Genome-wide linkage analysis and evidence of gene-by-gene interactions in a sample of 362 multiplex Parkinson disease families

Nathan Pankratz; William C. Nichols; Sean K. Uniacke; Cheryl Halter; Jill Murrell; Alice Rudolph; Clifford W. Shults; P. Michael Conneally; Tatiana Foroud; Daniel Truong; Mayank Pathak; An Tran; Robert Rodnitzky; Judith Dobson; William Koller; William Weiner; Kelly Lyons; Roger Kurlan; Debra Berry; John Bertoni; Carolyn Peterson; Wayne Martin; Marguerite Wieler; Paul Tuite; Robyn Schacherer; Karen Marder; Juliette Harris; Joseph Jankovic; Christine Hunter; Anthony Lang; Galit Kleimer-Fisman; Anette Nieves; Julie So; Stewart Factor; Sharon Evans; Bala Manyam; Brian Wulbrecht; Francis Walker; Victoria Hunt; Mark F. Gordon; Joanna Hamman; Un Jang Kang; Joan Young; Karen Blindauer; Jeannine Petit; Jayaraman Rao; Maureen Cook; Mark Stacy; Kelli Williamson; Kapil Dev Sethi; Karyn Boyar; Maureen Leehey; Theresa Derian; Paul Gordon; Joan Werner; Brad Racette; Laura Good; David Simon; Lisa Scollins; Donna Schwieterman; Richard Dewey; Melinda Meacham; James Sutton; Brad Hutchinson; Mandar Jog; Cheryl Horn; Kapil Sethi; Joan Carpenter; Paul Atchison; Susan Rolli; Lewis Sudarsky; Claire Corwin; Miodrag Velickovic; Sabrina Phipps; Tanya Simuni; Annette Kaczmarek; Neal Hermanowicz; Shari Niswonger; Andrew Feigin; Barbara Shannon; Vincent Calabrese; Peggy Roberge; Hunter Homes; Lisa Shulman; Kelly Dustin; Todd Ajax; Janet Mannetter; G. David Podskalny; Lisa Giffin; Ryan Uitti; Margaret Foster Turk

doi:10.1093/hmg/ddg270

Genome-wide linkage analysis and evidence of gene-by-gene interactions in a sample of 362 multiplex Parkinson disease families

Nathan Pankratz, William C. Nichols, Sean K. Uniacke, Cheryl Halter, Jill Murrell, Alice Rudolph, Clifford W. Shults, P. Michael Conneally, Tatiana Foroud, Daniel Truong, Mayank Pathak, An Tran, Robert Rodnitzky, Judith Dobson, William Koller, William Weiner, Kelly Lyons, Roger Kurlan, Debra Berry, John BertoniCarolyn Peterson, Wayne Martin, Marguerite Wieler, Paul Tuite, Robyn Schacherer, Karen Marder, Juliette Harris, Joseph Jankovic, Christine Hunter, Anthony Lang, Galit Kleimer-Fisman, Anette Nieves, Julie So, Stewart Factor, Sharon Evans, Bala Manyam, Brian Wulbrecht, Francis Walker, Victoria Hunt, Mark F. Gordon, Joanna Hamman, Un Jang Kang, Joan Young, Karen Blindauer, Jeannine Petit, Jayaraman Rao, Maureen Cook, Mark Stacy, Kelli Williamson, Kapil Dev Sethi, Karyn Boyar, Maureen Leehey, Theresa Derian, Paul Gordon, Joan Werner, Brad Racette, Laura Good, David Simon, Lisa Scollins, Donna Schwieterman, Richard Dewey, Melinda Meacham, James Sutton, Brad Hutchinson, Mandar Jog, Cheryl Horn, Kapil Sethi, Joan Carpenter, Paul Atchison, Susan Rolli, Lewis Sudarsky, Claire Corwin, Miodrag Velickovic, Sabrina Phipps, Tanya Simuni, Annette Kaczmarek, Neal Hermanowicz, Shari Niswonger, Andrew Feigin, Barbara Shannon, Vincent Calabrese, Peggy Roberge, Hunter Homes, Lisa Shulman, Kelly Dustin, Todd Ajax, Janet Mannetter, G. David Podskalny, Lisa Giffin, Ryan Uitti, Margaret Foster Turk

