1982
DOI: 10.1515/dmdi.1982.4.4.289
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Drug-Pyridoxal Phosphate Interactions

Abstract: In this review it has been pointed out that vitamin B6 and its vitamers can be involved in many interactions with a number of drugs, as well as with the actions of various endocrines and neurotransmitters. Nutritional deficiencies, especially of vitamins and proteins, can affect the manner in which drugs undergo biotransformation, and thereby may also modify the therapeutic efficacy of certain drugs. The differences between nutritional vitamin B6 deficiency and the hereditary disorder producing pyridoxine depe… Show more

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Cited by 21 publications
(12 citation statements)
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References 180 publications
(183 reference statements)
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“…Anti-TB drugs such as linezolid, cycloserine, isoniazid, fluoroquinolones, SLDs, ethambutol, and ethionamide are blamed for peripheral neuropathy ( Gupta et al, 2020 ). These drugs interfere with pyridoxine metabolism by various mechanisms ( Ebadi et al, 1982 ; Cohen, 2001 ). In the present study, only cycloserine was suspected of causing neuropathy.…”
Section: Discussionmentioning
confidence: 99%
“…Anti-TB drugs such as linezolid, cycloserine, isoniazid, fluoroquinolones, SLDs, ethambutol, and ethionamide are blamed for peripheral neuropathy ( Gupta et al, 2020 ). These drugs interfere with pyridoxine metabolism by various mechanisms ( Ebadi et al, 1982 ; Cohen, 2001 ). In the present study, only cycloserine was suspected of causing neuropathy.…”
Section: Discussionmentioning
confidence: 99%
“…6 Esto no explicaría la persistencia del temblor, midriasis e hiperreflexia 72 h después de la convulsión, pero sí pueden corresponderse con un nivel elevado de serotonina en el SNC. 7 Se consideró el síndrome neuroléptico maligno (SNM) como diagnóstico diferencial.…”
Section: Discussionunclassified
“…In human biopsy specimen, hydrocortisone pretreatments induced twoto sixfold increases in hepatic TDO activity [222,223]. In light of TDO induction by (adrenal) glucocorticoids [224], it is instructive that PLP "in physiological concentrations seems to function as an endogenous 'down regulator' of a number of receptor sites" (including those for glucocorticoids) [225], whereby PLP insuffi ciencies infl uence diverse hormone:receptor complexes and cognate end-organ responses. Other (ancillary) regulatory mechanisms underlying TDO activity include [184]: substrate-based stabilization against enzymatic degradation; conversion of apoenzyme into holoenzyme by conjugation with ferriprotoporphyrin IX (hematin) or ferroprotoporphyrin IX (heme) prosthetic groups; reductive activation of the oxidized holoenzyme, e. g., by trace hydrogen peroxide [226]; and allosteric feedback inhibition by pyridine nucleotides (a.k.a.…”
Section: Potential Toxicity Of Large Doses Of Single Amino Acidsmentioning
confidence: 99%