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115 research outputs found

Collagenous gastritis, a new spectrum of disease in pediatric patients: two case reports

Author: Christie Dennis
Kapur Raj P
Murray Karen
Suskind David
Wahbeh Ghassan
Publication venue: Cases Network Ltd
Publication date: 01/01/2009
Field of study

Collagenous gastritis is a rare gastrointestinal disorder characterized in pediatrics by abdominal pain and anemia. The literature divides collagenous gastritis into distinct pediatric-onset and adult-onset phenotypes. As opposed to pediatric form, the adult form is associated with collagenous colitis and presents clinically with voluminous non-bloody diarrhea. There are over 25 case reports of collagenous gastritis of which 10 are pediatric cases. We present two cases of pediatric onset collagenous gastritis: one with a classic pediatric presentation, the other with findings typical of adult-onset disease. This is the first report of the adult-onset phenotype collagenous gastritis in a pediatric patient

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PubMed Central

The Politics of Preemption and the War on Terror in Europe

Author: Ackerman Bruce
Adams John
Adams John
Adams John
Alvaro Alexander Nuno
Amnesty International EU Office
Andersson Torbjörn
Arendt Hannah
Ash Timothy Garton
Baker Tom
Balibar Étienne
Banks Christopher P.
Bigo Didier
Bigo Didier
Bunyan Tony
Bush George W.
Butler Judith
Cameron Iain
Cauley Leslie
Chertoff Michael
Clarke Charles
Coker Christopher
Cole David
Cole David
Commission of the European Communities
Council of the European Union
Council of the European Union
Court of First Instance
Court of First Instance
Cox Michael
De Goede Marieke
De Goede Marieke
Dershowitz Alan M.
Dimitriu Eugenia
EDPWP European Data Protection Working Party
Engström Mats
Ericson Richard V.
Ericson Richard V.
European Court of Justice
European Parliament and the Council of the European Union
European Security Strategy
Foucault Michel
Goede
Hansell Saul
Huysmans Jef
Lyon David
Marieke De Goede
Neve Rudie
O'Harrow Robert
O'Malley Pat
Rees Wyn
Roth John
Runciman David
Snow John
Stalder Felix
Suskind Ron
Suskind Ron
Vedder Anton
Vlcek William
Walters William
White House
Zalm Gerrit
Zarate Juan Carlos
Zureik Elia
Publication venue: 'SAGE Publications'
Publication date
Field of study

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Maternal microchimerism in the livers of patients with Biliary atresia

Author: A Nonomura
B Fischler
B Fischler
C Shimazaki
David L Suskind
Denice Kong
EL Assche
F Amersi
FM Karrer
Greg Magrane
HZ Hu
J Schroder
J. Chang M., Lee H., Muench M.O. Chen
JA Bezerra
JA Sterling
JG Ocejo-Vinyals
JL Ferrara
JM Ben-Ezra
Lee-Ann Baxter-Lowe
M Hollander
M Hollander
M Nakada
Marcus O Muench
Melvin B Heyman
NJ Chao
Philip Rosenthal
PW Dillon
R Ohi
SM Müller
T Ohya
U Broome
VJ Desmet
W Reed
YM Lo
Publication venue: BioMed Central
Publication date: 01/01/2004
Field of study

BACKGROUND: Biliary atresia (BA) is a neonatal cholestatic disease of unknown etiology. It is the leading cause of liver transplantation in children. Many similarities exist between BA and graft versus host disease suggesting engraftment of maternal cells during gestation could result in immune responses that lead to BA. The aim of this study was to determine the presence and extent of maternal microchimerism (MM) in the livers of infants with BA. METHODS: Using fluorescent in situ hybridization (FISH), 11 male BA & 4 male neonatal hepatitis (NH) livers, which served as controls, were analyzed for X and Y-chromosomes. To further investigate MM in BA, 3 patients with BA, and their mothers, were HLA typed. Using immunohistochemical stains, the BA livers were examined for MM. Four additional BA livers underwent analysis by polymerase chain reaction (PCR) for evidence of MM. RESULTS: By FISH, 8 BA and 2 NH livers were interpretable. Seven of eight BA specimens showed evidence of MM. The number of maternal cells ranged from 2–4 maternal cells per biopsy slide. Neither NH specimen showed evidence of MM. In addition, immunohistochemical stains confirmed evidence of MM. Using PCR, a range of 1–142 copies of maternal DNA per 25,000 copies of patients DNA was found. CONCLUSIONS: Maternal microchimerism is present in the livers of patients with BA and may contribute to the pathogenesis of BA

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Directory of Open Access Journals

PubMed Central

Comparison of gastrointestinal pH in cystic fibrosis and healthy subjects

Author: A Benn
AM Connell
AM Weber
AV Aynaciyan
BJ Boyle
Carole A. Youngberg
CF Abrams
DJS Cameron
DM Chalmers
DM Small
DR Yarbrough
EA Mitchell
EG Nassif
EH Mischler
F Bieville De
FB Kopel
Gordon L. Amidon
H Worning
HP Chase
HP Chase
HW Smith
James H. Meyer
JB Dressman
Jennifer B. Dressman
JN Isenberg
JR Malagelada
K Gaskin
KL Cox
KL Cox
KT Khaw
L Ehrhardt
LP DiMagno
M Corey
Martha L. Hyneck
PL Zentler-Munro
PR Durie
PR Durie
R Gow
RC Talamo
RE Knauff
RF McCloy
RM Suskind
Rosemary R. Berardi
S Lemire
SJ Rune
SK Dutta
SS David
VLW Go
VS Hubbard
VS Hubbard
VS Hubbard
WC Watson
WD Heizer
WH Steinberg
William F. Howatt
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/05/1987
Field of study

The primary objective of this study was to define the pH conditions under which supplemental pancreatic enzyme preparations must function in the upper gastrointestinal tract. The hypothesis was that normal or greater gastric acid output in patients with cystic fibrosis (CF), combined with low pancreatic bicarbonate output, results in an acidic duodenal pH, compromising both dosage-form performance and enzyme activity. Gastrointestinal pH profiles were obtained in 10 CF and 10 healthy volunteers under fasting and postprandial conditions. A radiotelemetric monitoring method, the Heidelberg capsule, was used to continuously monitor pH. Postprandial duodenal pH was lower in CF than in healthy subjects, especially in the first postprandial hour (mean time greater than pH 6 was 5 min in CF, 11 min in healthy subjects, P <0.05). Based on the dissolution pH profiles of current enteric-coated pancreatic enzyme products, the duodenal postprandial pH in CF subjects may be too acidic to permit rapid dissolution of current enteric-coated dosage forms. However, the pH was above 4 more than 90% of the time on the average, suggesting that irreversible lipase inactivation in the duodenum is not likely to be a significant limitation to enzyme efficacy. Overall results suggest that slow dissolution of pH-sensitive coatings, rather than enzyme inactivation, may contribute to the failure of enteric-coated enzyme supplements to normalize fat absorption.Peer Reviewedhttp://deepblue.lib.umich.edu/bitstream/2027.42/44403/1/10620_2005_Article_BF01296029.pd

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Deep Blue Documents at the University of Michigan