The role of phosphatases in the initiation of skeletal mineralization.
TLDR
It is shown that PHOSPHO1, a soluble phosphatase with specificity for two molecules present in MVs, phosphoethanolamine and phosphocholine, is responsible for initiating HA crystal formation inside MVs and that PHosPHO 1 and TNAP have nonredundant functional roles during endochondral ossification.Abstract:
Endochondral ossification is a carefully orchestrated process mediated by promoters and inhibitors of mineralization. Phosphatases are implicated, but their identities and functions remain unclear. Mutations in the tissue-nonspecific alkaline phosphatase (TNAP) gene cause hypophosphatasia, a heritable form of rickets and osteomalacia, caused by an arrest in the propagation of hydroxyapatite (HA) crystals onto the collagenous extracellular matrix due to accumulation of extracellular inorganic pyrophosphate (PPi), a physiological TNAP substrate and a potent calcification inhibitor. However, TNAP knockout (Alpl(-/-)) mice are born with a mineralized skeleton and have HA crystals in their chondrocyte- and osteoblast-derived matrix vesicles (MVs). We have shown that PHOSPHO1, a soluble phosphatase with specificity for two molecules present in MVs, phosphoethanolamine and phosphocholine, is responsible for initiating HA crystal formation inside MVs and that PHOSPHO1 and TNAP have nonredundant functional roles during endochondral ossification. Double ablation of PHOSPHO1 and TNAP function leads to the complete absence of skeletal mineralization and perinatal lethality, despite normal systemic phosphate and calcium levels. This strongly suggests that the Pi needed for initiation of MV-mediated mineralization is produced locally in the perivesicular space. As both TNAP and nucleoside pyrophosphohydrolase-1 (NPP1) behave as potent ATPases and pyrophosphatases in the MV compartment, our current model of the mechanisms of skeletal mineralization implicate intravesicular PHOSPHO1 function and Pi influx into MVs in the initiation of mineralization and the functions of TNAP and NPP1 in the extravesicular progression of mineralization.read more
Citations
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Journal ArticleDOI
A homozygous intronic branch-point deletion in the ALPL gene causes infantile hypophosphatasia.
TL;DR: The functional characterization of a gene mutation detected in intron 7 of the ALPL gene of a boy with infantile HPP, in whom routine sequencing of the coding region failed to detect any mutation, reaffirm that in clear cut clinical cases, deeper analyses of regulatory important motifs like branch-point sequences are required to establish a genetic diagnosis.
Journal ArticleDOI
Loss of Nmp4 optimizes osteogenic metabolism and secretion to enhance bone quality.
Yu Shao,Emily Wichern,Paul Childress,Michele Adaway,Jagannath Misra,Angela Klunk,David B. Burr,David B. Burr,Ronald C. Wek,Amber L. Mosley,Yunlong Liu,Alexander G. Robling,Nickolay Brustovetsky,James A. Hamilton,Kylie Jacobs,Deepak Vashishth,Keith R. Stayrook,Matthew R. Allen,Matthew R. Allen,Joseph M. Wallace,Joseph M. Wallace,Joseph P. Bidwell +21 more
TL;DR: This paper showed that mice lacking the transcription factor nuclear matrix protein 4 (Nmp4, Zfp384, Ciz, ZNF384) respond to osteoporosis therapy.
Journal ArticleDOI
Reappearance of hypomineralized bone after discontinuation of asfotase alfa treatment for severe childhood hypophosphatasia.
Sasigarn A. Bowden,B. H. Adler +1 more
TL;DR: Treatment outcome after asfotase alfa treatment for 1 year in a 16-year-old male with severe childhood HPP, and the importance of continuing therapy to improve his bone health and prevent further skeletal deteriorations is emphasized.
Journal ArticleDOI
Matrix vesicle biomimetics harboring Annexin A5 and alkaline phosphatase bind to the native collagen matrix produced by mineralizing vascular smooth muscle cells.
Maytê Bolean,Benedetta Izzi,Soetkin Van kerckhoven,Massimo Bottini,Ana Paula Ramos,José Luis Millán,Marc Hoylaerts,Pietro Ciancaglini +7 more
TL;DR: These findings support the hypothesis that TNAP is cleaved from the MVs membrane just before ECM binding, such facilitating MV anchoring to ECM via AnxA5 interaction, and help to develop novel therapeutic strategies to prevent or inhibit ectopic mineralization.
Journal ArticleDOI
Docosahexaenoic Acid (DHA) Inhibits Bone Morphogenetic Protein-2 (BMP-2) Elevated Osteoblast Potential of Metastatic Breast Cancer (MDA-MB-231) Cells in Mammary Microcalcification
TL;DR: It is unraveled for the first time that DHA may mitigate microcalcification by blocking osteoblast-like potential of breast cancer cells by showing an inhibitory effect on BMP-2 induced osteoblasts presumably by abrogating BMP signaling.
References
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Book
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TL;DR: It is suggested that matrix vesicles are derived from cells and that they may play a role in initiating calcification at the epiphysis.
Journal ArticleDOI
Tissue-nonspecific alkaline phosphatase and plasma cell membrane glycoprotein-1 are central antagonistic regulators of bone mineralization
Lovisa Hessle,Kristen Johnson,H. Clarke Anderson,Sonoko Narisawa,Adnan Sali,James W. Goding,Robert Terkeltaub,José Luis Millán +7 more
TL;DR: The results suggest that inhibiting PC-1 function may be a viable therapeutic strategy for hypophosphatasia, and interfere with TNAP activity may correct pathological hyperossification because of PPi insufficiency.
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TL;DR: Robison was able to study for two years in Leipzig in the kdbordtories of Professor Hantz as mentioned in this paper, where he obtained a scholarship to attend the University of Nottingham.
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