Exome sequence analysis and follow up genotyping implicates rare ULK1 variants to be involved in susceptibility to schizophrenia

Summary Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater understanding of the altered underlying neurobiological mechanisms. The aim of this study was to identify likely aetiological variants in su...

Full description

Saved in:

Bibliographic Details
Published in	Annals of human genetics Vol. 82; no. 2; pp. 88 - 92
Main Authors	Al Eissa, Mariam M., Fiorentino, Alessia, Sharp, Sally I., O'Brien, Niamh L., Wolfe, Kate, Giaroli, Giovanni, Curtis, David, Bass, Nicholas J., McQuillin, Andrew
Format	Journal Article
Language	English
Published	England Wiley Subscription Services, Inc 01.03.2018 John Wiley and Sons Inc
Subjects	association Autophagy Autophagy-Related Protein-1 Homolog - genetics burden analysis Case-Control Studies Exome Exome Sequencing Genotype Genotyping Humans Intracellular Signaling Peptides and Proteins - genetics Introns Kinases Mental disorders Mutation, Missense olanzapine Original Phagocytosis Schizophrenia Schizophrenia - genetics Signal transduction Sweden TOR protein Sweden olanzapine association burden analysis
Online Access	Get full text

Cover

Loading…

Abstract	Summary Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater understanding of the altered underlying neurobiological mechanisms. The aim of this study was to identify likely aetiological variants in subjects affected with SCZ. Exome sequence data from a SCZ cas–control sample from Sweden was analysed for likely aetiological variants using a weighted burden test. Suggestive evidence implicated the UNC‐51‐like kinase (ULK1) gene, and it was observed that four rare variants that were more common in the Swedish SCZ cases were also more common in UK10K SCZ cases, as compared to obesity cases. These three missense variants and one intronic variant were genotyped in the University College London cohort of 1304 SCZ cases and 1348 ethnically matched controls. All four variants were more common in the SCZ cases than controls and combining them produced a result significant at P = 0.02. The results presented here demonstrate the importance of following up exome sequencing studies using additional datasets. The roles of ULK1 in autophagy and mTOR signalling strengthen the case that these pathways may be important in the pathophysiology of SCZ. The findings reported here await independent replication.
AbstractList	Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater understanding of the altered underlying neurobiological mechanisms. The aim of this study was to identify likely aetiological variants in subjects affected with SCZ. Exome sequence data from a SCZ cas–control sample from Sweden was analysed for likely aetiological variants using a weighted burden test. Suggestive evidence implicated the UNC‐51‐like kinase ( ULK1 ) gene, and it was observed that four rare variants that were more common in the Swedish SCZ cases were also more common in UK10K SCZ cases, as compared to obesity cases. These three missense variants and one intronic variant were genotyped in the University College London cohort of 1304 SCZ cases and 1348 ethnically matched controls. All four variants were more common in the SCZ cases than controls and combining them produced a result significant at P = 0.02. The results presented here demonstrate the importance of following up exome sequencing studies using additional datasets. The roles of ULK1 in autophagy and mTOR signalling strengthen the case that these pathways may be important in the pathophysiology of SCZ. The findings reported here await independent replication. Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater understanding of the altered underlying neurobiological mechanisms. The aim of this study was to identify likely aetiological variants in subjects affected with SCZ. Exome sequence data from a SCZ cas-control sample from Sweden was analysed for likely aetiological variants using a weighted burden test. Suggestive evidence implicated the UNC-51-like kinase (ULK1) gene, and it was observed that four rare variants that were more common in the Swedish SCZ cases were also more common in UK10K SCZ cases, as compared to obesity cases. These three missense variants and one intronic variant were genotyped in the University College London cohort of 1304 SCZ cases and 1348 ethnically matched controls. All four variants were more common in the SCZ cases than controls and combining them produced a result significant at P = 0.02. The results presented here demonstrate the importance of following up exome sequencing studies using additional datasets. The roles of ULK1 in autophagy and mTOR signalling strengthen the case that these pathways may be important in the pathophysiology of SCZ. The findings reported here await independent replication. Summary Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater understanding of the altered underlying neurobiological mechanisms. The aim of this study was to identify likely aetiological variants in subjects affected with SCZ. Exome sequence data from a SCZ cas–control sample from Sweden was analysed for likely aetiological variants using a weighted burden test. Suggestive evidence implicated the UNC‐51‐like kinase (ULK1) gene, and it was observed that four rare variants that were more common in the Swedish SCZ cases were also more common in UK10K SCZ cases, as compared to obesity cases. These three missense variants and one intronic variant were genotyped in the University College London cohort of 1304 SCZ cases and 1348 ethnically matched controls. All four variants were more common in the SCZ cases than controls and combining them produced a result significant at P = 0.02. The results presented here demonstrate the importance of following up exome sequencing studies using additional datasets. The roles of ULK1 in autophagy and mTOR signalling strengthen the case that these pathways may be important in the pathophysiology of SCZ. The findings reported here await independent replication. Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater understanding of the altered underlying neurobiological mechanisms. The aim of this study was to identify likely aetiological variants in subjects affected with SCZ. Exome sequence data from a SCZ cas-control sample from Sweden was analysed for likely aetiological variants using a weighted burden test. Suggestive evidence implicated the UNC-51-like kinase (ULK1) gene, and it was observed that four rare variants that were more common in the Swedish SCZ cases were also more common in UK10K SCZ cases, as compared to obesity cases. These three missense variants and one intronic variant were genotyped in the University College London cohort of 1304 SCZ cases and 1348 ethnically matched controls. All four variants were more common in the SCZ cases than controls and combining them produced a result significant at P = 0.02. The results presented here demonstrate the importance of following up exome sequencing studies using additional datasets. The roles of ULK1 in autophagy and mTOR signalling strengthen the case that these pathways may be important in the pathophysiology of SCZ. The findings reported here await independent replication.Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater understanding of the altered underlying neurobiological mechanisms. The aim of this study was to identify likely aetiological variants in subjects affected with SCZ. Exome sequence data from a SCZ cas-control sample from Sweden was analysed for likely aetiological variants using a weighted burden test. Suggestive evidence implicated the UNC-51-like kinase (ULK1) gene, and it was observed that four rare variants that were more common in the Swedish SCZ cases were also more common in UK10K SCZ cases, as compared to obesity cases. These three missense variants and one intronic variant were genotyped in the University College London cohort of 1304 SCZ cases and 1348 ethnically matched controls. All four variants were more common in the SCZ cases than controls and combining them produced a result significant at P = 0.02. The results presented here demonstrate the importance of following up exome sequencing studies using additional datasets. The roles of ULK1 in autophagy and mTOR signalling strengthen the case that these pathways may be important in the pathophysiology of SCZ. The findings reported here await independent replication.
