Follow-up of a report of a potential linkage for schizophrenia on chromosome 22q12-q13.1: Part 2

Ann E. Pulver; Maria Karayiorgou; Virginia K. Lasseter; Paula Wolyniec; Laura Kasch; Stylianos Antonarakis; David Housman; Haig H. Kazazian; Deborah Meyers; Gerald Nestadt; Jurg Ott; Kung Yee Liang; Malgorzata Lamacz; Marion Thomas; Barton Childs; Scott R. Diehl; Shengbiao Wang; Bernadette Murphy; Cui e. Sun; F. Anthony O'Neill; Li Nie; Pak Sham; John Burke; Betty W. Duke; Fiona Duke; Barbara R. Kipps; Joseph Bray; Wanda Hunt; Rosmarie Shinkwin; Maurin Ni Nuallain; Ying Su; Charles J. MacLean; Dermot Walsh; Kenneth S. Kendler; Michael Gill; Homero Vallada; Rebecca Mant; Philip Asherson; David Collier; Elizabeth Parfitt; Enriquetta Roberts; Shin Nanko; Cathy Walsh; Johanna Daniels; Robin Murray; Peter McGuffin; Mike Owen; Claudine Laurent; Jean Baptiste Dumas; Thierry d'Amato; Maurice Jay; Maria Martinez; Dominique Campion; Jacques Mallet

doi:10.1002/ajmg.1320540109

Follow-up of a report of a potential linkage for schizophrenia on chromosome 22q12-q13.1: Part 2

Ann E. Pulver
, Maria Karayiorgou
, Virginia K. Lasseter
, Paula Wolyniec
, Laura Kasch
, Stylianos Antonarakis
, David Housman
, Haig H. Kazazian
, Deborah Meyers
, Gerald Nestadt
, Jurg Ott
, Kung Yee Liang
, Malgorzata Lamacz
, Marion Thomas
, Barton Childs
, Scott R. Diehl
, Shengbiao Wang
, Bernadette Murphy
, Cui e. Sun
, F. Anthony O'Neill

Li Nie, Pak Sham, John Burke, Betty W. Duke, Fiona Duke, Barbara R. Kipps, Joseph Bray, Wanda Hunt, Rosmarie Shinkwin, Maurin Ni Nuallain, Ying Su, Charles J. MacLean, Dermot Walsh, Kenneth S. Kendler, Michael Gill, Homero Vallada, Rebecca Mant, Philip Asherson, David Collier, Elizabeth Parfitt, Enriquetta Roberts, Shin Nanko, Cathy Walsh, Johanna Daniels, Robin Murray, Peter McGuffin, Mike Owen, Claudine Laurent, Jean Baptiste Dumas, Thierry d'Amato, Maurice Jay, Maria Martinez, Dominique Campion, Jacques Mallet

Research output: Contribution to journal › Article › peer-review

96 Scopus citations

Abstract

A collaboration involving four groups of investigators (Johns Hopkins University/Massachusetts Institute of Technology; Medical College of Virginia/The Health Research Board, Dublin; Institute of Psychiatry, London/University of Wales, Cardiff; Centre National de la Recherche Scientifique, Paris) was organized to confirm results suggestive of a schizophrenia susceptibility locus on chromosome 22 identified by the JHU/MIT group after a random search of the genome. Diagnostic, laboratory, and analytical reliability exercises were conducted among the groups to ensure uniformity of procedures. Data from genotyping of 3 dinucleotide repeat polymorphisms (at the loci D22S268, IL2RB, D22S307) for a combined replication sample of 256 families, each having 2 or more affected individuals with DNA, were analysed using a complex autosomal dominant model. This study provided no evidence for linkage or heterogeneity for the region 22q12-q13 under this model. We conclude that if this region confers susceptibility to schizophrenia, it must be in only a small proportion of families. Collaborative efforts to obtain large samples must continue to play an important role in the genetic search for clues to complex psychiatric disorders such as schizophrenia.

