The genetic basis of asymptomatic codon 8 frame-shift (HBB: C25_26delAA) β0-thalassaemia homozygotes

Zhihua Jiang; Hong yuan Luo; Shengwen Huang; John J. Farrell; Lance Davis; Roger Théberge; Katherine A. Benson; Suchada Riolueang; Vip Viprakasit; Nasir A.S. Al-Allawi; Sule Ünal; Fatma Gümrük; Nejat Akar; A. Nazli Başak; Leonor Osorio; Catherine Badens; Serge Pissard; Philippe Joly; Andrew D. Campbell; Patrick G. Gallagher; Martin H. Steinberg; Bernard G. Forget; David H.K. Chui

doi:10.1111/bjh.13909

The genetic basis of asymptomatic codon 8 frame-shift (HBB: C25_26delAA) β⁰-thalassaemia homozygotes

Zhihua Jiang
, Hong yuan Luo
, Shengwen Huang
, John J. Farrell
, Lance Davis
, Roger Théberge
, Katherine A. Benson
, Suchada Riolueang
, Vip Viprakasit
, Nasir A.S. Al-Allawi
, Sule Ünal
, Fatma Gümrük
, Nejat Akar
, A. Nazli Başak
, Leonor Osorio
, Catherine Badens
, Serge Pissard
, Philippe Joly
, Andrew D. Campbell
, Patrick G. Gallagher

Martin H. Steinberg, Bernard G. Forget, David H.K. Chui

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

4 Citations (Scopus)

Abstract

Two 21-year old dizygotic twin men of Iraqi descent were homozygous for HBB codon 8, deletion of two nucleotides (-AA) frame-shift β⁰-thalassaemia mutation (FSC8; HBB:c25_26delAA). Both were clinically well, had splenomegaly, and were never transfused. They had mild microcytic anaemia (Hb 120-130 g/l) and 98% of their haemoglobin was fetal haemoglobin (HbF). Both were carriers of Hph α-thalassaemia mutation. On the three major HbF quantitative trait loci (QTL), the twins were homozygous for G>A HBG2 Xmn1 site at single nucleotide polymorphism (SNP) rs7482144, homozygous for 3-bp deletion HBS1L-MYB intergenic polymorphism (HMIP) at rs66650371, and heterozygous for the A>C BCL11A intron 2 polymorphism at rs766432. These findings were compared with those found in 22 other FSC8 homozygote patients: four presented with thalassaemia intermedia phenotype, and 18 were transfusion dependent. The inheritance of homozygosity for HMIP 3-bp deletion at rs66650371 and heterozygosity for Hph α-thalassaemia mutation was found in the twins and not found in any of the other 22 patients. Further studies are needed to uncover likely additional genetic variants that could contribute to the exceptionally high HbF levels and mild phenotype in these twins.

Original language	English
Pages (from-to)	958-965
Number of pages	8
Journal	British Journal of Haematology
Volume	172
Issue number	6
DOIs	https://doi.org/10.1111/bjh.13909
Publication status	Published - 1 Mar 2016

Keywords

Fetal haemoglobin
HBS1L-MYB intergenic polymorphism
HbF quantitative trait loci
α-Thalassaemia
β-Thalassaemia

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10.1111/bjh.13909

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Jiang, Z., Luo, H. Y., Huang, S., Farrell, J. J., Davis, L., Théberge, R., Benson, K. A., Riolueang, S., Viprakasit, V., Al-Allawi, N. A. S., Ünal, S., Gümrük, F., Akar, N., Başak, A. N., Osorio, L., Badens, C., Pissard, S., Joly, P., Campbell, A. D., ... Chui, D. H. K. (2016). The genetic basis of asymptomatic codon 8 frame-shift (HBB: C25_26delAA) β⁰-thalassaemia homozygotes. British Journal of Haematology, 172(6), 958-965. https://doi.org/10.1111/bjh.13909