Author	O'Brien, Niamh L. Giaroli, Giovanni Fiorentino, Alessia Sharp, Sally I. Bass, Nicholas J. Wolfe, Kate Al Eissa, Mariam M. McQuillin, Andrew Curtis, David
AuthorAffiliation	2 Current address: Institute of Opthalmology University College London London UK 1 Molecular Psychiatry Laboratory, Division of Psychiatry University College London London UK 3 University College London Genetics Institute University College London London UK
AuthorAffiliation_xml	– name: 3 University College London Genetics Institute University College London London UK – name: 1 Molecular Psychiatry Laboratory, Division of Psychiatry University College London London UK – name: 2 Current address: Institute of Opthalmology University College London London UK
Author_xml	– sequence: 1 givenname: Mariam M. surname: Al Eissa fullname: Al Eissa, Mariam M. organization: University College London – sequence: 2 givenname: Alessia surname: Fiorentino fullname: Fiorentino, Alessia organization: University College London – sequence: 3 givenname: Sally I. surname: Sharp fullname: Sharp, Sally I. organization: University College London – sequence: 4 givenname: Niamh L. surname: O'Brien fullname: O'Brien, Niamh L. organization: University College London – sequence: 5 givenname: Kate surname: Wolfe fullname: Wolfe, Kate organization: University College London – sequence: 6 givenname: Giovanni surname: Giaroli fullname: Giaroli, Giovanni organization: University College London – sequence: 7 givenname: David orcidid: 0000-0002-4089-9183 surname: Curtis fullname: Curtis, David organization: University College London – sequence: 8 givenname: Nicholas J. orcidid: 0000-0002-4481-778X surname: Bass fullname: Bass, Nicholas J. organization: University College London – sequence: 9 givenname: Andrew orcidid: 0000-0003-1567-2240 surname: McQuillin fullname: McQuillin, Andrew email: a.mcquillin@ucl.ac.uk organization: University College London
BackLink	https://www.ncbi.nlm.nih.gov/pubmed/29148569$$D View this record in MEDLINE/PubMed
BookMark	eNp9kU1v1DAQhi1URLcLB_4AssQFDmntxM7HBamqSotYiQs9W3Yy2XXl2MF2tg0nfjoOWyqoBHOZkf3Mq5l5T9CRdRYQek3JKU1xJnfbU5rnefkMrSgrm4zWpDlCK0JIkbGakGN0EsItITSvWfECHecNZTUvmxX6cXnvBsABvk1gW8DSSjMHHVLR4d4Z4-7wNOItWBfnUdst1sNodCsjBOylB3yz-UzxXnotbQw4OqwAa7t3Zg9dKnCYQgtj1EobHecFCO1Of3fjzoPV8iV63ksT4NVDXqObj5dfL66zzZerTxfnm6xlrCgzpYhSjao4k51SfcVUSTnvasVkXnU954wrBmVHaHpqihpakFXbMFZB3TPWF2v04aA7TmqArgUbvTRi9HqQfhZOavH3j9U7sXV7wWtaUE6TwLsHAe_SsUIUg06bGSMtuCkI2pRlzuiCr9HbJ-itm3y67EI1rGAVLxfqzZ8TPY7y25wEvD8ArXcheOgfEUrEYrxIxotfxif27Anb6iijdssy2vyv404bmP8tLc6vrw4dPwGwlcHJ
CitedBy_id	crossref_primary_10_1016_j_gene_2022_146772 crossref_primary_10_3390_ijms19082226 crossref_primary_10_3390_cells10030694 crossref_primary_10_1016_j_apsb_2022_06_004 crossref_primary_10_1038_s41380_021_01135_9 crossref_primary_10_1002_mgg3_1561 crossref_primary_10_1097_MD_0000000000028745 crossref_primary_10_1080_15548627_2022_2039994 crossref_primary_10_1016_j_tins_2020_07_003 crossref_primary_10_1016_j_schres_2018_03_001 crossref_primary_10_1002_ajmg_b_32722 crossref_primary_10_1016_j_schres_2022_07_016 crossref_primary_10_3389_fncel_2020_554548 crossref_primary_10_1016_j_neuron_2022_01_017 crossref_primary_10_1016_j_coph_2021_07_013 crossref_primary_10_1111_jnc_16204
Cites_doi	10.1124/jpet.113.207621 10.1111/jnc.12622 10.1038/ncb2152 10.1038/nature19057 10.1097/YPG.0000000000000050 10.1002/(SICI)1096-8628(200021)97:1<12::AID-AJMG3>3.0.CO;2-U 10.1016/j.schres.2013.02.006 10.1093/nar/gks539 10.1001/archgenpsychiatry.2011.12 10.1038/nature11632 10.1038/nature12975 10.1038/nmeth0410-248 10.1038/nmeth.2890 10.1016/j.molcel.2015.05.031 10.1038/mp.2013.174 10.1001/archpsyc.60.5.497 10.1038/nn.4402 10.1017/CBO9781139025997 10.1016/j.conb.2014.12.001 10.1111/ahg.12109 10.1111/bdi.12203 10.1111/ahg.12135
ContentType	Journal Article
Copyright	2017 The Authors. published by University College London (UCL) and John Wiley & Sons Ltd. 2017 The Authors. Annals of Human Genetics published by University College London (UCL) and John Wiley & Sons Ltd. 2017. This article is published under http://creativecommons.org/licenses/by/4.0/ (the “License”). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
