Diagnostic challenge of Diamond–Blackfan anemia in mothers and children by whole-exome sequencing

被引：0

作者：

Takuya Ichimura

Kenichi Yoshida

Yusuke Okuno

Toshiaki Yujiri

Kozo Nagai

Masanori Nishi

Yuichi Shiraishi

Hiroo Ueno

Tsutomu Toki

Kenichi Chiba

Hiroko Tanaka

Hideki Muramatsu

Toshiro Hara

Hitoshi Kanno

Seiji Kojima

Satoru Miyano

Etsuro Ito

Seishi Ogawa

Shouichi Ohga

机构：

[1] Yamaguchi University Graduate School of Medicine,Department of Pediatrics

[2] Graduate School of Medicine,Department of Pathology and Tumor Biology

[3] Kyoto University,Department of Pediatrics

[4] Nagoya University Graduate School of Medicine,Center for Advanced Medicine and Clinical Research

[5] Nagoya University Hospital,Third Department of Internal Medicine

[6] Yamaguchi University Graduate School of Medicine,Department of Pediatrics

[7] Faculty of Medicine,Laboratory of DNA Information Analysis, Human Genome Center, Institute of Medical Science

[8] Saga University,Department of Pediatrics

[9] The University of Tokyo,Laboratory of Sequence Analysis, Human Genome Center, Institute of Medical Science

[10] Hirosaki University Graduate School of Medicine,Department of Pediatrics

[11] The University of Tokyo,Department of Transfusion Medicine and Cell Processing

[12] Graduate School of Medical Sciences,undefined

[13] Kyushu University,undefined

[14] Tokyo Women’s Medical University,undefined

来源：

International Journal of Hematology | 2017年 / 105卷

关键词：

Diamond–Blackfan anemia; Ribosomal protein; Inherited bone marrow failure syndrome; Whole-exome sequencing;

D O I：

暂无

中图分类号：

学科分类号：

摘要：

Diamond–Blackfan anemia (DBA) is a pure red cell aplasia that arises from defective ribosomal proteins (RPs). Patients with this rare ribosomopathy present with neonatal anemia and occasional dysmorphism. Clinical heterogeneity and clusters of causative RP genes hamper the diagnosis and perinatal management. We report three mother-and-child pairs of anemia who were finally diagnosed by whole-exome sequencing. Each pair showed distinct disease severity and response to anemia treatment. Only one mother had the diagnostic dysmorphism, including short stature, webbed neck, and thenar hypoplasia. This mother had a frame-shift mutation of RPL11 (exon 3, c.58_59del). Her infant showed transient neonatal anemia, but had no mutations of RP genes. The other mother–child pairs had a missense mutation of RPS19 (exon 4, c.185G>A), and a splicing error of RPS7 (exon 3, c.76-1G>T), respectively. Other than the reported mutations, there were no variants in genes significantly associated with anemia. Our results suggested that whole-exome sequencing (WES) is effective for achieving a prompt and correct diagnosis of human ribosomopathy.

