Similarity of DMD gene deletion and duplication in the Chinese patients compared to global populations

1744-9081-4-20 1744-9081 Research Similarity of DMD gene deletion and duplication in the Chinese patients compared to global populations Wang Xiaozhu wangzhu2242002@yahoo.com.cn Wang Zheng wzhengsn@yahoo.com.cn Yan Ming ym303@gmail.com Huang Shangzhi hangzhihuang_pumc@yahoo.com.cn Chen Tian-Jian tjchen@jaguar1.usouthal.edu Zhong Nanbert nanbert.zhong@omr.state.ny.us

Peking University Center of Medical Genetics, Peking University, Beijing, China

Department of Medical Genetics, Peking University Health Science Center, Peking University, Beijing, China

Department of Medical Genetics, Peking Union Medical College/Institute of Medical Sciences, Chinese Academy of Medical Sciences, Beijing, China

Department of Human Genetics, New York State Institute for Basic Research in Development Disabilities, Staten Island, New York, USA

Department of Medical Genetics, University of South Alabama, Mobile, Alabama, USA

Behavioral and Brain Functions 1744-9081 2008 4 1 20 http://www.behavioralandbrainfunctions.com/content/4/1/20 18445268 10.1186/1744-9081-4-20 12 2 2008 29 4 2008 29 4 2008 2008 Wang et al; licensee BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Abstract

Background

DNA deletion and duplication were determined as the major mutation underlying Duchenne muscular dystrophy (DMD) and Becker muscular dystrophy (BMD).

Method

Applying multiplex ligation-dependent probe amplification (MLPA), we have analyzed 179 unrelated DMD/BMD subjects from northern China.

Results

Seventy-three percent of the subjects were found having a deletion (66.25%) or duplication (6.25%). Exons 51–52 were detected as the most common fragment deleted in single-exon deletion, and the region of exons 45–50 was the most common exons deleted in multi-exon deletions. About 90% of DMD/BMD cases carry a small size deletion that involves 10 exons or less, 26.67% of which carry a single-exon deletion. Most of the smaller deletions resulted in an out-of-frame mutation. The most common exons deleted were determined to be between exon 48 and exon 52, with exon 50 was the model allele. Verifying single-exon deletion, one sample with a deletion of exon 53 that was initially observed from MLPA showed that there was a single base deletion that abolished the ligation site in MLPA. Confirmation of single-exon deletion is recommended to exclude single base deletion or mutation at the MLPA ligation site.

Conclusion

The frequency of deletion and duplication in northern China is similar to global ethnic populations.

Background

Duchenne muscular dystrophy (DMD) and its less severe allelic form Becker muscular dystrophy (BMD) are common X-linked recessive neuromuscular degeneration diseases 12. The incidence of DMD is 1/3500 and BMD is 1/18,000 in male living births, respectively 34. They both are caused by genetic defects of the dystrophin gene, which is located at Xq21.2, spanning 2.4 Mb 56. The dystrophin gene consists of 79 exons and encodes a 14.6 kb mRNA, which is expressed in skeleton, muscles and brain 7. Deletions, duplications and point mutations have been reported in most exons of this gene. There were two deletion hot-spot regions, one is located at the 5' exons 2–20 and the other, located between exons 44–53 89. Mutations affecting open-reading frame (ORF), due to a frameshift, may result in an aberrantly spliced mRNA and generate a truncated, nonfunctional dystrophin protein that usually gives rise to the DMD/BMD phenotypes. However, mutations not affecting the ORF may produce a semi-functional dystrophin protein and usually correlate with mild phenotypes 10. Levels of dystrophin protein in DMD are very low (<3% of normal) or absent, however, BMD patients have 10–40% of the normal amount of dystrophin with an abnormal molecular weight 1112. About 65% of cases are caused by deletion 8913, approximately 5% by duplication 914 and the remaining is point mutation of the dystrophin gene 15. Due to no effective treatment available for DMD/BMD, presently an accurate genetic diagnosis may offer prenatal diagnosis for the familial DMD/BMD although about one-third of mutations are de novo 16. Although the frequency of complex rearrangement was reported as high as 4% 17, usually complex rearrangement is considered as a rare condition 181920 that includes double deletion 17 and non-contiguous duplications 212223.

In this study, we have analyzed a subset of DMD/BMD patients from Northern China.

Methods

Subjects

A total number of 179 unrelated patients in northern China were studied. There were 160 affected male probands and 19 females who had an affected son clinically diagnosed as DMD/BMD. This study was approved by the Institutional Ethic Committee and informed consent was obtained from all participants.

