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Citations to this article

Alkaline phosphatase: placental and tissue-nonspecific isoenzymes hydrolyze phosphoethanolamine, inorganic pyrophosphate, and pyridoxal 5'-phosphate. Substrate accumulation in carriers of hypophosphatasia corrects during pregnancy.
M P Whyte, … , J D Mahuren, S P Coburn
M P Whyte, … , J D Mahuren, S P Coburn
Published April 1, 1995
Citation Information: J Clin Invest. 1995;95(4):1440-1445. https://doi.org/10.1172/JCI117814.
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Research Article Article has an altmetric score of 9

Alkaline phosphatase: placental and tissue-nonspecific isoenzymes hydrolyze phosphoethanolamine, inorganic pyrophosphate, and pyridoxal 5'-phosphate. Substrate accumulation in carriers of hypophosphatasia corrects during pregnancy.

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Abstract

Hypophosphatasia features selective deficiency of activity of the tissue-nonspecific (liver/bone/kidney) alkaline phosphatase (ALP) isoenzyme (TNSALP); placental and intestinal ALP isoenzyme (PALP and IALP, respectively) activity is not reduced. Three phosphocompounds (phosphoethanolamine [PEA], inorganic pyrophosphate [PPi], and pyridoxal 5'-phosphate [PLP]) accumulate endogenously and appear, therefore, to be natural substrates for TNSALP. Carriers for hypophosphatasia may have decreased serum ALP activity and elevated substrate levels. To test whether human PALP and TNSALP are physiologically active toward the same substrates, we studied PEA, PPi, and PLP levels during and after pregnancy in three women who are carriers for hypophosphatasia. Hypophosphatasemia corrected during the third trimester because of PALP in maternal blood. Blood or urine concentrations of PEA, PPi, and PLP diminished substantially during that time. After childbirth, maternal circulating levels of PALP decreased, and PEA, PPi, and PLP levels abruptly increased. In serum, unremarkable concentrations of IALP and low levels of TNSALP did not change during the study period. We conclude that PALP, like TNSALP, is physiologically active toward PEA, PPi, and PLP in humans. We speculate from molecular/crystallographic information, indicating significant similarity of structure of the substrate-binding site of ALPs throughout nature, that all ALP isoenzymes recognize these same three phosphocompound substrates.

Authors

M P Whyte, M Landt, L M Ryan, R A Mulivor, P S Henthorn, K N Fedde, J D Mahuren, S P Coburn

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Citations to this article in year 2008 (7)

Title and authors Publication Year
Phosphate: Known and potential roles during development and regeneration of teeth and supporting structures
BL Foster, KA Tompkins, RB Rutherford, H Zhang, EY Chu, H Fong, MJ Somerman
Birth Defects Research Part C: Embryo Today: Reviews 2008
How can calcium pyrophosphate crystals induce inflammation in hypophosphatasia or chronic inflammatory joint diseases?
C Beck, H Morbach, P Richl, M Stenzel, HJ Girschick
Rheumatology International 2008
Case Report
F Barvencik, M Gebauer, T Schinke, M Amling
Clinical Orthopaedics and Related Research 2008
Selective drug delivery to bone using acidic oligopeptides
J Ishizaki, Y Waki, T Takahashi-Nishioka, K Yokogawa, K Miyamoto
Journal of Bone and Mineral Metabolism 2008
Inhibition of alkaline phosphatase by thioureido derivatives of methylenebisphosphonic acid
AI Vovk, AL Chuiko, LA Kononets, VY Tanchuk, IV Murav’eva, MO Lozinsky, VP Kukhar
Russian Journal of Bioorganic Chemistry 2008
Principles of Bone Biology
CJ Rosen, T Niu
Principles of Bone Biology 2008
Effects of pyrophosphate on desmal and endochondral mineralization and TNAP activity in organoid culture
B Zimmermann
Annals of Anatomy - Anatomischer Anzeiger 2008

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