Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypes

Tiia Maria Luukkonen; Mana M Mehrjouy; Minna Pöyhönen; Anna-Kaisa Anttonen; Päivi Lahermo; Pekka Ellonen; Lars Paulin; Niels Tommerup; Aarno Palotie; Teppo Varilo

doi:10.1002/mgg3.346

Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypes

Tiia Maria Luukkonen, Mana M Mehrjouy, Minna Pöyhönen, Anna-Kaisa Anttonen, Päivi Lahermo, Pekka Ellonen, Lars Paulin, Niels Tommerup, Aarno Palotie, Teppo Varilo

Medical Genetics Program

4 Citations (Scopus)

46 Downloads (Pure)

Abstract

BACKGROUND: The risk of serious congenital anomaly for de novo balanced translocations is estimated to be at least 6%. We identified two apparently independent families with a balanced t(1;12)(q43;q21.1) as an outcome of a "Systematic Survey of Balanced Chromosomal Rearrangements in Finns." In the first family, carriers (n = 6) manifest with learning problems in childhood, and later with unexplained neurological symptoms (chronic headache, balance problems, tremor, fatigue) and cerebral infarctions in their 50s. In the second family, two carriers suffer from tetralogy of Fallot, one from transient ischemic attack and one from migraine. The translocation cosegregates with these vascular phenotypes and neurological symptoms.

METHODS AND RESULTS: We narrowed down the breakpoint regions using mate pair sequencing. We observed conserved haplotypes around the breakpoints, pointing out that this translocation has arisen only once. The chromosome 1 breakpoint truncates a CHRM3 processed transcript, and is flanked by the 5' end of CHRM3 and the 3' end of RYR2. TRHDE, KCNC2, and ATXN7L3B flank the chromosome 12 breakpoint.

CONCLUSIONS: This study demonstrates a balanced t(1;12)(q43;q21.1) with conserved haplotypes on the derived chromosomes. The translocation seems to result in vascular phenotype, with or without neurological symptoms, in at least two families. We suggest that the translocation influences the positional expression of CHRM3, RYR2, TRHDE, KCNC2, and/or ATXN7L3B.

Original language	English
Journal	Molecular genetics & genomic medicine
Volume	6
Issue number	1
Pages (from-to)	56-68
ISSN	2324-9269
DOIs	https://doi.org/10.1002/mgg3.346
Publication status	Published - Jan 2018

Access to Document

10.1002/mgg3.346Licence: CC BY

Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypesFinal published version, 2.07 MBLicence: CC BY

Cite this

Luukkonen, T. M., Mehrjouy, M. M., Pöyhönen, M., Anttonen, A-K., Lahermo, P., Ellonen, P., Paulin, L., Tommerup, N., Palotie, A., & Varilo, T. (2018). Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypes. Molecular genetics & genomic medicine, 6(1), 56-68. https://doi.org/10.1002/mgg3.346

Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypes. / Luukkonen, Tiia Maria; Mehrjouy, Mana M; Pöyhönen, Minna et al.

In: Molecular genetics & genomic medicine, Vol. 6, No. 1, 01.2018, p. 56-68.

Research output: Contribution to journal › Journal article › Research › peer-review

Luukkonen, TM, Mehrjouy, MM, Pöyhönen, M, Anttonen, A-K, Lahermo, P, Ellonen, P, Paulin, L, Tommerup, N, Palotie, A & Varilo, T 2018, 'Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypes', Molecular genetics & genomic medicine, vol. 6, no. 1, pp. 56-68. https://doi.org/10.1002/mgg3.346

@article{65f0f6f2190a4d209b1d51eafc646c30,

title = "Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypes",

abstract = "BACKGROUND: The risk of serious congenital anomaly for de novo balanced translocations is estimated to be at least 6%. We identified two apparently independent families with a balanced t(1;12)(q43;q21.1) as an outcome of a {"}Systematic Survey of Balanced Chromosomal Rearrangements in Finns.{"} In the first family, carriers (n = 6) manifest with learning problems in childhood, and later with unexplained neurological symptoms (chronic headache, balance problems, tremor, fatigue) and cerebral infarctions in their 50s. In the second family, two carriers suffer from tetralogy of Fallot, one from transient ischemic attack and one from migraine. The translocation cosegregates with these vascular phenotypes and neurological symptoms.METHODS AND RESULTS: We narrowed down the breakpoint regions using mate pair sequencing. We observed conserved haplotypes around the breakpoints, pointing out that this translocation has arisen only once. The chromosome 1 breakpoint truncates a CHRM3 processed transcript, and is flanked by the 5' end of CHRM3 and the 3' end of RYR2. TRHDE, KCNC2, and ATXN7L3B flank the chromosome 12 breakpoint.CONCLUSIONS: This study demonstrates a balanced t(1;12)(q43;q21.1) with conserved haplotypes on the derived chromosomes. The translocation seems to result in vascular phenotype, with or without neurological symptoms, in at least two families. We suggest that the translocation influences the positional expression of CHRM3, RYR2, TRHDE, KCNC2, and/or ATXN7L3B.",