Multiplex ligation-dependent probe amplification (MLPA)

MLPA is a reliable technology for quantitative analysis of the copy number in clinical diagnosis of genetic diseases 24. It has the capability of detecting either large or small genomic deletions or duplications 2025. An MLPA kit with probes of P034 and P035 for detecting deletion and/or duplication of the DMD gene was purchased commercially from MRC Holland (Amsterdam, Netherlands). Procedures were following the manufacturer's instruction. Ligation and amplification were carried out with an ABI 9800 Thermal Cycler. The PCR conditions were 35 cycles at 95°C for 30s, 60°C for 30s, and 72°C for 60s; followed by a final incubation at 72°C for 20 min.

The PCR products were separated by capillary electrophoresis in an ABI 310 Genetic Analyzer with Genescan 3.7 (Applied Biosystems, Foster City, California) software. The raw data was analyzed by Genescan Analysis 3.7 software. The peaks obtained after the analysis of the row data (Fig. 1A) could be distinguished and assigned to specific exons on the basis of their different lengths representing the variability of their stuffer sequences. Peak area of raw data can be also exported into a Microsoft excel spreadsheet program (Fig. 1B), which normalizes each peak to that of a known normal control (Fig. 1, 1). Peaks derived from DMD/BMD patients (Fig. 1, 2–5) that vary more than 20% from the normal should be flagged for review. If a deletion of a single exon was observed, conventional PCR and DNA sequencing analysis of the specific region embedding the deleted exon was performed to verify the deletion 2021.

Figure 1

MLPA results were selected from a normal control (1), a multi-exon deletion (2), a multi-exon duplication (3), a single-exon duplication (4), and a single-exon deletion (5)

MLPA results were selected from a normal control (1), a multi-exon deletion (2), a multi-exon duplication (3), a single-exon duplication (4), and a single-exon deletion (5). Raw data are shown on the left panels (A). Each peak represents one exon of the dystrophin gene. Arrow(s) indicate missing signals representing deleted exon(s). The corresponding relative peak area (RPA) ratios, after statistical analysis, are shown on the right panels (B), in which each bar represents the RPA ratio compared to the mean of two male control samples.

Results

Detection of DMD gene deletion with MLPA

Among 160 male probands, 106 were found to have deletions, accounting for 66.25% of male patients analyzed. Among 19 females who had an affected boy but without previous genetic confirmation, 14 with exonic deletion were detected, which brought the deletion rate to 67.04% (120/179). Duplication mutation was identified from 10 (16.95%) of the remaining 59 people (54 male patients and 5 female carriers) who had no deletion identified. Totally, 130 of 179 (72.63%) were found to have mutations (Table 1).

Table 1

Mutation Detected in Dystrophin Gene

Size of deletion or duplication

Independent cases (N = 120)

Distribution (%)

Exon deleted or duplicated

Fragment deleted or duplicated Δ

IF/OF OF

Minimal deletion/duplication (bp)

1 exon (n = 32)

0.83

DelEX07

c.531-?*_649+?*del

118

0.83

DelEX17

c.1993-?_2168+?del

175

1.67

DelEX18

c.2169-?_2292+?del

123

0.83

DelEX19

c.2293-?_2380+?del

0.83

DelEX35

c.4846-?_5025+?del

179

1.67

DelEX43

c.6118-?_6290+?del

172

0.83

DelEX44

c.6291-?_6438+?del

147

4.17

DelEX45

c.6439-?_6614+?del

175

1.67

DelEX50

c.7201-?_7309+?del

108

DelEX51

c.7310-?_7542+?del

232

DelEX52

c.7543-?_7660+?del

117

1.67

DelEX53*

c.7661-?_7872+?del

211

1.67

DelEX54

c.7873-?_8027+?del

154

2 exons (n = 10)

0.83

DelEX10-11

c.961-?_1331+?del

1020

0.83

DelEX42-43

c.5923-?_6290+?del

22747

1.67

DelEX46-47

c.6615-?_6912+?del

2631

3.33

DelEX48-49

c.6913-?_7200+?del

38655

1.67

DelEX49-50

c.7099-?_7309+?del

104

3 exons (n = 17)

0.83

DelEX03-05

c.94-?_357+?del

26525

0.83

DelEX46-48

c.6615-?_7098+?del

57036

DelEX48-50

c.6913-?_7309+?del

55398

1.67

DelEX50-52

c.7201-?_7660+?del

90452

2.5

DelEX51-53

c.7310-?_7872+?del

94817

0.83

DelEX52-54

c.7543-?_8027+?del

71758

1.67

DelEX53-55

c.7661-?_8217+?del

51913

4 exons (n = 9)

