Inhibiting the osteocyte-specific protein sclerostin increases bone mass and fracture resistance in multiple myeloma

Michelle M. McDonald; Michaela R. Reagan; Scott E. Youlten; Sindhu T. Mohanty; Anja Seckinger; Rachael L. Terry; Jessica A. Pettitt; Marija K. Simic; Tegan L. Cheng; Alyson Morse; Lawrence M.T. Le; David Abi-Hanna; Ina Kramer; Carolyne Falank; Heather Fairfield; Irene M. Ghobrial; Paul A. Baldock; David G. Little; Michaela Kneissel; Karin Vanderkerken; J. H.Duncan Bassett; Graham R. Williams; Babatunde O. Oyajobi; Dirk Hose; Tri G. Phan; Peter I. Croucher

doi:10.1182/blood-2017-03-773341

Inhibiting the osteocyte-specific protein sclerostin increases bone mass and fracture resistance in multiple myeloma

Michelle M. McDonald, Michaela R. Reagan, Scott E. Youlten, Sindhu T. Mohanty, Anja Seckinger, Rachael L. Terry, Jessica A. Pettitt, Marija K. Simic, Tegan L. Cheng, Alyson Morse, Lawrence M.T. Le, David Abi-Hanna, Ina Kramer, Carolyne Falank, Heather Fairfield, Irene M. Ghobrial, Paul A. Baldock, David G. Little, Michaela Kneissel, Karin VanderkerkenJ. H.Duncan Bassett, Graham R. Williams, Babatunde O. Oyajobi, Dirk Hose, Tri G. Phan, Peter I. Croucher

Department of Cell Systems & Anatomy

Resultado de la investigación: Article › revisión exhaustiva

135 Citas (Scopus)

Resumen

Multiple myeloma (MM) is a plasma cell cancer that develops in the skeleton causing profound bone destruction and fractures. The bone disease is mediated by increased osteoclastic bone resorption and suppressed bone formation. Bisphosphonates used for treatment inhibit bone resorption and prevent bone loss but fail to influence bone formation and do not replace lost bone, so patients continue to fracture. Stimulating bone formation to increase bone mass and fracture resistance is a priority; however, targeting tumor-derived modulators of bone formation has had limited success. Sclerostin is an osteocyte-specific Wnt antagonist that inhibits bone formation. We hypothesized that inhibiting sclerostin would prevent development of bone disease and increase resistance to fracture in MM. Sclerostin was expressed in osteocytes from bones from naive and myeloma-bearing mice. In contrast, sclerostin was not expressed by plasma cells from 630 patients with myeloma or 54 myeloma cell lines. Mice injected with 5TGM1-eGFP, 5T2MM, or MM1.S myeloma cells demonstrated significant bone loss, which was associated with a decrease in fracture resistance in the vertebrae. Treatment with anti-sclerostin antibody increased osteoblast numbers and bone formation rate but did not inhibit bone resorption or reduce tumor burden. Treatment with anti-sclerostin antibody prevented myeloma-induced bone loss, reduced osteolytic bone lesions, and increased fracture resistance. Treatment with anti-sclerostin antibody and zoledronic acid combined increased bone mass and fracture resistance when compared with treatment with zoledronic acid alone. This study defines a therapeuticstrategysuperior tothecurrent standardof care that will reducefractures forpatients with MM.

Idioma original	English (US)
Páginas (desde-hasta)	3452-3464
Número de páginas	13
Publicación	Blood
Volumen	129
N.º	26
DOI	https://doi.org/10.1182/blood-2017-03-773341
Estado	Published - jun 29 2017

ASJC Scopus subject areas

Hematology
Biochemistry
Cell Biology
Immunology

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10.1182/blood-2017-03-773341

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McDonald, M. M., Reagan, M. R., Youlten, S. E., Mohanty, S. T., Seckinger, A., Terry, R. L., Pettitt, J. A., Simic, M. K., Cheng, T. L., Morse, A., Le, L. M. T., Abi-Hanna, D., Kramer, I., Falank, C., Fairfield, H., Ghobrial, I. M., Baldock, P. A., Little, D. G., Kneissel, M., ... Croucher, P. I. (2017). Inhibiting the osteocyte-specific protein sclerostin increases bone mass and fracture resistance in multiple myeloma. Blood, 129(26), 3452-3464. https://doi.org/10.1182/blood-2017-03-773341

McDonald, MM, Reagan, MR, Youlten, SE, Mohanty, ST, Seckinger, A, Terry, RL, Pettitt, JA, Simic, MK, Cheng, TL, Morse, A, Le, LMT, Abi-Hanna, D, Kramer, I, Falank, C, Fairfield, H, Ghobrial, IM, Baldock, PA, Little, DG, Kneissel, M, Vanderkerken, K, Bassett, JHD, Williams, GR, Oyajobi, BO, Hose, D, Phan, TG & Croucher, PI 2017, 'Inhibiting the osteocyte-specific protein sclerostin increases bone mass and fracture resistance in multiple myeloma', Blood, vol. 129, n.º 26, pp. 3452-3464. https://doi.org/10.1182/blood-2017-03-773341