@article{479ca513b21643bc864083b5e79c0c87,

title = "The genetic basis of asymptomatic codon 8 frame-shift (HBB: C25\_26delAA) β0-thalassaemia homozygotes",

abstract = "Two 21-year old dizygotic twin men of Iraqi descent were homozygous for HBB codon 8, deletion of two nucleotides (-AA) frame-shift β0-thalassaemia mutation (FSC8; HBB:c25\_26delAA). Both were clinically well, had splenomegaly, and were never transfused. They had mild microcytic anaemia (Hb 120-130 g/l) and 98\% of their haemoglobin was fetal haemoglobin (HbF). Both were carriers of Hph α-thalassaemia mutation. On the three major HbF quantitative trait loci (QTL), the twins were homozygous for G>A HBG2 Xmn1 site at single nucleotide polymorphism (SNP) rs7482144, homozygous for 3-bp deletion HBS1L-MYB intergenic polymorphism (HMIP) at rs66650371, and heterozygous for the A>C BCL11A intron 2 polymorphism at rs766432. These findings were compared with those found in 22 other FSC8 homozygote patients: four presented with thalassaemia intermedia phenotype, and 18 were transfusion dependent. The inheritance of homozygosity for HMIP 3-bp deletion at rs66650371 and heterozygosity for Hph α-thalassaemia mutation was found in the twins and not found in any of the other 22 patients. Further studies are needed to uncover likely additional genetic variants that could contribute to the exceptionally high HbF levels and mild phenotype in these twins.",

keywords = "Fetal haemoglobin, HBS1L-MYB intergenic polymorphism, HbF quantitative trait loci, α-Thalassaemia, β-Thalassaemia",

author = "Zhihua Jiang and Luo, \{Hong yuan\} and Shengwen Huang and Farrell, \{John J.\} and Lance Davis and Roger Th{\'e}berge and Benson, \{Katherine A.\} and Suchada Riolueang and Vip Viprakasit and Al-Allawi, \{Nasir A.S.\} and Sule {\"U}nal and Fatma G{\"u}mr{\"u}k and Nejat Akar and Ba{\c s}ak, \{A. Nazli\} and Leonor Osorio and Catherine Badens and Serge Pissard and Philippe Joly and Campbell, \{Andrew D.\} and Gallagher, \{Patrick G.\} and Steinberg, \{Martin H.\} and Forget, \{Bernard G.\} and Chui, \{David H.K.\}",

note = "Publisher Copyright: {\textcopyright} 2016 John Wiley \& Sons Ltd.",

year = "2016",

month = mar,

day = "1",

doi = "10.1111/bjh.13909",

language = "English",

volume = "172",

pages = "958--965",

journal = "British Journal of Haematology",

issn = "0007-1048",

publisher = "John Wiley and Sons Inc",

number = "6",

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Jiang, Z, Luo, HY, Huang, S, Farrell, JJ, Davis, L, Théberge, R, Benson, KA, Riolueang, S, Viprakasit, V, Al-Allawi, NAS, Ünal, S, Gümrük, F, Akar, N, Başak, AN, Osorio, L, Badens, C, Pissard, S, Joly, P, Campbell, AD, Gallagher, PG, Steinberg, MH, Forget, BG & Chui, DHK 2016, 'The genetic basis of asymptomatic codon 8 frame-shift (HBB: C25_26delAA) β⁰-thalassaemia homozygotes', British Journal of Haematology, vol. 172, no. 6, pp. 958-965. https://doi.org/10.1111/bjh.13909

TY - JOUR

T1 - The genetic basis of asymptomatic codon 8 frame-shift (HBB: C25_26delAA) β0-thalassaemia homozygotes

AU - Jiang, Zhihua

AU - Luo, Hong yuan

AU - Huang, Shengwen

AU - Farrell, John J.

AU - Davis, Lance

AU - Théberge, Roger

AU - Benson, Katherine A.

