Unusual Rearrangement of the α-Globin Gene Cluster Containing Both the ?α3.7 and αααanti-4.2 Crossover Junctions: Clinical Diagnostic Implications and Possible Mechanisms

Amy Y.Y. Chan; Edmond S.K. Ma; Li-Chong Chan; Samuel S. Chong; Wen Wang

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Unusual Rearrangement of the α-Globin Gene Cluster Containing Both the ?α3.7 and αααanti-4.2 Crossover Junctions: Clinical Diagnostic Implications and Possible Mechanisms

机译：包含αα3.7和αααanti-4.2交叉连接的α-球蛋白基因簇的异常重排：临床诊断意义和可能的机制。

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Misalignment of the homologous regions of the α-globin gene cluster and unequal crossover during meiosis produce single α-globin gene deletions (?α) and reciprocal α-globin gene triplications (ααα). Further unequal crossover of such recombinant alleles with wild-type alleles may produce more complex derivative alleles, such as quadruplicated alleles (1)(2)(3). Complex crossover events producing “patchwork” genes have also been reported at the human α- and β-globin gene cluster (4)(5)(6). In this report, we describe the identification of a novel rearrangement of the α-globin gene cluster containing both the ?α3.7 and αααanti-4.2 crossover junctions. This allele was identified in 2 unrelated individuals and a parent in the course of screening by Southern analysis of patients with β-thalassemia major and minor for α-globin gene deletions (Table 1? ). For patient 1, a routine α-globin gene configuration Southern analysis was performed to screen for the presence of the ?-SEA α-thalassemia deletion, a common amelioration factor of severe β-thalassemia (7). In the case of patient 2, Southern analysis was performed to rule out the presence of the ?-SEA α-thalassemia deletion, because hemoglobin H inclusion bodies typically present in α-thalassemia are absent when there is concurrent β-thalassemia (8).Southern analysis was performed by hybridizing [32P]dATP-labeled α- or ζ-globin gene probes to Bam HI- or Bgl II-digested genomic DNA. With an α-globin probe, an αααanti-4.2 triplication contributes an 18.2-kb hybridizing Bam HI band and 16.8- and 7.4-kb Bgl II bands, whereas a ?α3.7 deletion contributes a 10.3-kb Bam HI band and a 16.3-kb Bgl II band. With a ζ-globin probe, both the αααanti-4.2 and ?α3.7 alleles contribute 5.9-kb and 10.8/11.3-kb Bam HI bands, whereas αααanti-4.2 contributes 11.3/12.6-kb and 16.8-kb Bgl II bands, and ?α3.7 contributes 11.3/12.6-kb …

机译：α-珠蛋白基因簇的同源区域的错位和减数分裂过程中的不相等交换会产生单个α-珠蛋白基因缺失（？α）和相互的α-珠蛋白基因三倍重复（ααα）。此类重组等位基因与野生型等位基因的进一步不平等交换可能会产生更复杂的衍生等位基因，例如四重等位基因（1）（2）（3）。在人α-和β-珠蛋白基因簇上也已经报道了产生“拼凑”基因的复杂交换事件（4）（5）（6）。在本报告中，我们描述了包含αα3.7和αααanti-4.2交叉连接的α-珠蛋白基因簇的新型重排的鉴定。通过Southern分析对患有β和地中海贫血的大，小地中海贫血患者的α-珠蛋白基因缺失进行筛选，在2名无关个体和一名父母中鉴定出该等位基因（表1）。对于患者1，进行常规的α-珠蛋白基因构型Southern分析，以筛选是否存在β-SEAα-地中海贫血缺失，这是严重的β-地中海贫血的常见缓解因素（7）。在患者2的情况下，进行了Southern分析以排除是否存在β-SEAα-地中海贫血，因为当同时存在β-地中海贫血时，不存在通常在α-地中海贫血中存在的血红蛋白H包涵体（8）。通过将[32P] dATP标记的α-或ζ-珠蛋白基因探针与Bam HI-或Bgl II消化的基因组DNA杂交，进行Southern分析。使用α-球蛋白探针，αααanti-4.2重复贡献了18.2kb的杂交Bam HI谱带以及16.8和7.4kb的Bgl II谱带，而αα3.7缺失则贡献了10.3kb的Bam HI谱带和16.3kb。 -kb Bgl II带。使用ζ珠蛋白探针，αααanti-4.2和βα3.7等位基因均贡献5.9-kb和10.8 / 11.3-kb Bam HI谱带，而αααanti-4.2贡献11.3 / 12.6-kb和16.8-kb Bgl II谱带，而αα3.7贡献11.3 / 12.6-kb…

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《Clinical Chemistry: Journal of the American Association for Clinical Chemists》 |2005年第11期|共页
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Amy Y.Y. Chan; Edmond S.K. Ma; Li-Chong Chan; Samuel S. Chong; Wen Wang;
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1. Single-Tube Multiplex-PCR Screen for Anti-3.7 and Anti-4.2 α-Globin Gene Triplications [J] . Amy Y.Y. Chan, David H.K. Chui, Edmond S.K. Ma, Clinical Chemistry: Journal of the American Association for Clinical Chemists . 2003,第10期

机译：单管多重PCR筛选抗3.7和抗4.2α-球蛋白基因重复
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5. CLONING AND SEQUENCE ANALYSIS OF THE EMBRYONIC ALPHA- AND BETA-TYPE GOAT GLOBIN GENES: EVOLUTIONARY ANALYSIS OF THE GOAT ALPHA AND BETA GLOBIN GENE CLUSTERS. [D] . WERNKE, SUZANNE MARIE. 1987

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7. Unusual rearrangement of the α-globin gene cluster containing both the -α3.7 and αααanti-4.2 crossover junctions: Clinical diagnostic implications and possible mechanisms [O] . Chan, LC, Chong, SS, Wang, W, 2005

机译：包含-α3.7和αααanti-4.2交叉连接的α-珠蛋白基因簇的异常重排：临床诊断意义和可能的机制

Unusual Rearrangement of the α-Globin Gene Cluster Containing Both the ?α3.7 and αααanti-4.2 Crossover Junctions: Clinical Diagnostic Implications and Possible Mechanisms

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