Copyright_xml	– notice: 2017 The Authors. published by University College London (UCL) and John Wiley & Sons Ltd. – notice: 2017 The Authors. Annals of Human Genetics published by University College London (UCL) and John Wiley & Sons Ltd. – notice: 2017. This article is published under http://creativecommons.org/licenses/by/4.0/ (the “License”). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
DBID	24P AAYXX CITATION CGR CUY CVF ECM EIF NPM 8FD FR3 K9. P64 RC3 7X8 5PM
DOI	10.1111/ahg.12226
DatabaseName	Wiley Online Library Open Access CrossRef Medline MEDLINE MEDLINE (Ovid) MEDLINE MEDLINE PubMed Technology Research Database Engineering Research Database ProQuest Health & Medical Complete (Alumni) Biotechnology and BioEngineering Abstracts Genetics Abstracts MEDLINE - Academic PubMed Central (Full Participant titles)
DatabaseTitle	CrossRef MEDLINE Medline Complete MEDLINE with Full Text PubMed MEDLINE (Ovid) ProQuest Health & Medical Complete (Alumni) Genetics Abstracts Engineering Research Database Technology Research Database Biotechnology and BioEngineering Abstracts MEDLINE - Academic
DatabaseTitleList	CrossRef MEDLINE MEDLINE - Academic ProQuest Health & Medical Complete (Alumni)
Database_xml	– sequence: 1 dbid: 24P name: Wiley Online Library Open Access url: https://authorservices.wiley.com/open-science/open-access/browse-journals.html sourceTypes: Publisher – sequence: 2 dbid: NPM name: PubMed url: https://proxy.k.utb.cz/login?url=http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed sourceTypes: Index Database – sequence: 3 dbid: EIF name: MEDLINE url: https://proxy.k.utb.cz/login?url=https://www.webofscience.com/wos/medline/basic-search sourceTypes: Index Database
DeliveryMethod	fulltext_linktorsrc
Discipline	Sociology & Social History Biology
DocumentTitleAlternate	AL EISSA et al
EISSN	1469-1809
EndPage	92
ExternalDocumentID	PMC5813151 29148569 10_1111_ahg_12226 AHG12226
Genre	article Research Support, Non-U.S. Gov't Journal Article Research Support, N.I.H., Extramural
GeographicLocations	Sweden
GeographicLocations_xml	– name: Sweden
GrantInformation_xml	– fundername: Central London NHS Blood Transfusion Service – fundername: Sylvan C. Herman Foundation – fundername: Primary Care Research Network – fundername: NIMH Grand Opportunity funderid: RCMH089905 – fundername: Stanley Medical Research Institute – fundername: Stanley Foundation – fundername: NHS Mental Health Trusts – fundername: Medical Research Council funderid: G0500791; G0701007; G1000708; G9623693N – fundername: Stanley Center for Psychiatric Research – fundername: National Institute for Health Research Mental Health Research Network – fundername: Medical Research Council grantid: G0500791 – fundername: Wellcome Trust – fundername: NIMH NIH HHS grantid: R01 MH077139 – fundername: Medical Research Council grantid: G9623693N – fundername: Wellcome Trust grantid: WT091310 – fundername: Medical Research Council grantid: G0701007 – fundername: Medical Research Council grantid: G1000708 – fundername: Medical Research Council grantid: G0500791; G0701007; G1000708; G9623693N – fundername: NIMH Grand Opportunity grantid: RCMH089905 – fundername: Swedish Research Council grantid: 2009–4959; 2011–4659 – fundername: NIMH grantid: R01MH077139
GroupedDBID	--- -~X .3N .55 .GA .GJ .Y3 05W 0R~ 10A 1OB 1OC 23M 24P 2WC 31~ 33P 36B 3O- 3SF 4.4 50Y 50Z 51W 51X 52M 52N 52O 52P 52R 52S 52T 52U 52V 52W 52X 53G 5GY 5HH 5LA 5RE 5VS 66C 6J9 702 7PT 8-0 8-1 8-3 8-4 8-5 8UM 930 A01 A03 AAESR AAEVG AAHHS AAHQN AAIPD AAMNL AANHP AANLZ AAONW AASGY AAXRX AAYCA AAZKR ABCQN ABCUV ABDBF ABEML ABGDZ ABJNI ABPVW ABQWH ABVKB ABXGK ACAHQ ACBWZ ACCFJ ACCJX ACCZN ACFBH ACGFO ACGFS ACGOF ACMXC ACNCT ACPOU ACPRK ACQPF ACRPL ACSCC ACUHS ACXBN ACXQS ACYXJ ADBBV ADBTR ADEOM ADIZJ ADKYN ADMGS ADNMO ADOZA ADXAS ADZMN ADZOD AEEZP AEGXH AEIGN AEIMD AENEX AEQDE AEUQT AEUYR AFBPY AFEBI AFFNX AFFPM AFGKR AFPWT AFWVQ AFZJQ AHBTC AHEFC AI. AIACR AIAGR AITYG AIURR AIWBW AJBDE ALAGY ALMA_UNASSIGNED_HOLDINGS ALUQN ALVPJ AMBMR AMYDB ATUGU AZBYB AZFZN AZVAB BAFTC BAWUL BDRZF BFHJK BHBCM BMXJE BROTX BRXPI BY8 C45 CAG COF CS3 D-6 