Your search keyword '"Akarca US"' showing total 102 results

101. Detection of precore hepatitis B virus mutants in asymptomatic HBsAg-positive family members.

Author

Akarca US, Greene S, and Lok AS

Subjects

Adolescent, Adult, Base Sequence, Child, Child, Preschool, DNA Primers chemistry, DNA, Viral analysis, DNA, Viral chemistry, Family, Female, Follow-Up Studies, Hepatitis B transmission, Hepatitis B e Antigens blood, Humans, Male, Middle Aged, Molecular Sequence Data, Polymerase Chain Reaction, Carrier State microbiology, Hepatitis B microbiology, Hepatitis B Surface Antigens blood, Hepatitis B virus genetics, Mutation

Abstract

Precore hepatitis B virus mutants have been detected mainly in HBeAg-negative patients with active liver disease. We previously reported two novel mutations: M1 (C-to-T change at nucleotide 1856 [proser at codon 15]) and M3 (G-to-A change at nucleotide 1898 [gly-ser at codon 29]) in addition to two well-described mutations: M2 (G-to-A change at nucleotide 1896 [trp-stop at codon 28]); and M4 (G-to-A change at nucleotide 1899 [gly-asp at codon 29]) in Chinese patients. The aims of this study were to determine (a) the prevalence of precore HBV mutations in asymptomatic carriers and (b) whether family members share the same mutated sequence as the index patients. Fifty-three index patients and 89 HBsAg-positive family members were studied by means of direct sequencing of polymerase chain reaction-amplified hepatitis B virus DNA. M0, a conserved mutation (T-to-C at nucleotide 1858, codon 15), was detected in 81% and 12% family members of index patients with and without M0, respectively (p < 0.0001). The clustering of M0 indicates that most subjects were infected through intrafamilial transmission. M1 was detected in all the family members of patients with M1 but in none of the family members of patients with wild-type or M2 sequences (p < 0.0001). M2 was detected in 25%, 0% and 15% of family members of patients with M2, M1 and WT sequences, respectively (p = 0.19). M3 was detected in five and M4 in four family members.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1994

102. Characterization of somatostatin receptor subtypes controlling rat gastric acid and pancreatic amylase release.

Author

Rossowski WJ, Gu ZF, Akarca US, Jensen RT, and Coy DH

Subjects

Amino Acid Sequence, Animals, Dose-Response Relationship, Drug, Gastric Mucosa drug effects, Male, Molecular Sequence Data, Pancreas drug effects, Pentagastrin pharmacology, Peptide Fragments pharmacology, Rats, Receptors, Somatostatin classification, Receptors, Somatostatin drug effects, Structure-Activity Relationship, Amylases metabolism, Gastric Acid metabolism, Pancreas enzymology, Receptors, Somatostatin physiology, Somatostatin analogs & derivatives, Somatostatin pharmacology

Abstract

An examination of the binding characteristics of a large number of somatostatin analogues with respect to the five known somatostatin receptor subtypes has recently resulted in the discovery of several peptides with some selectivity for types 2, 3, and 4 and little affinity for type 1 or 5 receptor. A panel of these peptides has thus far implicated type 2 receptors in the inhibition of release of pituitary growth hormone and type 4 receptors in inhibiting pancreatic insulin release. In the present article, we have examined the inhibitory effects of the same group of peptides on in vivo rat gastric acid and pancreatic amylase release and binding to rat pancreatic acinar cells. The type 2-selective ligand NC-8-12 was a potent inhibitor of gastric acid release (EC50s in the 1.5 nM region) whereas the type 4-selective ligand, DC-23-99, elicited little response. However, some involvement of type 3 receptors could not be ruled out because the type 3-selective analogue, DC-25-20, exhibited inhibitory effects at higher dose levels (EC50 > 10 nM). Conversely, the type 4 analogue was a potent inhibitor of amylase release (EC50 1.1 nM) whereas the type 3 analogue had no significant effects at doses tested. DC-23-99 also bound with high affinity to rat acinar cells (EC50 3.8 nM), whereas DC-25-20 exhibited more than 10-fold less affinity. Thus, these two major biological functions of somatostatin appear to be controlled by different receptors and, furthermore, effects on both endocrine and exocrine pancreas appear to be type 4 receptor mediated.

Published

1994