0.83

DelEX10-13

c.961-?_1602+?del

49395

0.83

DelEX22-25

c.2804-?_3432+?del

8870

2.5

DelEX45-48

c.6439-?_7098+?del

93323

0.83

DelEX46-49

c.6615-?_7200+?del

95509

1.67

DelEX49-52

c.7099-?_7660+?del

107011

0.83

DelEX50-53

c.7201-?_7872+?del

140708

5 exons (n = 12)

1.67

DelEX03-07

c.94-?_649+?del

40327

0.83

DelEX13-17

c.1483-?_2168+?del

50717

0.83

DelEX17-21

c.1993-?_2803+?del

60415

2.5

DelEX46-50

c.6615-?_7309+?del

102252

2.5

DelEX48-52

c.6913-?_7660+?del

145742

0.83

DelEX50-54

c.7201-?_8027+?del

162093

0.83

DelEX51-55

c.7310-?_8217+?del

146519

6 exons (n = 13)

5.83

DelEX45-50

c.6439-?_7309+?del

148539

0.83

DelEX46-51

c.6615-?_7542+?del

158627

0.83

DelEX47-52

c.6763-?_7660+?del

200114

3.33

DelEX49-54

c.7099-?_8027+?del

178832

7 exons (n = 2)

1.67

DelEX46-52

c.6615-?_7660+?del

202596

8 exons (n = 5)

3.33

DelEX45-52

c.6439-?_7660+?del

238883

0.83

DelEX46-53

c.6615-?_7872+?del

252852

10 exons (n = 6)

2.5

DelEX45-54

c.6439-?_8027+?del

310524

2.5

DelEX46-55

c.6615-?_8217+?del

304554

11 exons (n = 3)

2.5

DelEX45-55

c.6439-?_8217+?del

340841

12 exons (n = 1)

0.83

DelEX31-42

c.4234-?_6117+?del

80099

16 exons (n = 1)

0.83

DelEX8-23

c.650-?_3162+?del

230795

20 exons (n = 1)

0.83

DelEX11-30

c.1150-?_4233+?del

232561

27 exons (n = 1)

0.83

DelEX3-29

c.832-?_3162+?del

411579

30 exons (n = 1)

0.83

DelEX10-39

c.961-?_5586+?del

299209

35 exons (n = 1)

0.83

DelEX10-44

c.961-?_6438+?del

428236

37 exons (n = 1)

0.83

DelEx8-44

c.650-?_6438+?del

482377

39 exons (n = 1)

0.83

DelEX3-41

c.94-?_5922+?del

507720

41 exons (n = 1)

0.83

DelEX3-43

c.94-?_6290+?del

562291

42 exons (n = 2)

1.67

DelEX3-44

c.94-?_6438+?del

632904

Dup1 exons

0.83

DupEX45

c.6439?_6614+?dup

175

Dup3 exons

0.83

DupEX48-50

c.6913?_7309+?dup

55398

Dup5 exons

0.83

DupEX3-7

c.94-?_649+?dup

40327

Dup11 exons

0.83

DupEX64-74

53678

Dup14 exons

0.83

DupEX3-16

c.94-?_1992+?dup

284118

Dup21 exons

0.83

DupEX54-74

c.7873-?_10553+?dup

488701

Dup27 exons

0.83

DupEX8-34

c.650-?_4845+?dup

318783

Dup29 exons

0.83

DupEX13-41

c.1483-?_5922+?dup

253776

Dup37 exons

0.83

DupEX8-44

c.650-?_6438+?dup

482377

Dup41 exons

0.83

DupEX3-43

c.94-?_6290+?dup

562291

Δ: data were obtained through online search from [26].

?: the actual breakpoint is unknown.

*: DNA sequencing analysis determined that this single exon deletion is due to a single base pair deletion (Fig. 2).

IF/OF: in frame or out-of-frame.

Detection of single-exon deletion may result from 1-bp deletion

When a single-exon deletion was observed, DNA sequencing would be applied for verification. Among 32 DNA samples with single-exon deletion, DNA sequencing observed a 1-bp deletion (NM_004006.1, c.8027delG) in one case that had a deletion of exon 53 detected by initial MLPA. This 1-bp deletion (Fig. 2) was located precisely at the ligation site and destroyed the ligation that resulted in failure of amplification of the probes in MLPA.