AU - Riolueang, Suchada

AU - Viprakasit, Vip

AU - Al-Allawi, Nasir A.S.

AU - Ünal, Sule

AU - Gümrük, Fatma

AU - Akar, Nejat

AU - Başak, A. Nazli

AU - Osorio, Leonor

AU - Badens, Catherine

AU - Pissard, Serge

AU - Joly, Philippe

AU - Campbell, Andrew D.

AU - Gallagher, Patrick G.

AU - Steinberg, Martin H.

AU - Forget, Bernard G.

AU - Chui, David H.K.

PY - 2016/3/1

Y1 - 2016/3/1

N2 - Two 21-year old dizygotic twin men of Iraqi descent were homozygous for HBB codon 8, deletion of two nucleotides (-AA) frame-shift β0-thalassaemia mutation (FSC8; HBB:c25_26delAA). Both were clinically well, had splenomegaly, and were never transfused. They had mild microcytic anaemia (Hb 120-130 g/l) and 98% of their haemoglobin was fetal haemoglobin (HbF). Both were carriers of Hph α-thalassaemia mutation. On the three major HbF quantitative trait loci (QTL), the twins were homozygous for G>A HBG2 Xmn1 site at single nucleotide polymorphism (SNP) rs7482144, homozygous for 3-bp deletion HBS1L-MYB intergenic polymorphism (HMIP) at rs66650371, and heterozygous for the A>C BCL11A intron 2 polymorphism at rs766432. These findings were compared with those found in 22 other FSC8 homozygote patients: four presented with thalassaemia intermedia phenotype, and 18 were transfusion dependent. The inheritance of homozygosity for HMIP 3-bp deletion at rs66650371 and heterozygosity for Hph α-thalassaemia mutation was found in the twins and not found in any of the other 22 patients. Further studies are needed to uncover likely additional genetic variants that could contribute to the exceptionally high HbF levels and mild phenotype in these twins.

AB - Two 21-year old dizygotic twin men of Iraqi descent were homozygous for HBB codon 8, deletion of two nucleotides (-AA) frame-shift β0-thalassaemia mutation (FSC8; HBB:c25_26delAA). Both were clinically well, had splenomegaly, and were never transfused. They had mild microcytic anaemia (Hb 120-130 g/l) and 98% of their haemoglobin was fetal haemoglobin (HbF). Both were carriers of Hph α-thalassaemia mutation. On the three major HbF quantitative trait loci (QTL), the twins were homozygous for G>A HBG2 Xmn1 site at single nucleotide polymorphism (SNP) rs7482144, homozygous for 3-bp deletion HBS1L-MYB intergenic polymorphism (HMIP) at rs66650371, and heterozygous for the A>C BCL11A intron 2 polymorphism at rs766432. These findings were compared with those found in 22 other FSC8 homozygote patients: four presented with thalassaemia intermedia phenotype, and 18 were transfusion dependent. The inheritance of homozygosity for HMIP 3-bp deletion at rs66650371 and heterozygosity for Hph α-thalassaemia mutation was found in the twins and not found in any of the other 22 patients. Further studies are needed to uncover likely additional genetic variants that could contribute to the exceptionally high HbF levels and mild phenotype in these twins.

KW - Fetal haemoglobin

KW - HBS1L-MYB intergenic polymorphism

KW - HbF quantitative trait loci

KW - α-Thalassaemia

KW - β-Thalassaemia

UR - https://www.scopus.com/pages/publications/84960101241

U2 - 10.1111/bjh.13909

DO - 10.1111/bjh.13909

M3 - Article

C2 - 26771086

AN - SCOPUS:84960101241

SN - 0007-1048

VL - 172

SP - 958

EP - 965

JO - British Journal of Haematology

JF - British Journal of Haematology

IS - 6

ER -

The genetic basis of asymptomatic codon 8 frame-shift (HBB: C25_26delAA) β⁰-thalassaemia homozygotes

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Keywords

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