Ectopic calcification in pseudoxanthoma elasticum responds to inhibition of tissue-nonspecific alkaline phosphatase

Shira G. Ziegler; Carlos R. Ferreira; Elena Gallo Macfarlane; Ryan C. Riddle; Ryan E. Tomlinson; Emily Y. Chew; Ludovic Martin; Chen Ting Ma; Eduard Sergienko; Anthony B. Pinkerton; José Luis Millán; William A. Gahl; Harry C. Dietz

doi:10.1126/scitranslmed.aal1669

Ectopic calcification in pseudoxanthoma elasticum responds to inhibition of tissue-nonspecific alkaline phosphatase

Shira G. Ziegler, Carlos R. Ferreira, Elena Gallo Macfarlane, Ryan C. Riddle, Ryan E. Tomlinson, Emily Y. Chew, Ludovic Martin, Chen Ting Ma, Eduard Sergienko, Anthony B. Pinkerton, José Luis Millán, William A. Gahl, Harry C. Dietz

Research output: Contribution to journal › Article › peer-review

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Abstract

Biallelic mutations in ABCC6 cause pseudoxanthoma elasticum (PXE), a disease characterized by calcification in the skin, eyes, and blood vessels. The function of ATP-binding cassette C6 (ABCC6) and the pathogenesis of PXE remain unclear. We used mouse models and patient fibroblasts to demonstrate genetic interaction and shared biochemical and cellular mechanisms underlying ectopic calcification in PXE and related disorders caused by defined perturbations in extracellular adenosine 5′-Triphosphate catabolism. Under osteogenic culture conditions, ABCC6 mutant cells calcified, suggesting a provoked cell-Autonomous defect. Using a conditional Abcc6 knockout mouse model, we excluded the prevailing pathogenic hypothesis that singularly invokes failure of hepatic secretion of an endocrine inhibitor of calcification. Instead, deficiency of Abcc6 in both local and distant cells was necessary to achieve the early onset and penetrant ectopic calcification observed upon constitutive gene targeting. ABCC6 mutant cells additionally had increased expression and activity of tissuenonspecific alkaline phosphatase (TNAP), an enzyme that degrades pyrophosphate, a major inhibitor of calcification. A selective and orally bioavailable TNAP inhibitor prevented calcification in ABCC6 mutant cells in vitro and attenuated both the development and progression of calcification in Abcc6^-/- mice in vivo, without the deleterious effects on bone associated with other proposed treatment strategies.

Original language	English (US)
Article number	eaal1669
Journal	Science translational medicine
Volume	9
Issue number	393
DOIs	https://doi.org/10.1126/scitranslmed.aal1669
State	Published - Jun 7 2017

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General Medicine

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Ziegler, S. G., Ferreira, C. R., Macfarlane, E. G., Riddle, R. C., Tomlinson, R. E., Chew, E. Y., Martin, L., Ma, C. T., Sergienko, E., Pinkerton, A. B., Millán, J. L., Gahl, W. A., & Dietz, H. C. (2017). Ectopic calcification in pseudoxanthoma elasticum responds to inhibition of tissue-nonspecific alkaline phosphatase. Science translational medicine, 9(393), Article eaal1669. https://doi.org/10.1126/scitranslmed.aal1669

Ziegler, SG, Ferreira, CR, Macfarlane, EG, Riddle, RC, Tomlinson, RE, Chew, EY, Martin, L, Ma, CT, Sergienko, E, Pinkerton, AB, Millán, JL, Gahl, WA & Dietz, HC 2017, 'Ectopic calcification in pseudoxanthoma elasticum responds to inhibition of tissue-nonspecific alkaline phosphatase', Science translational medicine, vol. 9, no. 393, eaal1669. https://doi.org/10.1126/scitranslmed.aal1669

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title = "Ectopic calcification in pseudoxanthoma elasticum responds to inhibition of tissue-nonspecific alkaline phosphatase",