Original language	English (US)
Pages (from-to)	44-50
Number of pages	7
Journal	American journal of medical genetics
Volume	54
Issue number	1
DOIs	https://doi.org/10.1002/ajmg.1320540109
State	Published - 1994
Externally published	Yes

Keywords

collaboration
human chromosome 22
linkage
replication
schizophrenia

ASJC Scopus subject areas

Genetics(clinical)

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10.1002/ajmg.1320540109

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Pulver, A. E., Karayiorgou, M., Lasseter, V. K., Wolyniec, P., Kasch, L., Antonarakis, S., Housman, D., Kazazian, H. H., Meyers, D., Nestadt, G., Ott, J., Liang, K. Y., Lamacz, M., Thomas, M., Childs, B., Diehl, S. R., Wang, S., Murphy, B., Sun, C. E., ... Mallet, J. (1994). Follow-up of a report of a potential linkage for schizophrenia on chromosome 22q12-q13.1: Part 2. American journal of medical genetics, 54(1), 44-50. https://doi.org/10.1002/ajmg.1320540109

Pulver, AE, Karayiorgou, M, Lasseter, VK, Wolyniec, P, Kasch, L, Antonarakis, S, Housman, D, Kazazian, HH, Meyers, D, Nestadt, G, Ott, J, Liang, KY, Lamacz, M, Thomas, M, Childs, B, Diehl, SR, Wang, S, Murphy, B, Sun, CE, O'Neill, FA, Nie, L, Sham, P, Burke, J, Duke, BW, Duke, F, Kipps, BR, Bray, J, Hunt, W, Shinkwin, R, Nuallain, MN, Su, Y, MacLean, CJ, Walsh, D, Kendler, KS, Gill, M, Vallada, H, Mant, R, Asherson, P, Collier, D, Parfitt, E, Roberts, E, Nanko, S, Walsh, C, Daniels, J, Murray, R, McGuffin, P, Owen, M, Laurent, C, Dumas, JB, d'Amato, T, Jay, M, Martinez, M, Campion, D & Mallet, J 1994, 'Follow-up of a report of a potential linkage for schizophrenia on chromosome 22q12-q13.1: Part 2', American journal of medical genetics, vol. 54, no. 1, pp. 44-50. https://doi.org/10.1002/ajmg.1320540109

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title = "Follow-up of a report of a potential linkage for schizophrenia on chromosome 22q12-q13.1: Part 2",

abstract = "A collaboration involving four groups of investigators (Johns Hopkins University/Massachusetts Institute of Technology; Medical College of Virginia/The Health Research Board, Dublin; Institute of Psychiatry, London/University of Wales, Cardiff; Centre National de la Recherche Scientifique, Paris) was organized to confirm results suggestive of a schizophrenia susceptibility locus on chromosome 22 identified by the JHU/MIT group after a random search of the genome. Diagnostic, laboratory, and analytical reliability exercises were conducted among the groups to ensure uniformity of procedures. Data from genotyping of 3 dinucleotide repeat polymorphisms (at the loci D22S268, IL2RB, D22S307) for a combined replication sample of 256 families, each having 2 or more affected individuals with DNA, were analysed using a complex autosomal dominant model. This study provided no evidence for linkage or heterogeneity for the region 22q12-q13 under this model. We conclude that if this region confers susceptibility to schizophrenia, it must be in only a small proportion of families. Collaborative efforts to obtain large samples must continue to play an important role in the genetic search for clues to complex psychiatric disorders such as schizophrenia.",

keywords = "collaboration, human chromosome 22, linkage, replication, schizophrenia",

author = "Pulver, \{Ann E.\} and Maria Karayiorgou and Lasseter, \{Virginia K.\} and Paula Wolyniec and Laura Kasch and Stylianos Antonarakis and David Housman and Kazazian, \{Haig H.\} and Deborah Meyers and Gerald Nestadt and Jurg Ott and Liang, \{Kung Yee\} and Malgorzata Lamacz and Marion Thomas and Barton Childs and Diehl, \{Scott R.\} and Shengbiao Wang and Bernadette Murphy and Sun, \{Cui e.\} and O'Neill, \{F. Anthony\} and Li Nie and Pak Sham and John Burke and Duke, \{Betty W.\} and Fiona Duke and Kipps, \{Barbara R.\} and Joseph Bray and Wanda Hunt and Rosmarie Shinkwin and Nuallain, \{Maurin Ni\} and Ying Su and MacLean, \{Charles J.\} and Dermot Walsh and Kendler, \{Kenneth S.\} and Michael Gill and Homero Vallada and Rebecca Mant and Philip Asherson and David Collier and Elizabeth Parfitt and Enriquetta Roberts and Shin Nanko and Cathy Walsh and Johanna Daniels and Robin Murray and Peter McGuffin and Mike Owen and Claudine Laurent and Dumas, \{Jean Baptiste\} and Thierry d'Amato and Maurice Jay and Maria Martinez and Dominique Campion and Jacques Mallet",

year = "1994",

doi = "10.1002/ajmg.1320540109",

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T1 - Follow-up of a report of a potential linkage for schizophrenia on chromosome 22q12-q13.1

T2 - Part 2

AU - Pulver, Ann E.