Neurology

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

130 Scopus citations

Abstract

Parkinson disease (PD) is the second most common neurodegenerative disorder. We studied 754 affected individuals, comprising 425 sibling pairs, to identify PD susceptibility genes. Screening of the parkin gene was performed in a subset of the sample having earlier age of PD onset or a positive LOD score with a marker in the parkin gene. All subjects were evaluated using a rigorous neurological assessment. Two diagnostic models were considered for genome-wide, non-parametric linkage analyses. Model I included only those individuals with a more stringent diagnosis of verified PD (216 sibling pairs) and resulted in a maximum LOD score of 3.4 on chromosome 2. Model II included all affected individuals (425 sibling pairs) and yielded a LOD score of 3.1 on the X chromosome. Our large sample was then employed to test for gene-by-gene (epistatic) interactions. A genome screen using the 23 families with PD patients having a mutation in only one allele of the parkin gene detected evidence of linkage to chromosome 10 (LOD = 2.3). The 85 families with a very strong family history of PD were employed in a genome screen and, in addition to strong evidence of linkage to chromosome 2 (LOD = 4.9), also produced a LOD of 2.4 on chromosome 14. A genome screen performed in the 277 families without a strong family history of PD detected linkage to chromosomes 10 (LOD = 2.4) and X (LOD = 3.2). These findings demonstrate consistent evidence of linkage to chromosomes 2 and X and also support the hypothesis that gene-by-gene interactions are important in PD susceptibility.

Original language	English (US)
Pages (from-to)	2599-2608
Number of pages	10
Journal	Human Molecular Genetics
Volume	12
Issue number	20
DOIs	https://doi.org/10.1093/hmg/ddg270
State	Published - Oct 15 2003

ASJC Scopus subject areas

Molecular Biology
Genetics
Genetics(clinical)

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10.1093/hmg/ddg270

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Pankratz, N., Nichols, W. C., Uniacke, S. K., Halter, C., Murrell, J., Rudolph, A., Shults, C. W., Conneally, P. M., Foroud, T., Truong, D., Pathak, M., Tran, A., Rodnitzky, R., Dobson, J., Koller, W., Weiner, W., Lyons, K., Kurlan, R., Berry, D., ... Turk, M. F. (2003). Genome-wide linkage analysis and evidence of gene-by-gene interactions in a sample of 362 multiplex Parkinson disease families. Human Molecular Genetics, 12(20), 2599-2608. https://doi.org/10.1093/hmg/ddg270

Pankratz, N, Nichols, WC, Uniacke, SK, Halter, C, Murrell, J, Rudolph, A, Shults, CW, Conneally, PM, Foroud, T, Truong, D, Pathak, M, Tran, A, Rodnitzky, R, Dobson, J, Koller, W, Weiner, W, Lyons, K, Kurlan, R, Berry, D, Bertoni, J, Peterson, C, Martin, W, Wieler, M, Tuite, P, Schacherer, R, Marder, K, Harris, J, Jankovic, J, Hunter, C, Lang, A, Kleimer-Fisman, G, Nieves, A, So, J, Factor, S, Evans, S, Manyam, B, Wulbrecht, B, Walker, F, Hunt, V, Gordon, MF, Hamman, J, Kang, UJ, Young, J, Blindauer, K, Petit, J, Rao, J, Cook, M, Stacy, M, Williamson, K, Sethi, KD, Boyar, K, Leehey, M, Derian, T, Gordon, P, Werner, J, Racette, B, Good, L, Simon, D, Scollins, L, Schwieterman, D, Dewey, R, Meacham, M, Sutton, J, Hutchinson, B, Jog, M, Horn, C, Sethi, K, Carpenter, J, Atchison, P, Rolli, S, Sudarsky, L, Corwin, C, Velickovic, M, Phipps, S, Simuni, T, Kaczmarek, A, Hermanowicz, N, Niswonger, S, Feigin, A, Shannon, B, Calabrese, V, Roberge, P, Homes, H, Shulman, L, Dustin, K, Ajax, T, Mannetter, J, Podskalny, GD, Giffin, L, Uitti, R & Turk, MF 2003, 'Genome-wide linkage analysis and evidence of gene-by-gene interactions in a sample of 362 multiplex Parkinson disease families', Human Molecular Genetics, vol. 12, no. 20, pp. 2599-2608. https://doi.org/10.1093/hmg/ddg270