D-7 D-E D-F DCZOG DIK DPXWK DR2 DRFUL DRMAN DRSTM DVXWH E3Z EAD EAP EBC EBD EBS EJD EMB EMK EMOBN EST ESX EX3 F00 F01 F04 F5P FEDTE FIJ FUBAC G-S G.N GODZA GX1 H.X HF~ HGLYW HVGLF HZI HZ~ IH2 IHE IPNFZ IX1 J0M K48 KBYEO LATKE LC2 LC3 LEEKS LH4 LITHE LOXES LP6 LP7 LUTES LW6 LYRES MEWTI MK4 MRFUL MRMAN MRSTM MSFUL MSMAN MSSTM MVM MXFUL MXMAN MXSTM N04 N05 N9A NF~ O66 O9- OHT OIG OK1 OVD P2P P2W P2X P2Z P4B P4D PALCI Q.N Q11 QB0 R.K RCA RIG RIWAO RJQFR ROL RX1 SAMSI SUPJJ SV3 TEORI TN5 TR2 TUS UB1 UKR V8K VH1 W8V W99 WBKPD WIH WIJ WIK WIN WNSPC WOHZO WOW WQJ WRC WXI WXSBR WYISQ X7M XG1 XOL ZGI ZXP ZZTAW ~IA ~WT AAYXX ADXHL AEYWJ AGHNM AGQPQ AGYGG CITATION CGR CUY CVF ECM EIF NPM 8FD AAMMB AEFGJ AGXDD AIDQK AIDYY FR3 K9. P64 RC3 7X8 5PM
ID	FETCH-LOGICAL-c4436-bb0bb9b754adbbf74b6155d8b4a27df5545b4e6d018b4938ecea7c9447e8f44f3
IEDL.DBID	DR2
ISSN	0003-4800 1469-1809
IngestDate	Thu Aug 21 18:09:41 EDT 2025 Fri Jul 11 13:46:10 EDT 2025 Wed Aug 13 06:25:22 EDT 2025 Tue Jul 01 05:30:36 EDT 2025 Thu Apr 24 23:07:36 EDT 2025 Tue Jul 01 01:47:23 EDT 2025 Wed Jan 22 16:22:36 EST 2025
IsDoiOpenAccess	true
IsOpenAccess	true
IsPeerReviewed	true
IsScholarly	true
Issue	2
Keywords	olanzapine association burden analysis
Language	English
License	Attribution http://creativecommons.org/licenses/by/4.0 2017 The Authors. Annals of Human Genetics published by University College London (UCL) and John Wiley & Sons Ltd. This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
LinkModel	DirectLink
MergedId	FETCHMERGED-LOGICAL-c4436-bb0bb9b754adbbf74b6155d8b4a27df5545b4e6d018b4938ecea7c9447e8f44f3
Notes	Funding information http://www.ncbi.nlm.nih.gov/gap Genetic analysis of the UCL cohort has been supported by UK Medical Research Council project grants G9623693N, G0500791, G0701007, and G1000708. MMAE is funded by a PhD studentship scholarship from the Kingdom of Saudi Arabia, Ministry of Health. Drs McQuillin and Bass are supported by the UCLH NIHR BRC. The UK10K project was funded by Wellcome Trust grant WT091310. The Swedish case control datasets used for the analysis described in this manuscript were obtained from dbGaP at through dbGaP accession number phs000473. Samples used for data analysis were provided by the Swedish Cohort Collection supported by the NIMH grant R01MH077139, the Sylvan C. Herman Foundation, the Stanley Medical Research Institute and The Swedish Research Council (grants 2009–4959 and 2011–4659). Support for the exome sequencing was provided by the NIMH Grand Opportunity grant RCMH089905, the Sylvan C. Herman Foundation, a grant from the Stanley Medical Research Institute and multiple gifts to the Stanley Center for Psychiatric Research at the Broad Institute of MIT and Harvard. The UCL clinical and control samples were collected with the support from the Neuroscience Research Charitable Trust, the Central London NHS Blood Transfusion Service, the Camden and Islington NHS Foundation Trust and 10 other NHS Mental Health Trusts, the Stanley Foundation, the National Institute for Health Research Mental Health Research Network, and the NIHR supported Primary Care Research Network. ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 14 content type line 23 Funding information: Genetic analysis of the UCL cohort has been supported by UK Medical Research Council project grants G9623693N, G0500791, G0701007, and G1000708. MMAE is funded by a PhD studentship scholarship from the Kingdom of Saudi Arabia, Ministry of Health. Drs McQuillin and Bass are supported by the UCLH NIHR BRC. The UK10K project was funded by Wellcome Trust grant WT091310. The Swedish case control datasets used for the analysis described in this manuscript were obtained from dbGaP at http://www.ncbi.nlm.nih.gov/gap through dbGaP accession number phs000473. Samples used for data analysis were provided by the Swedish Cohort Collection supported by the NIMH grant R01MH077139, the Sylvan C. Herman Foundation, the Stanley Medical Research Institute and The Swedish Research Council (grants 2009–4959 and 2011–4659). Support for the exome sequencing was provided by the NIMH Grand Opportunity grant RCMH089905, the Sylvan C. Herman Foundation, a grant from the Stanley Medical Research Institute and multiple gifts to the Stanley Center for Psychiatric Research at the Broad Institute of MIT and Harvard. The UCL clinical and control samples were collected with the support from the Neuroscience Research Charitable Trust, the Central London NHS Blood Transfusion Service, the Camden and Islington NHS Foundation Trust and 10 other NHS Mental Health Trusts, the Stanley Foundation, the National Institute for Health Research Mental Health Research Network, and the NIHR supported Primary Care Research Network.