AU - Karayiorgou, Maria

AU - Lasseter, Virginia K.

AU - Wolyniec, Paula

AU - Kasch, Laura

AU - Antonarakis, Stylianos

AU - Housman, David

AU - Kazazian, Haig H.

AU - Meyers, Deborah

AU - Nestadt, Gerald

AU - Ott, Jurg

AU - Liang, Kung Yee

AU - Lamacz, Malgorzata

AU - Thomas, Marion

AU - Childs, Barton

AU - Diehl, Scott R.

AU - Wang, Shengbiao

AU - Murphy, Bernadette

AU - Sun, Cui e.

AU - O'Neill, F. Anthony

AU - Nie, Li

AU - Sham, Pak

AU - Burke, John

AU - Duke, Betty W.

AU - Duke, Fiona

AU - Kipps, Barbara R.

AU - Bray, Joseph

AU - Hunt, Wanda

AU - Shinkwin, Rosmarie

AU - Nuallain, Maurin Ni

AU - Su, Ying

AU - MacLean, Charles J.

AU - Walsh, Dermot

AU - Kendler, Kenneth S.

AU - Gill, Michael

AU - Vallada, Homero

AU - Mant, Rebecca

AU - Asherson, Philip

AU - Collier, David

AU - Parfitt, Elizabeth

AU - Roberts, Enriquetta

AU - Nanko, Shin

AU - Walsh, Cathy

AU - Daniels, Johanna

AU - Murray, Robin

AU - McGuffin, Peter

AU - Owen, Mike

AU - Laurent, Claudine

AU - Dumas, Jean Baptiste

AU - d'Amato, Thierry

AU - Jay, Maurice

AU - Martinez, Maria

AU - Campion, Dominique

AU - Mallet, Jacques

PY - 1994

Y1 - 1994

N2 - A collaboration involving four groups of investigators (Johns Hopkins University/Massachusetts Institute of Technology; Medical College of Virginia/The Health Research Board, Dublin; Institute of Psychiatry, London/University of Wales, Cardiff; Centre National de la Recherche Scientifique, Paris) was organized to confirm results suggestive of a schizophrenia susceptibility locus on chromosome 22 identified by the JHU/MIT group after a random search of the genome. Diagnostic, laboratory, and analytical reliability exercises were conducted among the groups to ensure uniformity of procedures. Data from genotyping of 3 dinucleotide repeat polymorphisms (at the loci D22S268, IL2RB, D22S307) for a combined replication sample of 256 families, each having 2 or more affected individuals with DNA, were analysed using a complex autosomal dominant model. This study provided no evidence for linkage or heterogeneity for the region 22q12-q13 under this model. We conclude that if this region confers susceptibility to schizophrenia, it must be in only a small proportion of families. Collaborative efforts to obtain large samples must continue to play an important role in the genetic search for clues to complex psychiatric disorders such as schizophrenia.

AB - A collaboration involving four groups of investigators (Johns Hopkins University/Massachusetts Institute of Technology; Medical College of Virginia/The Health Research Board, Dublin; Institute of Psychiatry, London/University of Wales, Cardiff; Centre National de la Recherche Scientifique, Paris) was organized to confirm results suggestive of a schizophrenia susceptibility locus on chromosome 22 identified by the JHU/MIT group after a random search of the genome. Diagnostic, laboratory, and analytical reliability exercises were conducted among the groups to ensure uniformity of procedures. Data from genotyping of 3 dinucleotide repeat polymorphisms (at the loci D22S268, IL2RB, D22S307) for a combined replication sample of 256 families, each having 2 or more affected individuals with DNA, were analysed using a complex autosomal dominant model. This study provided no evidence for linkage or heterogeneity for the region 22q12-q13 under this model. We conclude that if this region confers susceptibility to schizophrenia, it must be in only a small proportion of families. Collaborative efforts to obtain large samples must continue to play an important role in the genetic search for clues to complex psychiatric disorders such as schizophrenia.

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KW - linkage

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Follow-up of a report of a potential linkage for schizophrenia on chromosome 22q12-q13.1: Part 2

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

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