abstract = "Biallelic mutations in ABCC6 cause pseudoxanthoma elasticum (PXE), a disease characterized by calcification in the skin, eyes, and blood vessels. The function of ATP-binding cassette C6 (ABCC6) and the pathogenesis of PXE remain unclear. We used mouse models and patient fibroblasts to demonstrate genetic interaction and shared biochemical and cellular mechanisms underlying ectopic calcification in PXE and related disorders caused by defined perturbations in extracellular adenosine 5′-Triphosphate catabolism. Under osteogenic culture conditions, ABCC6 mutant cells calcified, suggesting a provoked cell-Autonomous defect. Using a conditional Abcc6 knockout mouse model, we excluded the prevailing pathogenic hypothesis that singularly invokes failure of hepatic secretion of an endocrine inhibitor of calcification. Instead, deficiency of Abcc6 in both local and distant cells was necessary to achieve the early onset and penetrant ectopic calcification observed upon constitutive gene targeting. ABCC6 mutant cells additionally had increased expression and activity of tissuenonspecific alkaline phosphatase (TNAP), an enzyme that degrades pyrophosphate, a major inhibitor of calcification. A selective and orally bioavailable TNAP inhibitor prevented calcification in ABCC6 mutant cells in vitro and attenuated both the development and progression of calcification in Abcc6-/- mice in vivo, without the deleterious effects on bone associated with other proposed treatment strategies.",

author = "Ziegler, {Shira G.} and Ferreira, {Carlos R.} and Macfarlane, {Elena Gallo} and Riddle, {Ryan C.} and Tomlinson, {Ryan E.} and Chew, {Emily Y.} and Ludovic Martin and Ma, {Chen Ting} and Eduard Sergienko and Pinkerton, {Anthony B.} and Mill{\'a}n, {Jos{\'e} Luis} and Gahl, {William A.} and Dietz, {Harry C.}",

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AU - Ziegler, Shira G.

AU - Ferreira, Carlos R.

AU - Macfarlane, Elena Gallo

AU - Riddle, Ryan C.

AU - Tomlinson, Ryan E.

AU - Chew, Emily Y.

AU - Martin, Ludovic

AU - Ma, Chen Ting

AU - Sergienko, Eduard

AU - Pinkerton, Anthony B.

AU - Millán, José Luis

AU - Gahl, William A.

AU - Dietz, Harry C.

PY - 2017/6/7

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N2 - Biallelic mutations in ABCC6 cause pseudoxanthoma elasticum (PXE), a disease characterized by calcification in the skin, eyes, and blood vessels. The function of ATP-binding cassette C6 (ABCC6) and the pathogenesis of PXE remain unclear. We used mouse models and patient fibroblasts to demonstrate genetic interaction and shared biochemical and cellular mechanisms underlying ectopic calcification in PXE and related disorders caused by defined perturbations in extracellular adenosine 5′-Triphosphate catabolism. Under osteogenic culture conditions, ABCC6 mutant cells calcified, suggesting a provoked cell-Autonomous defect. Using a conditional Abcc6 knockout mouse model, we excluded the prevailing pathogenic hypothesis that singularly invokes failure of hepatic secretion of an endocrine inhibitor of calcification. Instead, deficiency of Abcc6 in both local and distant cells was necessary to achieve the early onset and penetrant ectopic calcification observed upon constitutive gene targeting. ABCC6 mutant cells additionally had increased expression and activity of tissuenonspecific alkaline phosphatase (TNAP), an enzyme that degrades pyrophosphate, a major inhibitor of calcification. A selective and orally bioavailable TNAP inhibitor prevented calcification in ABCC6 mutant cells in vitro and attenuated both the development and progression of calcification in Abcc6-/- mice in vivo, without the deleterious effects on bone associated with other proposed treatment strategies.

AB - Biallelic mutations in ABCC6 cause pseudoxanthoma elasticum (PXE), a disease characterized by calcification in the skin, eyes, and blood vessels. The function of ATP-binding cassette C6 (ABCC6) and the pathogenesis of PXE remain unclear. We used mouse models and patient fibroblasts to demonstrate genetic interaction and shared biochemical and cellular mechanisms underlying ectopic calcification in PXE and related disorders caused by defined perturbations in extracellular adenosine 5′-Triphosphate catabolism. Under osteogenic culture conditions, ABCC6 mutant cells calcified, suggesting a provoked cell-Autonomous defect. Using a conditional Abcc6 knockout mouse model, we excluded the prevailing pathogenic hypothesis that singularly invokes failure of hepatic secretion of an endocrine inhibitor of calcification. Instead, deficiency of Abcc6 in both local and distant cells was necessary to achieve the early onset and penetrant ectopic calcification observed upon constitutive gene targeting. ABCC6 mutant cells additionally had increased expression and activity of tissuenonspecific alkaline phosphatase (TNAP), an enzyme that degrades pyrophosphate, a major inhibitor of calcification. A selective and orally bioavailable TNAP inhibitor prevented calcification in ABCC6 mutant cells in vitro and attenuated both the development and progression of calcification in Abcc6-/- mice in vivo, without the deleterious effects on bone associated with other proposed treatment strategies.

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Ectopic calcification in pseudoxanthoma elasticum responds to inhibition of tissue-nonspecific alkaline phosphatase

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