Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:2.4.2.7 (
adenine phosphoribosyltransferase
)
692
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Mouse teratocarcinoma stem cells deficient in activity of
adenine phosphoribosyltransferase
(
APRT
;
EC 2.4.2.7
) were obtained in order to have this marker in developmentally versatile cells. Mutagenized stem-cell cultures were selected for resistance to 8-azaadenine and four clonal cell lines were isolated. Three had severe deficiencies of
APRT
activity (7% or less of wild type) and one had a moderate reduction (73%). The enzyme in the latter clone was found to be an electrophoretic variant with slightly less anodal migration than the wild-type enzyme. Each clone remained stably
APRT
-deficient for at least 3 1/2 weeks, after subcutaneous inoculation, in the absence of the selective agent. The tumors formed from the inocula comprised a variety of differentiated tissues and thus showed persistence of stem-cell developmental pluripotency despite mutagenesis and selection. All mutants also retained the quasinormal karyotype (X/O sex chromosomal constitution,
trisomy
-19) of the parent line. These lines are appropriate for such uses as production (by blastocyst injection) of mouse models of the human genetic deficiency and for foreign-gene transfer, via teratocarcinoma cells, into mice.
...
PMID:Mouse teratocarcinoma mutant clones deficient in adenine phosphoribosyltransferase and developmentally pluripotent. 29 85
Two cousins with
trisomy
for the distal third of 16q due to a familial translocation, t(16;21)(q22.2;q22.2), are reported. The
APRT
gene locus could be assigned to 16q22.2 to 16qter. The phenotypic similarities of the first patient, who had
trisomy
16q22.3 to 16qter and monosomy 21q22.3, to six other patients with partial
trisomy
16q reported in literature allows the delineation of a syndrome due to
trisomy
16qter. In the second patient, with
trisomy
16q22.3 to 16qter and
trisomy
21pter to 21q22.2, similar features are present, but in association with the classical symptoms of trisomy 21.
...
PMID:[Increased activity of adenine phosphoribosyl transferase in a child trisomic for 16q22.2 to 16qter due to malsegregation of a t(16;21) (q22.2;q22;2)pat]. 629 60
Two cousins with
trisomy
for the distal third of 16q due to a familial translocation, t(16;21)(q22.2;q22-2), are reported. The
APRT
gene locus could be assigned to 16q22.2 to 16qter. The phenotypic similarities of the first patient, who had
trisomy
16q22.3 to 16qter and monosomy 21q22.3, to six other patients with partial
trisomy
16q reported in literature allows the delineation of a syndrome due to
trisomy
16qter. In the second patient, with
trisomy
16q22.3 to 16qter and
trisomy
21pter to 21q22.2 similar features are present but in association with the classical symptoms of trisomy 21.
...
PMID:[Increased activity of adenine phosphoribosyl transferase in a child trisomic for 16q22.2 to 16qter due to malsegregation of a t(16;21) (q22.2;q22;2)pat (author's transl)]. 697 98
