Prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.

Thiamine (Vitamin B1) is an essential vitamin that must be obtained from the diet for proper neurological function. At higher doses, thiamine and benfotiamine (S-benzoylthiamine O-monophosphate, BT)-a phosphorylated derivative of thiamine-have antinociceptive effects in animals and humans, although...

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Main Authors: Julie K Hurt, Jennifer L Coleman, Brendan J Fitzpatrick, Bonnie Taylor-Blake, Arlene S Bridges, Pirkko Vihko, Mark J Zylka
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23119057/pdf/?tool=EBI
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spelling doaj-94a81905acde459b9e7dc4a62c01d6f92021-03-03T20:26:50ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01710e4856210.1371/journal.pone.0048562Prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.Julie K HurtJennifer L ColemanBrendan J FitzpatrickBonnie Taylor-BlakeArlene S BridgesPirkko VihkoMark J ZylkaThiamine (Vitamin B1) is an essential vitamin that must be obtained from the diet for proper neurological function. At higher doses, thiamine and benfotiamine (S-benzoylthiamine O-monophosphate, BT)-a phosphorylated derivative of thiamine-have antinociceptive effects in animals and humans, although how these compounds inhibit pain is unknown. Here, we found that Prostatic acid phosphatase (PAP, ACPP) can dephosphorylate BT in vitro, in dorsal root ganglia (DRG) neurons and in primary-afferent axon terminals in the dorsal spinal cord. The dephosphorylated product S-benzoylthiamine (S-BT) then decomposes to O-benzoylthiamine (O-BT) and to thiamine in a pH-dependent manner, independent of additional enzymes. This unique reaction mechanism reveals that BT only requires a phosphatase for conversion to thiamine. However, we found that the antinociceptive effects of BT, thiamine monophosphate (TMP) and thiamine-a compound that is not phosphorylated-were entirely dependent on PAP at the spinal level. Moreover, pharmacokinetic studies with wild-type and Pap(-/-) mice revealed that PAP is not required for the conversion of BT to thiamine in vivo. Taken together, our study highlights an obligatory role for PAP in the antinociceptive effects of thiamine and phosphorylated thiamine analogs, and suggests a novel phosphatase-independent function for PAP.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23119057/pdf/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Julie K Hurt
Jennifer L Coleman
Brendan J Fitzpatrick
Bonnie Taylor-Blake
Arlene S Bridges
Pirkko Vihko
Mark J Zylka
spellingShingle Julie K Hurt
Jennifer L Coleman
Brendan J Fitzpatrick
Bonnie Taylor-Blake
Arlene S Bridges
Pirkko Vihko
Mark J Zylka
Prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.
PLoS ONE
author_facet Julie K Hurt
Jennifer L Coleman
Brendan J Fitzpatrick
Bonnie Taylor-Blake
Arlene S Bridges
Pirkko Vihko
Mark J Zylka
author_sort Julie K Hurt
title Prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.
title_short Prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.
title_full Prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.
title_fullStr Prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.
title_full_unstemmed Prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.
title_sort prostatic acid phosphatase is required for the antinociceptive effects of thiamine and benfotiamine.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Thiamine (Vitamin B1) is an essential vitamin that must be obtained from the diet for proper neurological function. At higher doses, thiamine and benfotiamine (S-benzoylthiamine O-monophosphate, BT)-a phosphorylated derivative of thiamine-have antinociceptive effects in animals and humans, although how these compounds inhibit pain is unknown. Here, we found that Prostatic acid phosphatase (PAP, ACPP) can dephosphorylate BT in vitro, in dorsal root ganglia (DRG) neurons and in primary-afferent axon terminals in the dorsal spinal cord. The dephosphorylated product S-benzoylthiamine (S-BT) then decomposes to O-benzoylthiamine (O-BT) and to thiamine in a pH-dependent manner, independent of additional enzymes. This unique reaction mechanism reveals that BT only requires a phosphatase for conversion to thiamine. However, we found that the antinociceptive effects of BT, thiamine monophosphate (TMP) and thiamine-a compound that is not phosphorylated-were entirely dependent on PAP at the spinal level. Moreover, pharmacokinetic studies with wild-type and Pap(-/-) mice revealed that PAP is not required for the conversion of BT to thiamine in vivo. Taken together, our study highlights an obligatory role for PAP in the antinociceptive effects of thiamine and phosphorylated thiamine analogs, and suggests a novel phosphatase-independent function for PAP.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23119057/pdf/?tool=EBI
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