Harvey Young scite author profile

We have conducted a genome screen of autism, by linkage analysis in an initial set of 90 multiplex sibships, with parents, containing 97 independent affected sib pairs (ASPs), with follow-up in 49 additional multiplex sibships, containing 50 ASPs. In total, 519 markers were genotyped, including 362 for the initial screen, and an additional 157 were genotyped in the follow-up. As a control, we also included in the analysis unaffected sibs, which provided 51 discordant sib pairs (DSPs) for the initial screen and 29 for the follow-up. In the initial phase of the work, we observed increased identity by descent (IBD) in the ASPs (sharing of 51.6%) compared with the DSPs (sharing of 50.8%). The excess sharing in the ASPs could not be attributed to the effect of a small number of loci but, rather, was due to the modest increase in the entire distribution of IBD. These results are most compatible with a model specifying a large number of loci (perhaps >/=15) and are less compatible with models specifying

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Increased risk of colorectal neoplasia in patients with primary sclerosing cholangitis and ulcerative colitis: A meta-analysis

Soetikno

Lin

Heidenreich

et al. 2002

Gastrointestinal Endoscopy

550

251

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Accelerated improvement of alcoholic liver disease with enteral nutrition

Kearns¹,

Young²,

Garcia³

et al. 1992

Gastroenterology

240

114

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Guidelines for credentialing and granting privileges for endoscopic ultrasound

Eisen¹,

Dominitz²,

Faigel³

et al. 2001

Gastrointestinal Endoscopy

212

133

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Gene Expression Profiling Reveals Stromal Genes Expressed in Common Between Barrett’s Esophagus and Adenocarcinoma

Ying

Triadafilopoulos

Sahbaie³

et al. 2006

Gastroenterology

131

133

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Background & Aims-Barrett's esophagus is a precursor of esophageal adenocarcinoma. DNA microarrays that enable a genome-wide assessment of gene expression enhance the identification of specific genes as well as gene expression patterns that are expressed by Barrett's esophagus and adenocarcinoma compared to normal tissues. Barrett's esophagus length has also been identified as a risk factor for progression to adenocarcinoma, but whether there are intrinsic biological differences between short and long-segment Barrett's esophagus can be explored with microarrays.

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Harvey Young

A Genomic Screen of Autism: Evidence for a Multilocus Etiology

Increased risk of colorectal neoplasia in patients with primary sclerosing cholangitis and ulcerative colitis: A meta-analysis

Accelerated improvement of alcoholic liver disease with enteral nutrition

Guidelines for credentialing and granting privileges for endoscopic ultrasound

Gene Expression Profiling Reveals Stromal Genes Expressed in Common Between Barrett’s Esophagus and Adenocarcinoma

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