author = "Luukkonen, {Tiia Maria} and Mehrjouy, {Mana M} and Minna P{\"o}yh{\"o}nen and Anna-Kaisa Anttonen and P{\"a}ivi Lahermo and Pekka Ellonen and Lars Paulin and Niels Tommerup and Aarno Palotie and Teppo Varilo",

note = "{\textcopyright} 2017 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals, Inc.",

year = "2018",

month = jan,

doi = "10.1002/mgg3.346",

language = "English",

volume = "6",

pages = "56--68",

journal = "Molecular Genetics & Genomic Medicine",

issn = "2324-9269",

publisher = "JohnWiley & Sons Ltd",

number = "1",

}

TY - JOUR

T1 - Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypes

AU - Luukkonen, Tiia Maria

AU - Mehrjouy, Mana M

AU - Pöyhönen, Minna

AU - Anttonen, Anna-Kaisa

AU - Lahermo, Päivi

AU - Ellonen, Pekka

AU - Paulin, Lars

AU - Tommerup, Niels

AU - Palotie, Aarno

AU - Varilo, Teppo

PY - 2018/1

Y1 - 2018/1

N2 - BACKGROUND: The risk of serious congenital anomaly for de novo balanced translocations is estimated to be at least 6%. We identified two apparently independent families with a balanced t(1;12)(q43;q21.1) as an outcome of a "Systematic Survey of Balanced Chromosomal Rearrangements in Finns." In the first family, carriers (n = 6) manifest with learning problems in childhood, and later with unexplained neurological symptoms (chronic headache, balance problems, tremor, fatigue) and cerebral infarctions in their 50s. In the second family, two carriers suffer from tetralogy of Fallot, one from transient ischemic attack and one from migraine. The translocation cosegregates with these vascular phenotypes and neurological symptoms.METHODS AND RESULTS: We narrowed down the breakpoint regions using mate pair sequencing. We observed conserved haplotypes around the breakpoints, pointing out that this translocation has arisen only once. The chromosome 1 breakpoint truncates a CHRM3 processed transcript, and is flanked by the 5' end of CHRM3 and the 3' end of RYR2. TRHDE, KCNC2, and ATXN7L3B flank the chromosome 12 breakpoint.CONCLUSIONS: This study demonstrates a balanced t(1;12)(q43;q21.1) with conserved haplotypes on the derived chromosomes. The translocation seems to result in vascular phenotype, with or without neurological symptoms, in at least two families. We suggest that the translocation influences the positional expression of CHRM3, RYR2, TRHDE, KCNC2, and/or ATXN7L3B.

AB - BACKGROUND: The risk of serious congenital anomaly for de novo balanced translocations is estimated to be at least 6%. We identified two apparently independent families with a balanced t(1;12)(q43;q21.1) as an outcome of a "Systematic Survey of Balanced Chromosomal Rearrangements in Finns." In the first family, carriers (n = 6) manifest with learning problems in childhood, and later with unexplained neurological symptoms (chronic headache, balance problems, tremor, fatigue) and cerebral infarctions in their 50s. In the second family, two carriers suffer from tetralogy of Fallot, one from transient ischemic attack and one from migraine. The translocation cosegregates with these vascular phenotypes and neurological symptoms.METHODS AND RESULTS: We narrowed down the breakpoint regions using mate pair sequencing. We observed conserved haplotypes around the breakpoints, pointing out that this translocation has arisen only once. The chromosome 1 breakpoint truncates a CHRM3 processed transcript, and is flanked by the 5' end of CHRM3 and the 3' end of RYR2. TRHDE, KCNC2, and ATXN7L3B flank the chromosome 12 breakpoint.CONCLUSIONS: This study demonstrates a balanced t(1;12)(q43;q21.1) with conserved haplotypes on the derived chromosomes. The translocation seems to result in vascular phenotype, with or without neurological symptoms, in at least two families. We suggest that the translocation influences the positional expression of CHRM3, RYR2, TRHDE, KCNC2, and/or ATXN7L3B.

U2 - 10.1002/mgg3.346

DO - 10.1002/mgg3.346

M3 - Journal article

C2 - 29168350

SN - 2324-9269

VL - 6

SP - 56

EP - 68

JO - Molecular Genetics & Genomic Medicine

JF - Molecular Genetics & Genomic Medicine

IS - 1

ER -

Breakpoint mapping and haplotype analysis of translocation t(1;12)(q43;q21.1) in two apparently independent families with vascular phenotypes

Abstract

Access to Document

Fingerprint

Cite this