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abstract = "Parkinson disease (PD) is the second most common neurodegenerative disorder. We studied 754 affected individuals, comprising 425 sibling pairs, to identify PD susceptibility genes. Screening of the parkin gene was performed in a subset of the sample having earlier age of PD onset or a positive LOD score with a marker in the parkin gene. All subjects were evaluated using a rigorous neurological assessment. Two diagnostic models were considered for genome-wide, non-parametric linkage analyses. Model I included only those individuals with a more stringent diagnosis of verified PD (216 sibling pairs) and resulted in a maximum LOD score of 3.4 on chromosome 2. Model II included all affected individuals (425 sibling pairs) and yielded a LOD score of 3.1 on the X chromosome. Our large sample was then employed to test for gene-by-gene (epistatic) interactions. A genome screen using the 23 families with PD patients having a mutation in only one allele of the parkin gene detected evidence of linkage to chromosome 10 (LOD = 2.3). The 85 families with a very strong family history of PD were employed in a genome screen and, in addition to strong evidence of linkage to chromosome 2 (LOD = 4.9), also produced a LOD of 2.4 on chromosome 14. A genome screen performed in the 277 families without a strong family history of PD detected linkage to chromosomes 10 (LOD = 2.4) and X (LOD = 3.2). These findings demonstrate consistent evidence of linkage to chromosomes 2 and X and also support the hypothesis that gene-by-gene interactions are important in PD susceptibility.",

author = "Nathan Pankratz and Nichols, {William C.} and Uniacke, {Sean K.} and Cheryl Halter and Jill Murrell and Alice Rudolph and Shults, {Clifford W.} and Conneally, {P. Michael} and Tatiana Foroud and Daniel Truong and Mayank Pathak and An Tran and Robert Rodnitzky and Judith Dobson and William Koller and William Weiner and Kelly Lyons and Roger Kurlan and Debra Berry and John Bertoni and Carolyn Peterson and Wayne Martin and Marguerite Wieler and Paul Tuite and Robyn Schacherer and Karen Marder and Juliette Harris and Joseph Jankovic and Christine Hunter and Anthony Lang and Galit Kleimer-Fisman and Anette Nieves and Julie So and Stewart Factor and Sharon Evans and Bala Manyam and Brian Wulbrecht and Francis Walker and Victoria Hunt and Gordon, {Mark F.} and Joanna Hamman and Kang, {Un Jang} and Joan Young and Karen Blindauer and Jeannine Petit and Jayaraman Rao and Maureen Cook and Mark Stacy and Kelli Williamson and Sethi, {Kapil Dev} and Karyn Boyar and Maureen Leehey and Theresa Derian and Paul Gordon and Joan Werner and Brad Racette and Laura Good and David Simon and Lisa Scollins and Donna Schwieterman and Richard Dewey and Melinda Meacham and James Sutton and Brad Hutchinson and Mandar Jog and Cheryl Horn and Kapil Sethi and Joan Carpenter and Paul Atchison and Susan Rolli and Lewis Sudarsky and Claire Corwin and Miodrag Velickovic and Sabrina Phipps and Tanya Simuni and Annette Kaczmarek and Neal Hermanowicz and Shari Niswonger and Andrew Feigin and Barbara Shannon and Vincent Calabrese and Peggy Roberge and Hunter Homes and Lisa Shulman and Kelly Dustin and Todd Ajax and Janet Mannetter and Podskalny, {G. David} and Lisa Giffin and Ryan Uitti and Turk, {Margaret Foster}",

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T1 - Genome-wide linkage analysis and evidence of gene-by-gene interactions in a sample of 362 multiplex Parkinson disease families

AU - Pankratz, Nathan

AU - Nichols, William C.

AU - Uniacke, Sean K.

AU - Halter, Cheryl

AU - Murrell, Jill

AU - Rudolph, Alice

AU - Shults, Clifford W.

AU - Conneally, P. Michael

AU - Foroud, Tatiana

AU - Truong, Daniel

AU - Pathak, Mayank

AU - Tran, An

AU - Rodnitzky, Robert

AU - Dobson, Judith

AU - Koller, William

AU - Weiner, William

AU - Lyons, Kelly

AU - Kurlan, Roger

AU - Berry, Debra

AU - Bertoni, John

AU - Peterson, Carolyn

AU - Martin, Wayne

AU - Wieler, Marguerite

AU - Tuite, Paul

AU - Schacherer, Robyn

AU - Marder, Karen

AU - Harris, Juliette

AU - Jankovic, Joseph

AU - Hunter, Christine

AU - Lang, Anthony

AU - Kleimer-Fisman, Galit

AU - Nieves, Anette

AU - So, Julie

AU - Factor, Stewart

AU - Evans, Sharon

AU - Manyam, Bala

AU - Wulbrecht, Brian

AU - Walker, Francis

AU - Hunt, Victoria

AU - Gordon, Mark F.

