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Characterization of contiguous gene deletions in COL4A6 and COL4A5 in Alport syndrome-diffuse leiomyomatosis

Characterization of contiguous gene deletions in COL4A6 and COL4A5 in Alport syndrome-diffuse leiomyomatosis
Characterization of contiguous gene deletions in COL4A6 and COL4A5 in Alport syndrome-diffuse leiomyomatosis
Alport syndrome-diffuse leiomyomatosis (AS-DL, OMIM: 308940) is a rare variant of the X-linked Alport syndrome that shows overgrowth of visceral smooth muscles in the gastrointestinal, respiratory and female reproductive tracts in addition to renal symptoms. AS-DL results from deletions that encompass the 5′ ends of the COL4A5 and COL4A6 genes, but deletion breakpoints between COL4A5 and COL4A6 have been determined in only four cases. Here, we characterize deletion breakpoints in five AS-DL patients and show a contiguous COL4A6/COL4A5 deletion in each case. We also demonstrate that eight out of nine deletion alleles involved sequences homologous between COL4A5 and COL4A6. Most breakpoints took place in recognizable transposed elements, including long and short interspersed repeats, DNA transposons and long-terminal repeat retrotransposons. Because deletions involved the bidirectional promoter region in each case, we suggest that the occurrence of leiomyomatosis in AS-DL requires inactivation of both genes. Altogether, our study highlights the importance of homologous recombination involving multiple transposed elements for the development of this continuous gene syndrome and other atypical loss-of-function phenotypes.
1434-5161
733-735
Nozu, Kandai
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Minamikawa, Shogo
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Yamada, Shiro
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Oka, Masafumi
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Yanagita, Motoko
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Morisada, Naoya
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Fujinaga, Shuichiro
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Nagano, China
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Gotoh, Yoshimitsu
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Takahashi, Eihiko
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Morishita, Takahiro
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Yamamura, Tomohiko
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Ninchoji, Takeshi
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Kaito, Hiroshi
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Morioka, Ichiro
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Nakanishi, Koichi
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Vorechovsky, Igor
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Iijima, Kazumoto
0025351f-84e0-429a-ba94-befdbe081d1a
Nozu, Kandai
5b83b5a2-174f-4fc4-81aa-58f7466ea38b
Minamikawa, Shogo
ca8c028e-d5bd-44d4-b919-8fe9e6975e25
Yamada, Shiro
1022bc54-f3dc-45f5-ab62-9da5adf4b88f
Oka, Masafumi
f42f22b8-61a9-464f-bda2-e8b0c0d07982
Yanagita, Motoko
d1cb9761-55db-4be1-8346-6fda7ef1ef01
Morisada, Naoya
409060b8-1786-4551-8bcd-88c40a237147
Fujinaga, Shuichiro
8adc1eca-2dae-4ce4-95e0-4a3404acce75
Nagano, China
10f8d12d-37f3-480f-bf24-ecd9abeab9bd
Gotoh, Yoshimitsu
b828b174-c68c-421f-bfb9-8759d13e8aa1
Takahashi, Eihiko
7c1c5f07-6428-4417-96ee-0d23e4948d84
Morishita, Takahiro
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Yamamura, Tomohiko
27cae891-fdd3-473e-8481-d1eff3aea6dd
Ninchoji, Takeshi
2c6a2137-39db-4ce5-b3e9-953be731a502
Kaito, Hiroshi
ca0486de-6b30-44c4-a7f0-5e103f701fa1
Morioka, Ichiro
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Nakanishi, Koichi
314cded2-4bdb-4275-95c9-0c8cd73c887e
Vorechovsky, Igor
7245de2f-8c9b-4034-8935-9a451d9b682e
Iijima, Kazumoto
0025351f-84e0-429a-ba94-befdbe081d1a

Nozu, Kandai, Minamikawa, Shogo, Yamada, Shiro, Oka, Masafumi, Yanagita, Motoko, Morisada, Naoya, Fujinaga, Shuichiro, Nagano, China, Gotoh, Yoshimitsu, Takahashi, Eihiko, Morishita, Takahiro, Yamamura, Tomohiko, Ninchoji, Takeshi, Kaito, Hiroshi, Morioka, Ichiro, Nakanishi, Koichi, Vorechovsky, Igor and Iijima, Kazumoto (2017) Characterization of contiguous gene deletions in COL4A6 and COL4A5 in Alport syndrome-diffuse leiomyomatosis. Journal of Human Genetics, 62 (7), 733-735. (doi:10.1038/jhg.2017.28).

Record type: Article

Abstract

Alport syndrome-diffuse leiomyomatosis (AS-DL, OMIM: 308940) is a rare variant of the X-linked Alport syndrome that shows overgrowth of visceral smooth muscles in the gastrointestinal, respiratory and female reproductive tracts in addition to renal symptoms. AS-DL results from deletions that encompass the 5′ ends of the COL4A5 and COL4A6 genes, but deletion breakpoints between COL4A5 and COL4A6 have been determined in only four cases. Here, we characterize deletion breakpoints in five AS-DL patients and show a contiguous COL4A6/COL4A5 deletion in each case. We also demonstrate that eight out of nine deletion alleles involved sequences homologous between COL4A5 and COL4A6. Most breakpoints took place in recognizable transposed elements, including long and short interspersed repeats, DNA transposons and long-terminal repeat retrotransposons. Because deletions involved the bidirectional promoter region in each case, we suggest that the occurrence of leiomyomatosis in AS-DL requires inactivation of both genes. Altogether, our study highlights the importance of homologous recombination involving multiple transposed elements for the development of this continuous gene syndrome and other atypical loss-of-function phenotypes.

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Accepted/In Press date: 31 January 2017
e-pub ahead of print date: 9 March 2017
Published date: July 2017
Organisations: Human Development & Health

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Local EPrints ID: 408099
URI: http://eprints.soton.ac.uk/id/eprint/408099
ISSN: 1434-5161
PURE UUID: ae727cc5-f489-493b-b378-1f63f83d876f
ORCID for Igor Vorechovsky: ORCID iD orcid.org/0000-0002-6740-6502

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Date deposited: 11 May 2017 01:10
Last modified: 16 Mar 2024 05:14

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Contributors

Author: Kandai Nozu
Author: Shogo Minamikawa
Author: Shiro Yamada
Author: Masafumi Oka
Author: Motoko Yanagita
Author: Naoya Morisada
Author: Shuichiro Fujinaga
Author: China Nagano
Author: Yoshimitsu Gotoh
Author: Eihiko Takahashi
Author: Takahiro Morishita
Author: Tomohiko Yamamura
Author: Takeshi Ninchoji
Author: Hiroshi Kaito
Author: Ichiro Morioka
Author: Koichi Nakanishi
Author: Kazumoto Iijima

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