Update on the Search for DNA Markers Linked to Manic-depressive Illness in the Old Order Amish

Overview

Journal J Psychiatr Res

Specialty Psychiatry

Date 1992 Oct 1

PMID 1362775

Citations 3

Authors

E I Ginns

J A Egeland

C R Allen

D L Pauls

K Falls

T P Keith

S M Paul

Affiliations

Soon will be listed here.

Abstract

In this report we describe our efforts to identify a gene involved in bipolar illness using a large, multigenerational Old Order Amish pedigree with many affected individuals. The original collection of cell lines from Amish pedigree 110 has been extended to include 169 individuals. We have used over 250 markers spaced at approximately 20 centiMorgans that detect restriction length fragment polymorphisms, but no LOD scores greater than 3 have been obtained from pairwise linkage analyses. We are expanding our collection of cell lines from both normal and affected family members and updating our diagnostic data as we continue our systematic screening of the genome for a gene involved in bipolar illness.

Citing Articles

Post-genomic era and gene discovery for psychiatric diseases: there is a new art of the trade? The example of the HUMTH01 microsatellite in the Tyrosine Hydroxylase gene.

Meloni R, Faucon Biguet N, Mallet J Mol Neurobiol. 2002; 26(2-3):389-403.

PMID: 12428766 DOI: 10.1385/MN:26:2-3:389.

Writing Amish culture into genes: biological reductionism in a study of manic depression.

Floersch J, Longhofer J, Latta K Cult Med Psychiatry. 1997; 21(2):137-59.

PMID: 9248676 DOI: 10.1023/a:1005352727300.

Linkage analyses of chromosome 18 markers do not identify a major susceptibility locus for bipolar affective disorder in the Old Order Amish.

Pauls D, Ott J, Paul S, Allen C, Fann C, Carulli J Am J Hum Genet. 1995; 57(3):636-43.

PMID: 7668292 PMC: 1801276.