AU - Hamman, Joanna

AU - Kang, Un Jang

AU - Young, Joan

AU - Blindauer, Karen

AU - Petit, Jeannine

AU - Rao, Jayaraman

AU - Cook, Maureen

AU - Stacy, Mark

AU - Williamson, Kelli

AU - Sethi, Kapil Dev

AU - Boyar, Karyn

AU - Leehey, Maureen

AU - Derian, Theresa

AU - Gordon, Paul

AU - Werner, Joan

AU - Racette, Brad

AU - Good, Laura

AU - Simon, David

AU - Scollins, Lisa

AU - Schwieterman, Donna

AU - Dewey, Richard

AU - Meacham, Melinda

AU - Sutton, James

AU - Hutchinson, Brad

AU - Jog, Mandar

AU - Horn, Cheryl

AU - Sethi, Kapil

AU - Carpenter, Joan

AU - Atchison, Paul

AU - Rolli, Susan

AU - Sudarsky, Lewis

AU - Corwin, Claire

AU - Velickovic, Miodrag

AU - Phipps, Sabrina

AU - Simuni, Tanya

AU - Kaczmarek, Annette

AU - Hermanowicz, Neal

AU - Niswonger, Shari

AU - Feigin, Andrew

AU - Shannon, Barbara

AU - Calabrese, Vincent

AU - Roberge, Peggy

AU - Homes, Hunter

AU - Shulman, Lisa

AU - Dustin, Kelly

AU - Ajax, Todd

AU - Mannetter, Janet

AU - Podskalny, G. David

AU - Giffin, Lisa

AU - Uitti, Ryan

AU - Turk, Margaret Foster

PY - 2003/10/15

Y1 - 2003/10/15

N2 - Parkinson disease (PD) is the second most common neurodegenerative disorder. We studied 754 affected individuals, comprising 425 sibling pairs, to identify PD susceptibility genes. Screening of the parkin gene was performed in a subset of the sample having earlier age of PD onset or a positive LOD score with a marker in the parkin gene. All subjects were evaluated using a rigorous neurological assessment. Two diagnostic models were considered for genome-wide, non-parametric linkage analyses. Model I included only those individuals with a more stringent diagnosis of verified PD (216 sibling pairs) and resulted in a maximum LOD score of 3.4 on chromosome 2. Model II included all affected individuals (425 sibling pairs) and yielded a LOD score of 3.1 on the X chromosome. Our large sample was then employed to test for gene-by-gene (epistatic) interactions. A genome screen using the 23 families with PD patients having a mutation in only one allele of the parkin gene detected evidence of linkage to chromosome 10 (LOD = 2.3). The 85 families with a very strong family history of PD were employed in a genome screen and, in addition to strong evidence of linkage to chromosome 2 (LOD = 4.9), also produced a LOD of 2.4 on chromosome 14. A genome screen performed in the 277 families without a strong family history of PD detected linkage to chromosomes 10 (LOD = 2.4) and X (LOD = 3.2). These findings demonstrate consistent evidence of linkage to chromosomes 2 and X and also support the hypothesis that gene-by-gene interactions are important in PD susceptibility.

AB - Parkinson disease (PD) is the second most common neurodegenerative disorder. We studied 754 affected individuals, comprising 425 sibling pairs, to identify PD susceptibility genes. Screening of the parkin gene was performed in a subset of the sample having earlier age of PD onset or a positive LOD score with a marker in the parkin gene. All subjects were evaluated using a rigorous neurological assessment. Two diagnostic models were considered for genome-wide, non-parametric linkage analyses. Model I included only those individuals with a more stringent diagnosis of verified PD (216 sibling pairs) and resulted in a maximum LOD score of 3.4 on chromosome 2. Model II included all affected individuals (425 sibling pairs) and yielded a LOD score of 3.1 on the X chromosome. Our large sample was then employed to test for gene-by-gene (epistatic) interactions. A genome screen using the 23 families with PD patients having a mutation in only one allele of the parkin gene detected evidence of linkage to chromosome 10 (LOD = 2.3). The 85 families with a very strong family history of PD were employed in a genome screen and, in addition to strong evidence of linkage to chromosome 2 (LOD = 4.9), also produced a LOD of 2.4 on chromosome 14. A genome screen performed in the 277 families without a strong family history of PD detected linkage to chromosomes 10 (LOD = 2.4) and X (LOD = 3.2). These findings demonstrate consistent evidence of linkage to chromosomes 2 and X and also support the hypothesis that gene-by-gene interactions are important in PD susceptibility.

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Genome-wide linkage analysis and evidence of gene-by-gene interactions in a sample of 362 multiplex Parkinson disease families

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