引用

页码：515 / 520

页数：5

共 50 条

[1] Diagnostic challenge of Diamond-Blackfan anemia in mothers and children by whole-exome sequencing
Ichimura, Takuya
Yoshida, Kenichi
Okuno, Yusuke
Yujiri, Toshiaki
Nagai, Kozo
Nishi, Masanori
Shiraishi, Yuichi
Ueno, Hiroo
Toki, Tsutomu
Chiba, Kenichi
Tanaka, Hiroko
Muramatsu, Hideki
Hara, Toshiro
Kanno, Hitoshi
Kojima, Seiji
Miyano, Satoru
Ito, Etsuro
Ogawa, Seishi
Ohga, Shouichi
INTERNATIONAL JOURNAL OF HEMATOLOGY, 2017, 105 (04) : 515 - 520
[2] Molecular diagnostic yield of whole-exome sequencing in Saudi autistic children with epilepsy
Alharbi, Asmaa Ali
Al-Zahrani, Maryam Hassan
Ebbi, Maram Mohammed
Alqurashi, May Majed
Baqays, Afnan Abdulrahman
Shami, Ashjan
Alghamdi, Rana Abdullah
Alzahrani, Alaa Hassan
INTERNATIONAL JOURNAL OF HEALTH SCIENCES-IJHS, 2024, 18 (03): : 15 - 22
[3] Effectiveness of whole-exome sequencing and costs of the traditional diagnostic trajectory in children with intellectual disability
Monroe, Glen R.
Frederix, Gerardus W.
Savelberg, Sanne M. C.
de Vries, Tamar I.
Duran, Karen J.
van der Smagt, Jasper J.
Terhal, Paulien A.
van Hasselt, Peter M.
Kroes, Hester Y.
Verhoeven-Duif, Nanda M.
Nijman, Isaac J.
Carbo, Ellen C.
van Gassen, Koen L.
Knoers, Nine V.
Hovels, Anke M.
van Haelst, Mieke M.
Visser, Gepke
van Haaften, Gijs
GENETICS IN MEDICINE, 2016, 18 (09) : 949 - 956
[4] Molecular diagnostic experience of whole-exome sequencing in adult patients
Posey, Jennifer E.
Rosenfeld, Jill A.
James, Regis A.
Bainbridge, Matthew
Niu, Zhiyv
Wang, Xia
Dhar, Shweta
Wiszniewski, Wojciech
Akdemir, Zeynep H. C.
Gambin, Tomasz
Xia, Fan
Person, Richard E.
Walkiewicz, Magdalena
Shaw, Chad A.
Sutton, V. Reid
Beaudet, Arthur L.
Muzny, Donna
Eng, Christine M.
Yang, Yaping
Gibbs, Richard A.
Lupski, James R.
Boerwinkle, Eric
Plon, Sharon E.
GENETICS IN MEDICINE, 2016, 18 (07) : 678 - 685
[5] Whole-exome sequencing as a diagnostic tool: current challenges and future opportunities
Tetreault, Martine
Bareke, Eric
Nadaf, Javad
Alirezaie, Najmeh
Majewski, Jacek
EXPERT REVIEW OF MOLECULAR DIAGNOSTICS, 2015, 15 (06) : 749 - 760
[6] Whole-exome sequencing as a diagnostic tool for distal renal tubular acidosis
Barros Pereira, Paula Cristina
Melo, Flavia Medeiros
Cunha De Marco, Luiz Armando
Oliveira, Eduardo Araujo
Miranda, Debora Marques
Simoes e Silva, Ana Cristina
JORNAL DE PEDIATRIA, 2015, 91 (06) : 583 - 589
[7] Identification of potential pathogenic genes for severe aplastic anemia by whole-exome sequencing
Zhang, Yang
Zhang, Yu
Ge, Hongyu
Li, Nianbin
Liu, Chunyan
Wang, Ting
Fu, Rong
Shao, Zonghong
JOURNAL OF CLINICAL LABORATORY ANALYSIS, 2022, 36 (05)
[8] Whole-Exome/Genome Sequencing and Genomics
Grody, Wayne W.
Thompson, Barry H.
Hudgins, Louanne
PEDIATRICS, 2013, 132 : S211 - S215
[9] Whole-exome sequencing in the differential diagnosis of primary adrenal insufficiency in children
Chan, Li F.
Campbell, Daniel C.
Novoselova, Tatiana V.
Clark, Adrian J. L.
Metherell, Louise A.
FRONTIERS IN ENDOCRINOLOGY, 2016, 6
[10] Whole-exome sequencing for genetic diagnosis of idiopathic liver injury in children
Lulecioglu, Aysima Atilgan
Yazici, Yilmaz Yucehan
Baran, Alperen
Warasnhe, Khaled
Beyaz, Sengul
Aytekin, Caner
Ozcay, Figen
Aydemir, Yusuf
Baris, Zeren
Belkaya, Serkan
JOURNAL OF CELLULAR AND MOLECULAR MEDICINE, 2024, 28 (11)

← 1 2 3 4 5 →