Figure 2

Sequencing analyses to validate single-exon deletion

Sequencing analyses to validate single-exon deletion. One sample detected as a single-exon deletion of exon 53 was found that the deletion was resulted from a single base pair deletion, rather than an entire exon deletion. This single base pair deletion abolished the ligation of the probe.

Deletion of small fragment is predominant in DMD gene

Analyses of 106 males and 14 females (Table 1) showed that 26.67% (29 males and 3 females) of deletions involved a single-exon; 14.17% (15 males and 2 females) exhibited 3-exon deletion; 10.83% (12 males and 1 female) had 5- or 6-exon deletion, 8.33% (10 males) had 2-exon deletion, 7.50% (5 males and 4 females) showed 4-exon deletion, 5.0% (6 males) had 10-exon deletion, 4.17% (5 males) had 8-exon deletion, and 1.67% (2 males) had 7-exon deletion. Our results showed that deletion of six exons and smaller accounts for 77.5% (93/120). To combine all deletions smaller than 10 exons, this group deletion may account for 88.33% (106/120) of patients and carriers.

Duplication detected in this study involved a large fragment

Ten patients with duplication were identified. Most of the duplications involved large fragments, among which six spun 11 to 41 exons. Eight duplications involved previously identified 3' region. A large 21-exon duplication was beyond the 3' hot-spot region that has reached exon 74. Only three duplications in this study were found to involve small fragment.

Exons 48–52 were the most common region deleted

Analysis of the single-exon deletion among the 32 (29 males, three females) patients showed that both exons 51 and 52 were the most common exons deleted, accounting for 18.75% (6/32) respectively, followed by exon 45 (15.63%). Single-exon deletion was not found in exons 1–6, 8–16, 20–34, 36–42, 46–49, and 55–79. Among the 88 cases with multiple exons (multi-exon), deletion of six exons in 45–50 were the most common (7.95%), followed by deletion of three exons in 48–50 (6.82%), and then two exons in 48–49 and eight exons in 45–52. When the frequency of deletion for individual exon of dystrophin gene was considered, the most common deleted was exon 50, followed by exon 49 (6.54%), then exon 48 (6.01%), and exons 51 (5.10%). Deletion of exons from 45 to 54 accounts for 50.16%. No deletion was found in either 5' end exons 1–2 or 3' end exons 56–79 (Fig. 3).

Figure 3

Frequency of DMD gene mutations showed that deletion of exon 50 is the most common in the DMD gene deletions, which brought the exon 50 as the model allele in the DMD gene deletion

Frequency of DMD gene mutations showed that deletion of exon 50 is the most common in the DMD gene deletions, which brought the exon 50 as the model allele in the DMD gene deletion. There is no specific peak showing a model duplicated exon.

Out-of-frame mutation is predominant in DMD/BMD

It has been considered that clinical severity is correlated to in frame or out-of-frame deletion of the dystrophine gene 26. An interesting result we noticed from this study was that for smaller deletions, they usually resulted in out-of-frame mutations. Among 106 small deletion that involved ten or less exons, there were only 11 cases that carried in-frame but 89.62% had out-of-frame. However, among 14 larger deletions, there were 11 (78.57%) cases had in-frame mutations. This data suggested that out-of-frame mutations in smaller deletion cases account for the majority of DMD mutations, which likely resulted in a severe phenotype. Among five larger duplications, there was only one that was an in-frame mutation while the others were out-of-frame mutations, and there was no in-frame mutation in two small duplications. Overall, 81.53% of duplications were out-of-frame. Correlating each DNA sample with its clinical phenotypes would be idea for drawing a clearer picture. A regret of this study, unfortunately, was that the clinical information had been incomplete which made us unable to perform an analysis on genotype-phenotype correlation. We encourage to perform a genotype-phenotype study with a larger cohort in order to draw a better clue.

Discussion

Several studies have shown that MLPA were useful in detecting mutation quantitatively, not only for deletions but also duplications and female carriers in the DMD gene 2025272829. We applied MLPA in a subset of DMD/BMD patients in northern China. Our results indicated that 66.25% (106/160) of our patients carry deletion and 6.25% (10/160) patients had a duplication, which brought the sensitivity of detecting DNA rearrangement up to 72.5%. In addition, MLPA may present higher sensitivity. In this study, three patients who had negative results in their previous DNA testing by multiplex PCR (data not shown) were identified. Furthermore, an advantage of employing MLPA in clinical genetic testing is that it is capable of identifying female carriers, as we have demonstrated among 14 out of 19 females who came to our prenatal clinics. Certainly, MLPA should be considered as the initial test for the clinically suspected DMD/BMD patients as well as for women who have a DMD/BMD family history, as suggested previously 29, to provide both confirmation of genetic defects on DMD gene and better genetic counseling.

