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: UMLS:C0262471 (
ENT
)
5,307
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
This study considers the efficacity of the ambulatory aerosol therapy in chronic cases of the
ENT
area. A nebulizer, air-jet type, of 4 microns MMAD, was the device employed, and an ample spectre antibiotic (cefotaxime) a mucolytic (N-acetyl-
cysteine
) plus a corticoid (methyl-prednisolone) the associated drugs. The antibiotic was discarded when otitis were the problem. The results have been favourable in 75 percent of the cases whilst negative in the resting 24 percent of the treated subjects.
...
PMID:[Ambulatory aerosol therapy in the treatment of chronic pathology of the O.R.L. region]. 189 3
Human equilibrative nucleoside transporter 1 (hENT1), the first identified member of the
ENT
family of integral membrane proteins, is the primary mechanism for cellular uptake of physiologic nucleosides and many antineoplastic and antiviral nucleoside drugs. hENT1, which is potently inhibited by nitrobenzylthioinosine (NBMPR), possesses 11 transmembrane helical domains with an intracellular N-terminus and an extracellular C-terminus. As a protein with 10 endogenous
cysteine
residues, it is sensitive to inhibition by the membrane permeable sulfhydryl-reactive reagent
N
-ethylmaleimide (NEM) but is unaffected by the membrane impermeable sulfhydryl-reactive reagent
p
-chloromercuriphenyl sulfonate. To identify the residue(s) involved in NEM inhibition, we created a
cysteine
-less version of hENT1 (hENT1C-), with all 10 endogenous
cysteine
residues mutated to serine, and showed that it displays wild-type uridine transport and NBMPR-binding characteristics when produced in the
Xenopus
oocyte heterologous expression system, indicating that endogenous
cysteine
residues are not essential for hENT1 function. We then tested NEM sensitivity of recombinant wild-type hENT1, hENT1 mutants C1S to C10S (single
cysteine
residues replaced by serine), hENT1C- (all
cysteine
residues replaced by serine), and hENT1C- mutants S1C to S10C (single serine residues converted back to
cysteine
). Mutants C9S (C416S/hENT1) and S9C (S416C/hENT1C-) were insensitive and sensitive, respectively, to inhibition by NEM, identifying Cys
416
as the endofacial
cysteine
residue in hENT1 responsible for NEM inhibition. Kinetic experiments suggested that NEM modification of Cys
416
, which is located at the inner extremity of TM10, results in the inhibition of hENT1 uridine transport and NBMPR binding by constraining the protein in its inward-facing conformation.
...
PMID:Role of cysteine 416 in
N
-ethylmaleimide sensitivity of human equilibrative nucleoside transporter 1 (hENT1). 3025 99