ORCID	0000-0003-1567-2240 0000-0002-4089-9183 0000-0002-4481-778X
OpenAccessLink	https://proxy.k.utb.cz/login?url=https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fahg.12226
PMID	29148569
PQID	1994347561
PQPubID	1026365
PageCount	5
ParticipantIDs	pubmedcentral_primary_oai_pubmedcentral_nih_gov_5813151 proquest_miscellaneous_1966241581 proquest_journals_1994347561 pubmed_primary_29148569 crossref_primary_10_1111_ahg_12226 crossref_citationtrail_10_1111_ahg_12226 wiley_primary_10_1111_ahg_12226_AHG12226
ProviderPackageCode	CITATION AAYXX
PublicationCentury	2000
PublicationDate	March 2018
PublicationDateYYYYMMDD	2018-03-01
PublicationDate_xml	– month: 03 year: 2018 text: March 2018
PublicationDecade	2010
PublicationPlace	England
PublicationPlace_xml	– name: England – name: London – name: Hoboken
PublicationTitle	Annals of human genetics
PublicationTitleAlternate	Ann Hum Genet
PublicationYear	2018
Publisher	Wiley Subscription Services, Inc John Wiley and Sons Inc
Publisher_xml	– name: Wiley Subscription Services, Inc – name: John Wiley and Sons Inc
References	2015; 79 2015; 59 2016; 19 2012 2013; 347 2015; 30 2013; 20 2014; 24 2013; 146 2011; 13 1978 1977 2012; 491 2014; 129 2014; 506 2016; 536 2000; 97 2014; 16 2011; 68 2014 2016; 80 2003; 60 2010; 7 2014; 11 2012; 40 e_1_2_8_24_1 e_1_2_8_3_1 e_1_2_8_2_1 e_1_2_8_5_1 e_1_2_8_4_1 e_1_2_8_7_1 e_1_2_8_6_1 e_1_2_8_9_1 e_1_2_8_8_1 R Core Team (e_1_2_8_20_1) 2014 e_1_2_8_21_1 e_1_2_8_22_1 e_1_2_8_23_1 e_1_2_8_17_1 e_1_2_8_18_1 e_1_2_8_19_1 e_1_2_8_13_1 e_1_2_8_14_1 e_1_2_8_15_1 e_1_2_8_16_1 e_1_2_8_10_1 e_1_2_8_11_1 Spitzer R. L. (e_1_2_8_26_1) 1978 e_1_2_8_12_1 Spitzer R. L. (e_1_2_8_25_1) 1977
References_xml	– volume: 506 start-page: 185 year: 2014 end-page: 190 article-title: A polygenic burden of rare disruptive mutations in schizophrenia publication-title: Nature – volume: 97 start-page: 12 year: 2000 end-page: 17 article-title: Twin studies of schizophrenia: from bow‐and‐arrow concordances to star wars Mx and functional genomics publication-title: American Journal of Medical Genetics – volume: 19 start-page: 1433 year: 2016 end-page: 1441 article-title: Increased burden of ultra‐rare protein‐altering variants among 4,877 individuals with schizophrenia publication-title: Nature Neuroscience – volume: 60 start-page: 497 year: 2003 end-page: 502 article-title: The heritability of bipolar affective disorder and the genetic relationship to unipolar depression publication-title: Archives of General Psychiatry – volume: 20 start-page: 126 year: 2013 end-page: 132 article-title: Autophagy has a key role in the pathophysiology of schizophrenia publication-title: Molecular Psychiatry – volume: 491 start-page: 56 year: 2012 end-page: 65 article-title: An integrated map of genetic variation from 1,092 human genomes publication-title: Nature – volume: 59 start-page: 285 year: 2015 end-page: 597 article-title: Small molecule inhibition of the autophagy kinase ULK1 and identification of ULK1 substrates publication-title: Molecular Cell – volume: 347 start-page: 126 year: 2013 end-page: 135 article-title: Olanzapine activates hepatic mammalian target of rapamycin: new mechanistic insight into metabolic dysregulation with atypical antipsychotic drugs publication-title: Journal of Pharmacology and Experimental Therapeutics – volume: 79 start-page: 313 year: 2015 end-page: 319 article-title: Investigation of recessive effects in schizophrenia using next‐generation exome sequence data publication-title: Annals of Human Genetics – year: 1977 – year: 2014 – volume: 24 start-page: 277 year: 2014 end-page: 278 article-title: The functional GRM3 Kozak sequence variant rs148754219 