with ELD and RALimproved bone mechanical strength by suppressing bone turnover and increasing BMD more than either monotherapyreduced the rise of blood Ca and urinary Ca excretion seen in ELD monotherapy.may avoid excessive reduction of bone turnover.showed additive effect on inhibition of mouse bone marrow osteoclastogenesis.

Fig. 1 Bone resorption marker

4 wks 8 wks 12 wks

Sham Vehicle ELD RAL ELD+RAL

OVXShamVehicle ELD RAL ELD+RAL

OVX

ShamVehicle ELD RAL ELD+RAL

OVX

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ELD + RAL significantly decreased urinary DPD compared with ELD (4 wks) or RAL (4, 8 and 12 wks) monotherapy.

Fig. 2 Bone mineral density

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Ultimate load Work to failure

Fig. 3 Mechanical strength of lumbar vertebra (L5) and femoral midshaft

Compression test of L5

Fig. 4 Bone histomorphometry

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ELD + RAL decreased the number of osteoclast compared with RAL monotherapy, and lowered bone formation parameters to sham control levels.

The combination treatment increased the mechanical strength of lumbar vertebra and femoral midshaft.

g y

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/cm

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Lumbar spine Femur (whole)

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ELD + RAL significantly increased BMD of lumbar spine and femur compared with either monotherapy.

OVX OVX

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3‐point bending test of femoral midshaft

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Bone formation rate

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Methods

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Proximal femur Mid femur Distal femur

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Mean + SD s P < 0.05 vs. sham by unpaired t‐test.v P < 0.05 vs. OVX + vehicle, e P < 0.05 vs. OVX + ELD, r P < 0.05 vs. OVX + RAL by Tukey’s multiple comparison test.

OVX


Serum Ca (mg/dL) 10.34±0.31 9.92±0.23 s 10.72±0.36v 9.62±0.24 10.25±0.34 e,r

Urinary Ca/Cre 0.037±0.011 0.038±0.011 0.346±0.058 v 0.042±0.054 0.198±0.046v,e,r

e

e

Table 1 Serum Ca and urinary Ca/Cre (12 wk)

ELD + RAL reduced the increase in serum Ca and urinary Ca/Cre by ELD.Sham Vehicle ELD RAL ELD+RAL

OVX

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MA

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Sham Vehicle ELD RAL ELD+RAL0

0.05 v,r

Fig. 5 In vitro osteoclastogenesis In vivo In vitro

BF

R/B

S (m

Animals: 8‐month‐old female Wistar‐Imamichi ratsTreatment: Daily, 12 weeks, by oral gavageGroups: (n = 10)

Sham VehicleOVX VehicleOVX ELD 7.5 ng/kgOVX RAL 0.3 mg/kgOVX ELD 7.5 ng/kg + RAL 0.3 mg/kg

samplesOVX

Treatment ( daily, oral gavage)

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urineurine

Vehicle ELD

RAL ELD + RAL

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Number of TRAP positive multinucleated osteoclasts

v, r

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with or without10‐7M ELD 10‐6M RAL10‐7M ELD + 10‐6M RAL

Mouse Bone Marrow 30 ng/mL M‐CSF30 ng/mL RANKL

Count a number of TRAP positive multinucleated osteoclast.

The combination treatment with ELD and RAL showed additive effect on inhibition of mouse bone marrow osteoclastogenesis.

7 days

bone, urine, serum

(/well)

Measurements:Bone resorption marker: Urinary deoxypyridinoline (DPD)BMD: Lumbar spine (L2‐L4), femurBone biomechanical strength: Lumbar vertebral body (L5), femurBone histomorphometry: Lumbar vertebral body (L3)Serum calcium (Ca), urinary Ca, urinary creatinine (Cre)

n=3v p<0.05 vs Vehicle by Tukey’s multiple comparison testr p<0.05 vs RAL by Tukey’s multiple comparison test

0

20

40

V ELD7 RAL6 COMVehicle ELD ELD + RALRAL

【COI】 All authors are employees of Chugai Pharmaceutical Co., Ltd.