Exons 2–20 and exons 44–53 had been previously reported as the two-hotspot regions 89. In this study, we have analyzed the distribution of individual exons regarding their frequency of deletion or duplication (Fig. 4). Our data indicates that the deletion occurs at exons 45 to 55 accounting for 47.67%, followed by exons 21–44 (26.67%) and exons 1–20 (23.66%). If both deletions and duplications are counted together, the most frequent mutant region occurs within exons 45–55 (41.06%) in the DMD gene, followed by exons 21–44 (30.43%), exons 1–20 (25.32%) and exons 56–79 (3.19%). We found the most common region in our study is the exons 45–55, and the least common region is the exons 56–79. These data are in agreement with other global populations 26. We have noticed that the frequency of duplication is more than 20% and it appears there is no model peak of deletion in Taiwan (Fig. 4) 212227303132. As well, the deletion rate in Hong Kong 31 showed difference from the northern Chinese. We hypothesize that the frequency of deletion is different in variant regions of China, and we propose that further investigation with molecular screening of deletion (and duplication) should be pursued among newborns in China. The pattern of duplication did not show significant difference among the global variant populations (Fig. 4).

Figure 4

Comparison of exon deletion (A) and duplication (B) among global populations

Comparison of exon deletion (A) and duplication (B) among global populations. All these data showed that exons 45–55 are the most frequent deletion region of DMD gene. Deletion and duplication were not common in region of exons 56–79, although the data may derive from variant methodology (MLPA for Hong Kong, Taiwan, Denmark, Australia, and the current study; quantitative multiplex PCR for Canada; and multiplex PCR and Southern blotting for Japan and USA).

The structure of introns of dystrophin gene determines the breakpoint that is responsible for the deletion 33. There were many repeated sequences in introns of dystrophin gene which resulted in many breakpoints. For example, in intron 44 there were 13 breakpoints resulted in the hot-spot deletion region 34. The repeated sequences included direct repeated sequence, inverted repeat sequence and homology sequence. It was reported that 22 repeated sequences had been found in intron 51 and intron 52, which was a possible reason for the high frequency of single-exon deletion at exon 51 35. We believe this might be the same case for the most common deletion at exon 50.

Recently, White et al 25 reported that as high as 87% of duplications can be detected among three subsets of selected DMD/BMD cases, among which no deletion or point mutation had been found. In this study, duplication was only detected in 18.51% of the cases where no deletion could be detected. This lower rate possibly resulted from either our small size of samples or a high rate of point mutation, which should be further investigated. To combine the rates of duplication with deletion, we estimate that a point mutation might account for 20–28% of our cases. In addition, the duplications in our cases mainly involved a larger fragment; however, among 118 cases of the reported duplications 25, there were only 12 cases where the duplication was more than 20 exons.

In summary, we have applied MLPA to detect DNA rearrangements of deletions and duplications among DMD/BMD male patients and female potential carriers. We have determined that deletions and duplications were 72.5% of our samples. We observed that the majority of deletions was small in size that the number of deleted exons was less than 10 but duplications usually involved larger sizes. Finally, we determined that the most common region of DMD gene rearrangement is between exons 45 and 55 and the 5' hotspot region was not a hotspot region in our study.

Conclusion

MLPA is an effective and cost effective technique to detect a large number of samples. In our study, we found the frequency of deletion/duplication of DMD in the northern China is similar to other population. We recommend that MLPA should be applied as the first line for clinical molecular testing for DMD/BMD.

List of abbreviations

DMD: Duchenne muscular dystrophy; BMD: Becker muscular dystrophy; MLPA: multiplex ligation-dependent probes amplification; PCR: ploymerase chain reaction.

Competing interests

The authors declare that they have no competing interests.

Authors' contributions

XZW conducted experiments, analyzed and interpreted results, and drafted the manuscript. ZW assisted in data analysis and manuscript drafting. SZH participated in DNA sample collection. MY assisted in operating fragment analysis with sequencer ABI310. TJC directed raw data analysis. NZ conceived of the project, designed, supervised, and coordinated the entire studies, and is responsible for the final edition of the manuscript and approval of the submission. All authors read and approved the final manuscript.

Acknowledgements

This project was partially funded by the Chinese Ministry of Education (985-2-035-39), the National Nature Science Fund of China (NSFC2004BA720A03 and 30671157), "973" Project (2007CB511902) and the New York State Office of Mental Retardation and Developmental Disabilities (NYS OMRDD). We would like to thank all participants in this study.

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