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Query: UNIPROT:P00492 (
hypoxanthine-guanine phosphoribosyltransferase
)
2,385
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
2-Amino-1-methyl-6-phenylimidazo[4,5-b]pyridine
(PhIP), a heterocyclic aromatic amine that is formed in abundance in cooked meats, has been found to be mutagenic in human lymphoblastoid TK6 cells at the thymidine kinase and hypoxanthine-guanine phosphoribosyl transferase (hgprt) loci. The mutations induced at the hgprt locus have been analysed. Of the mutations that have been identified, 60% were found in the coding sequence of the gene. Forty percent were in the introns which resulted in aberrant splicing and consequently, leading to exon losses in the mature
hprt
mRNA. Mutations resulting in a loss of exonIII appeared most frequently followed by losses of exonVI, exonVIII and partial loss of exonIX. All identified mutations occurred at GC base pairs, consistent with the adducts of PhIP that have been found previously and suggesting that the N-(deoxyguanosin-8-yl)-2-amino-1-methyl-6-phenylimidazo[4,5- b]pyridine, (dG-C8-PhIP) adduct may be the premutagenic lesion. Most of the mutations are GC-->TA transversions except for a cluster of single base pair deletions in a run of guanines. There appears to be strand bias in the induction of mutations with 85% of the mutations on the non-transcribed strand. Although the number of mutations analysed is limited (54 mutants), there are several sites (positions 166 and 207 of the coding sequence, and the splice acceptor site of exonIII) which are overrepresented. There is a preference for a 5' purine but not a strong bias for 3' A as has been found for other mutagens that form a premutagenic lesion at G. Triplet analysis shows that the triplets, 5'GGA3' and 5'AGG3', where the middle base is mutated are preferred.
...
PMID:Analysis of mutations induced by 2-amino-1-methyl-6-phenylimidazo[4,5-b]pyridine (PhIP) in human lymphoblastoid cells. 772 48
1. Heterocyclic amines are formed in parts per billion levels when meat is cooked. 2. The heterocyclic amines MeIQx and
PhIP
are efficiently absorbed into the systemic circulation after ingestion of cooked food. 3. We have shown that MeIQx and
PhIP
, both in vitro and in vivo, are substrates for human hepatic CYP1A2, which exclusively and efficiently catalyses their conversion to genotoxic hydroxylamines. 4. MeIQx and
PhIP
are promutagens. MeIQx is a very powerful bacterial mutagen whereas
PhIP
is a more potent mammalian cell mutagen. Using a mammalian cell target gene,
hprt
, we have shown that
PhIP
induces a characteristic mutational 'fingerprint'. 5. MeIQx and
PhIP
are carcinogenic in bioassays. The
PhIP
mutational 'fingerprint' has been detected in the Apc gene of 5/8 colonic tumours induced by
PhIP
in rats.
...
PMID:Heterocyclic amines: evaluation of their role in diet associated human cancer. 880 49
Heterocyclic amines such as MeIQx and
PhIP
are potent genotoxic chemicals which are formed at part per billion levels when meat is cooked. Using assays based on gas chromatography/mass spectrometry with stable isotope labelled analogues as internal standards we have demonstrated MeIQx and
PhIP
, are efficiently absorbed into the systemic circulation after ingestion of fried beef. Using a potent and selective inhibitor of human CYP1A2, furafylline, we have shown that N-hydroxylation catalysed by this enzyme is the major pathway of metabolism of MeIQx and
PhIP
and is solely responsible for their oxidation to mutagenic species. This is in contrast to the situation in laboratory animals in which both activation by N-hydroxylation and deactivation by C-oxidation occurs. When furafylline was administered to human volunteers before ingestion of fried beef, we showed that > 90% of MeIQx and approximately 70% of
PhIP
elimination could be inhibited, demonstrating the extent to which activation occurred in man. MeIQx is a very powerful mutagen in bacterial assays whereas
PhIP
is a more potent mammalian cell mutagen. Using a mammalian cell target gene,
hprt
, we have shown that
PhIP
induces a characteristic mutational 'fingerprint' which is identical to that detected in the Apc gene of 5/8 colonic tumours induced by
PhIP
in rats. These studies support a biological association between HA exposure and diet-related tumours but emphasise that information obtained from animal studies does not always reflect the situation in humans.
...
PMID:Assessing human risk to heterocyclic amines. 920 38
Heterocyclic amines are ubiquitously present in cooked meats and fish. They represent an important class of food-borne carcinogens. We describe the cytotoxic, apoptotic, and mutagenic responses of mismatch repair-proficient (TK6) and mismatch repair-deficient (MT1) human lymphoblastoid cells to
PhIP
, the most abundant heterocyclic amine. Dose-dependent increases in cytotoxicity, in apoptosis, and in mutant fractions at the
hprt
locus were observed following
PhIP
treatment. We present a statistical method that is useful for comparing two populations. With this method, we show that the data fitted a model that assumes that the
PhIP
-induced mutation rate is dependent on the cell line. Estimated rates of increase of 22.8 x 10(-6) and 2.2 x 10(-6) mutation per cell per microg
PhIP
were found in MT1 and TK6, respectively, showing that MT1 is hypermutable to
PhIP
. MT1 also exhibited lower
PhIP
-induced apoptosis. We conclude from these results that mismatch repair-deficient cells are hypermutable to the food-borne carcinogen
PhIP
and that the
PhIP
-DNA adducts, when not eliminated by apoptosis, can be transformed into mutations.
...
PMID:Comparison of the mutagenic responses of mismatch repair-proficient (TK6) and mismatch repair-deficient (MT1) human lymphoblast cells to the food-borne carcinogen PhIP. 1177 64