affects the risk of schizophrenia and alcohol dependence as well as bipolar disorder publication-title: Psychiatric Genetics – volume: 40 start-page: W452 year: 2012 end-page: 7 article-title: SIFT web server: predicting effects of amino acid substitutions on proteins publication-title: Nucleic Acids Research – year: 2012 – volume: 146 start-page: 349 year: 2013 end-page: 356 article-title: Has the prevalence, clinical presentation and social functioning of schizophrenia changed over the last 25years? Nithsdale schizophrenia survey revisited publication-title: Schizophrenia Research – volume: 16 start-page: 583 year: 2014 end-page: 591 article-title: Analysis of ANK3 and CACNA1C variants identified in bipolar disorder whole genome sequence data publication-title: Bipolar Disorders – volume: 536 start-page: 285 year: 2016 end-page: 291 article-title: Analysis of protein‐coding genetic variation in 60,706 humans publication-title: Nature – volume: 11 start-page: 361 year: 2014 end-page: 362 article-title: MutationTaster2: mutation prediction for the deep‐sequencing age publication-title: Nature Methods – volume: 68 start-page: 241 year: 2011 end-page: 251 article-title: Prevalence and correlates of bipolar spectrum disorder in the world mental health survey initiative publication-title: Archives of General Psychiatry – volume: 80 start-page: 38 year: 2016 end-page: 49 article-title: Practical experience of the application of a weighted burden test to whole exome sequence data for obesity and schizophrenia publication-title: Annals of Human Genetics – volume: 7 start-page: 248 year: 2010 end-page: 249 article-title: A method and server for predicting damaging missense mutations publication-title: Nature Methods – year: 1978 – volume: 129 start-page: 377 year: 2014 end-page: 387 article-title: Is the mTOR‐signalling cascade disrupted in schizophrenia publication-title: Journal of Neurochemistry – volume: 30 start-page: 131 year: 2015 end-page: 138 article-title: Genetic analysis of schizophrenia and bipolar disorder reveals polygenicity but also suggests new directions for molecular interrogation publication-title: Current Opinion in Neurobiology – volume: 13 start-page: 132 year: 2011 end-page: 141 article-title: AMPK and mTOR regulate autophagy through direct phosphorylation of Ulk1 publication-title: Nature Cell Biolology – ident: e_1_2_8_21_1 doi: 10.1124/jpet.113.207621 – ident: e_1_2_8_10_1 doi: 10.1111/jnc.12622 – ident: e_1_2_8_11_1 doi: 10.1038/ncb2152 – ident: e_1_2_8_12_1 doi: 10.1038/nature19057 – ident: e_1_2_8_18_1 doi: 10.1097/YPG.0000000000000050 – ident: e_1_2_8_4_1 doi: 10.1002/(SICI)1096-8628(200021)97:1<12::AID-AJMG3>3.0.CO;2-U – ident: e_1_2_8_23_1 doi: 10.1016/j.schres.2013.02.006 – ident: e_1_2_8_24_1 doi: 10.1093/nar/gks539 – volume-title: The schedule for affective disorders and schizophrenia, lifetime version year: 1977 ident: e_1_2_8_25_1 – ident: e_1_2_8_15_1 doi: 10.1001/archgenpsychiatry.2011.12 – ident: e_1_2_8_2_1 doi: 10.1038/nature11632 – ident: e_1_2_8_19_1 doi: 10.1038/nature12975 – ident: e_1_2_8_3_1 doi: 10.1038/nmeth0410-248 – ident: e_1_2_8_22_1 doi: 10.1038/nmeth.2890 – ident: e_1_2_8_7_1 doi: 10.1016/j.molcel.2015.05.031 – ident: e_1_2_8_14_1 doi: 10.1038/mp.2013.174 – volume-title: Research diagnostic criteria for a selected group of functional disorders year: 1978 ident: e_1_2_8_26_1 – ident: e_1_2_8_13_1 doi: 10.1001/archpsyc.60.5.497 – ident: e_1_2_8_9_1 doi: 10.1038/nn.4402 – volume-title: R Foundation for Statistical Computing year: 2014 ident: e_1_2_8_20_1 – ident: e_1_2_8_17_1 doi: 10.1017/CBO9781139025997 – ident: e_1_2_8_16_1 doi: 10.1016/j.conb.2014.12.001 – ident: e_1_2_8_5_1 doi: 10.1111/ahg.12109 – ident: e_1_2_8_8_1 doi: 10.1111/bdi.12203 – ident: e_1_2_8_6_1 doi: 10.1111/ahg.12135
SSID	ssj0012843
Score	2.2821765
Snippet	Summary Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater... Schizophrenia (SCZ) is a severe, highly heritable psychiatric disorder. Elucidation of the genetic architecture of the disorder will facilitate greater...
SourceID	pubmedcentral proquest pubmed crossref wiley
SourceType	Open Access Repository Aggregation Database Index Database Enrichment Source Publisher