@article{5ba7d06d3163442d8c39709ae775de64,

title = "Inhibiting the osteocyte-specific protein sclerostin increases bone mass and fracture resistance in multiple myeloma",

abstract = "Multiple myeloma (MM) is a plasma cell cancer that develops in the skeleton causing profound bone destruction and fractures. The bone disease is mediated by increased osteoclastic bone resorption and suppressed bone formation. Bisphosphonates used for treatment inhibit bone resorption and prevent bone loss but fail to influence bone formation and do not replace lost bone, so patients continue to fracture. Stimulating bone formation to increase bone mass and fracture resistance is a priority; however, targeting tumor-derived modulators of bone formation has had limited success. Sclerostin is an osteocyte-specific Wnt antagonist that inhibits bone formation. We hypothesized that inhibiting sclerostin would prevent development of bone disease and increase resistance to fracture in MM. Sclerostin was expressed in osteocytes from bones from naive and myeloma-bearing mice. In contrast, sclerostin was not expressed by plasma cells from 630 patients with myeloma or 54 myeloma cell lines. Mice injected with 5TGM1-eGFP, 5T2MM, or MM1.S myeloma cells demonstrated significant bone loss, which was associated with a decrease in fracture resistance in the vertebrae. Treatment with anti-sclerostin antibody increased osteoblast numbers and bone formation rate but did not inhibit bone resorption or reduce tumor burden. Treatment with anti-sclerostin antibody prevented myeloma-induced bone loss, reduced osteolytic bone lesions, and increased fracture resistance. Treatment with anti-sclerostin antibody and zoledronic acid combined increased bone mass and fracture resistance when compared with treatment with zoledronic acid alone. This study defines a therapeuticstrategysuperior tothecurrent standardof care that will reducefractures forpatients with MM.",

author = "McDonald, {Michelle M.} and Reagan, {Michaela R.} and Youlten, {Scott E.} and Mohanty, {Sindhu T.} and Anja Seckinger and Terry, {Rachael L.} and Pettitt, {Jessica A.} and Simic, {Marija K.} and Cheng, {Tegan L.} and Alyson Morse and Le, {Lawrence M.T.} and David Abi-Hanna and Ina Kramer and Carolyne Falank and Heather Fairfield and Ghobrial, {Irene M.} and Baldock, {Paul A.} and Little, {David G.} and Michaela Kneissel and Karin Vanderkerken and Bassett, {J. H.Duncan} and Williams, {Graham R.} and Oyajobi, {Babatunde O.} and Dirk Hose and Phan, {Tri G.} and Croucher, {Peter I.}",

note = "Funding Information: This work was supported by: Janice Gibson and the Ernest Heine Family Foundation (P.I.C.); an Australian Research Council Future Fellowship (P.A.B.); the National Institutes of Health, National Institute of GeneralMedical Sciences (grantGM106391) andNational Institute of Diabetes andDigestive andKidneyDiseases (grant R24 DK092759-01); theAmerican Cancer SocietyResearch (grant IRG-16-191-33); start-up funding from the Maine Medical Center Research Institute (M.R.R.); a Kay Stubbs Cancer Research Grant, Cancer Council New South Wales; and the Deutsche Forschungsgemeinschaft (grant SFB/TRR79, TP B1, B12, M9) and the German Federal Ministry of Education (Clinically-Applicable, Omics-based Assessment of Survival, Side Effects, and Targets in Multiple Myeloma [CLIOMMICS] [grant 01ZX1309] and Clinical ApplicableMultimodal Prediction of Survival in Multiple Myeloma [CAMPSIMM] [grant 01ES1103]). Publisher Copyright: {\textcopyright} 2017 by The American Society of Hematology.",

year = "2017",

month = jun,

day = "29",

doi = "10.1182/blood-2017-03-773341",

language = "English (US)",

volume = "129",

pages = "3452--3464",

journal = "Blood",

issn = "0006-4971",

publisher = "American Society of Hematology",

number = "26",

}

TY - JOUR

T1 - Inhibiting the osteocyte-specific protein sclerostin increases bone mass and fracture resistance in multiple myeloma

AU - McDonald, Michelle M.

AU - Reagan, Michaela R.

AU - Youlten, Scott E.

AU - Mohanty, Sindhu T.

AU - Seckinger, Anja

AU - Terry, Rachael L.

AU - Pettitt, Jessica A.

AU - Simic, Marija K.

AU - Cheng, Tegan L.

AU - Morse, Alyson

AU - Le, Lawrence M.T.

AU - Abi-Hanna, David

AU - Kramer, Ina

AU - Falank, Carolyne

AU - Fairfield, Heather

AU - Ghobrial, Irene M.

AU - Baldock, Paul A.

AU - Little, David G.

AU - Kneissel, Michaela

AU - Vanderkerken, Karin

AU - Bassett, J. H.Duncan

AU - Williams, Graham R.

AU - Oyajobi, Babatunde O.

AU - Hose, Dirk

AU - Phan, Tri G.

AU - Croucher, Peter I.

N1 - Funding Information: This work was supported by: Janice Gibson and the Ernest Heine Family Foundation (P.I.C.); an Australian Research Council Future Fellowship (P.A.B.); the National Institutes of Health, National Institute of GeneralMedical Sciences (grantGM106391) andNational Institute of Diabetes andDigestive andKidneyDiseases (grant R24 DK092759-01); theAmerican Cancer SocietyResearch (grant IRG-16-191-33); start-up funding from the Maine Medical Center Research Institute (M.R.R.); a Kay Stubbs Cancer Research Grant, Cancer Council New South Wales; and the Deutsche Forschungsgemeinschaft (grant SFB/TRR79, TP B1, B12, M9) and the German Federal Ministry of Education (Clinically-Applicable, Omics-based Assessment of Survival, Side Effects, and Targets in Multiple Myeloma [CLIOMMICS] [grant 01ZX1309] and Clinical ApplicableMultimodal Prediction of Survival in Multiple Myeloma [CAMPSIMM] [grant 01ES1103]). Publisher Copyright: © 2017 by The American Society of Hematology.

PY - 2017/6/29

Y1 - 2017/6/29

N2 - Multiple myeloma (MM) is a plasma cell cancer that develops in the skeleton causing profound bone destruction and fractures. The bone disease is mediated by increased osteoclastic bone resorption and suppressed bone formation. Bisphosphonates used for treatment inhibit bone resorption and prevent bone loss but fail to influence bone formation and do not replace lost bone, so patients continue to fracture. Stimulating bone formation to increase bone mass and fracture resistance is a priority; however, targeting tumor-derived modulators of bone formation has had limited success. Sclerostin is an osteocyte-specific Wnt antagonist that inhibits bone formation. We hypothesized that inhibiting sclerostin would prevent development of bone disease and increase resistance to fracture in MM. Sclerostin was expressed in osteocytes from bones from naive and myeloma-bearing mice. In contrast, sclerostin was not expressed by plasma cells from 630 patients with myeloma or 54 myeloma cell lines. Mice injected with 5TGM1-eGFP, 5T2MM, or MM1.S myeloma cells demonstrated significant bone loss, which was associated with a decrease in fracture resistance in the vertebrae. Treatment with anti-sclerostin antibody increased osteoblast numbers and bone formation rate but did not inhibit bone resorption or reduce tumor burden. Treatment with anti-sclerostin antibody prevented myeloma-induced bone loss, reduced osteolytic bone lesions, and increased fracture resistance. Treatment with anti-sclerostin antibody and zoledronic acid combined increased bone mass and fracture resistance when compared with treatment with zoledronic acid alone. This study defines a therapeuticstrategysuperior tothecurrent standardof care that will reducefractures forpatients with MM.

AB - Multiple myeloma (MM) is a plasma cell cancer that develops in the skeleton causing profound bone destruction and fractures. The bone disease is mediated by increased osteoclastic bone resorption and suppressed bone formation. Bisphosphonates used for treatment inhibit bone resorption and prevent bone loss but fail to influence bone formation and do not replace lost bone, so patients continue to fracture. Stimulating bone formation to increase bone mass and fracture resistance is a priority; however, targeting tumor-derived modulators of bone formation has had limited success. Sclerostin is an osteocyte-specific Wnt antagonist that inhibits bone formation. We hypothesized that inhibiting sclerostin would prevent development of bone disease and increase resistance to fracture in MM. Sclerostin was expressed in osteocytes from bones from naive and myeloma-bearing mice. In contrast, sclerostin was not expressed by plasma cells from 630 patients with myeloma or 54 myeloma cell lines. Mice injected with 5TGM1-eGFP, 5T2MM, or MM1.S myeloma cells demonstrated significant bone loss, which was associated with a decrease in fracture resistance in the vertebrae. Treatment with anti-sclerostin antibody increased osteoblast numbers and bone formation rate but did not inhibit bone resorption or reduce tumor burden. Treatment with anti-sclerostin antibody prevented myeloma-induced bone loss, reduced osteolytic bone lesions, and increased fracture resistance. Treatment with anti-sclerostin antibody and zoledronic acid combined increased bone mass and fracture resistance when compared with treatment with zoledronic acid alone. This study defines a therapeuticstrategysuperior tothecurrent standardof care that will reducefractures forpatients with MM.

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DO - 10.1182/blood-2017-03-773341

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AN - SCOPUS:85021774938

SN - 0006-4971

VL - 129

SP - 3452

EP - 3464

JO - Blood

JF - Blood

IS - 26

ER -

Inhibiting the osteocyte-specific protein sclerostin increases bone mass and fracture resistance in multiple myeloma

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