StartPage	88
SubjectTerms	association Autophagy Autophagy-Related Protein-1 Homolog - genetics burden analysis Case-Control Studies Exome Exome Sequencing Genotype Genotyping Humans Intracellular Signaling Peptides and Proteins - genetics Introns Kinases Mental disorders Mutation, Missense olanzapine Original Phagocytosis Schizophrenia Schizophrenia - genetics Signal transduction Sweden TOR protein
Title	Exome sequence analysis and follow up genotyping implicates rare ULK1 variants to be involved in susceptibility to schizophrenia
URI	https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fahg.12226 https://www.ncbi.nlm.nih.gov/pubmed/29148569 https://www.proquest.com/docview/1994347561 https://www.proquest.com/docview/1966241581 https://pubmed.ncbi.nlm.nih.gov/PMC5813151
Volume	82
hasFullText	1
inHoldings	1
isFullTextHit
isPrint
link	http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwnV1Li9RAEC7WFcGLj_U16zq0IuIlwyTppNN4mtUdB1-IOLAHIfQr7qAmi0lWx5M_3aq8mHEVxFuTriTdSVX318lXXwM8jIwR0krnTY2IPB5p7ikXxJ5SNpMhrj-cpOTk12_ixZK_OI6Od-BJnwvT6kMMH9woMprxmgJc6XIjyNXJx4mPsxvJbRNXiwDRu0E6iobdsN8tjyMq6lSFiMUznLk9F50DmOd5kpv4tZmA5lfhQ9_0lnfyaVJXemJ-_Kbq-J99uwZXOmDKZq0nXYcdl-_BpXaryvUe7A-ZLewRa3N6WSsxsr4BP4--F18c62nZTHVKJ1iwLENPK76x-pSRHmy1pgQttuqI7K5k2EzHlq9e-uwM1-1Ey2FVwbRjqxyHzjNnscDKumz4Nw2Vd00G5SZb8CYs50fvny68bmsHz3Aexp7WU62lFhFXVutMcE3_R22iuQqEzRDjoNe42E59PCTDxBmnhJGcC5dknGfhLdjNi9zdAZZIa0IjtfOxOjOxEgFCEryY7wI7teEIHvcvOTWd7jltv_E57dc_-LTT5mmP4MFgetqKffzJ6KD3lLSL9zIlheWQCwSjI7g_VGOk0u8XlbuiJps4JryUoM3t1rGGuwQSl6VRLEcgtlxuMCAV8O2afHXSqIHj9UKEbdjNxqP-3vB0tnjeFPb_3fQuXEaEmLSkuwPYrb7W7h6isEqP4ULA347h4uzw2eF83ATfL_CYM9g
linkProvider	Wiley-Blackwell
linkToHtml	http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwnV1Lb9QwEB6VIgQXHoXClgIGIcQlq03i2LHEpUItC932gLpSLyjyK3QFJBVJCsuJn87YeWiXgoS4WfFs4mRn7G-Sbz4DPE-05sIIG0w0TwKaKBpIG7FASpOLGPMPK1xx8tExm87pu9PkdANe9bUwrT7E8MLNRYafr12AuxfSK1Euzz6OQ1ze2BW46nb09gnV-0E8yk28cb9fHkVc1OkKOR7P8NP11egSxLzMlFxFsH4JOrgFH_rBt8yTT-OmVmP94zddx_-9u9tws8OmZK91pjuwYYstuNbuVrncgp2huIW8IG1ZL2lVRpZ34ef-9_KLJT0zm8hO7AQbhuTobOU30pwTJwlbL12NFll0XHZbERynJfPZYUguMHV3zBxSl0RZsihw9rywBhukaipPwfFs3qUzqFYJg_dgfrB_8noadLs7BJrSmAVKTZQSiidUGqVyTpX7RGpSRWXETY4wBx3HMjMJ8ZCIU6ut5FpQym2aU5rH27BZlIV9ACQVRsdaKBtid66Z5BGiEjxZaCMzMfEIXvb_cqY76XO3A8fnrE-B8Gln_mmP4Nlget7qffzJaLd3lawL-SpzIssx5YhHR_B06MZgdV9gZGHLxtkw5iBTijb3W88arhIJzEwTJkbA13xuMHBC4Os9xeLMC4Lj-WJEbnib3qX-PvBsb_rGN3b-3fQJXJ-eHM2y2dvjw4dwAwFj2nLwdmGz_trYRwjKavXYx94vFLk1qg
linkToPdf	http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwnV1Lb9QwEB6VIhAXHuW1pYBBCHHJKg_HjsWpol0WWiqEWKkHpMiv0FVLsiJJYTnx0xnnpV0KEuJmxZPETmbsz8k3nwGexVpzYYT1fM1jj8aKetKGzJPSZCLC9YcVLjn53RGbzujb4_h4A172uTCtPsTwwc1FRjNeuwBfmGwlyOXJ53GAsxu7BJcp8xPn0nsfBu0oN-5G_XZ5FGFRJyvkaDzDqeuT0QWEeZEouQpgmxlocgM-9W1viSen47pSY_3jN1nH_-zcTbjeIVOy27rSLdiw-RZcafeqXG7B9pDaQp6TNqmXtBojy9vwc_978cWSnpdNZCd1ggVDMnS14hupF8QJwlZLl6FF5h2T3ZYEm2nJ7PAgIOe4cHe8HFIVRFkyz3HsPLcGC6Ssy4aA03B5l86gXKUL3oHZZP_jq6nX7e3gaUoj5inlKyUUj6k0SmWcKveD1CSKypCbDEEOuo1lxg_wkIgSq63kWlDKbZJRmkV3YTMvcnsfSCKMjrRQNsDqTDPJQ8QkeLHAhsY30Qhe9C851Z3wudt_4yztF0D4tNPmaY_g6WC6aNU-_mS003tK2gV8mTqJ5YhyRKMjeDJUY6i6_y8yt0XtbBhzgClBm3utYw13CQWuS2MmRsDXXG4wcDLg6zX5_KSRA8frRYjbsJuNR_294enu9HVT2P5308dw9f3eJD18c3TwAK4hWkxaAt4ObFZfa_sQEVmlHjWR9wt3bTRi
openUrl	ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fsummon.serialssolutions.com&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Ajournal&rft.genre=article&rft.atitle=Exome+sequence+analysis+and+follow+up+genotyping+implicates+rare+ULK1+variants+to+be+involved+in+susceptibility+to+schizophrenia&rft.jtitle=Annals+of+human+genetics&rft.au=Al+Eissa%2C+Mariam+M&rft.au=Fiorentino%2C+Alessia&rft.au=Sharp%2C+Sally+I&rft.au=O%27Brien%2C+Niamh+L&rft.date=2018-03-01&rft.issn=1469-1809&rft.eissn=1469-1809&rft.volume=82&rft.issue=2&rft.spage=88&rft_id=info:doi/10.1111%2Fahg.12226&rft.externalDBID=NO_FULL_TEXT
thumbnail_l	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/lc.gif&issn=0003-4800&client=summon
thumbnail_m	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/mc.gif&issn=0003-4800&client=summon
thumbnail_s	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/sc.gif&issn=0003-4800&client=summon