Your search keyword '"Yi-xin, Zhan"' showing total 4 results

1. Study on preimplantation genetic diagnosis and follow-up for Duchenne muscular dystrophy

Author

Juan YANG, Hui-fang XIE, Ji-qing CAO, Hui ZHENG, Can-quan ZHOU, Zhen-hua LIU, Yu-ling ZHU, Yi-xin ZHAN, Xiao-ting SHEN, Ya-qin LI, and Cheng ZHANG

Subjects

Muscular dystrophy, Duchenne, Preimplantation diagnosis, Follow-up studies, Neurology. Diseases of the nervous system, RC346-429

Abstract

Objective To carry out preimplantation genetic diagnosis (PGD) for Duchenne muscular dystrophy (DMD) carrier, so as to prevent the birth of affected infants with DMD. Methods One DMD gene carrier with a deletion of exon 10-30 received fertilization with intracytoplasmic sperm injection (ICSI). DMD gene and haplotype were tested after amplification of genome DNA in multiple displacement amplification (MDA), then healthy embryos were transferred to uterus according to the genetic results. Genetic testing was made in second trimester and after delivery, and also periodic follow-up was made for over 3 years. Results The second cycle of PGD was successful, and a total of 14 single blastomeres obtained from 7 embryos were used for genetic analysis. The success rate of MDA was 13/14, and the allele dropout rate was 18.75% (18/96). Three unaffected embryos were transferred, resulting in twin pregnancy. One healthy boy and one healthy girl were born in cesarean section at the pregnant week of 35. Genetic results on DNA from both amniotic fluid at 16 weeks of gestation and peripheral blood after birth were normal. During the 3-year follow-up, both 2 infants were normal in growth and development, motor function and dynamic monitor of serum creatine kinase (CK). Conclusions Preimplantation genetic diagnosis can help DMD gene carrier give birth to healthy infants, and these infants have normal development. DOI: 10.3969/j.issn.1672-6731.2015.06.008

Published

2015

2. Clinical features and genetic analysis of 7 patients with late-onset glycogen storage disease typeⅡ

Author

Juan YANG, Ji-qing CAO, Zhen-hua LIU, Yi-xin ZHAN, Ying-yin LIANG, Gui-ling MO, Ya-qin LI, Yi-ming SUN, Min-zi LI, Jing LI, and Cheng ZHANG

Subjects

Glycogen storage disease type Ⅱ, Alpha-glucosidases, Genes, Mutation, Neurology. Diseases of the nervous system, RC346-429

Abstract

Objective In order to make a well understanding on glycogen storage disease typeⅡ (GSDⅡ), this paper explored clinical features and genetic analysis of 7 patients with late-onset glycogen storage disease typeⅡ. Methods Clinical data of 7 patients with late-onset glycogen storage disease type Ⅱ were collected and acid α-glucosidase (GAA) gene sequencing was performed. Results Seven patients who belong to 4 families were at the age of 13-31 years old. The first symptom occurred at 6-17 years old, and the age at first and definitive diagnosis was 12-29 and 12-30 years old, respectively. The initial symptoms were mostly related to limb girdle muscular atrophy and weakness. The GAA activity ranged from 0 to 5.27 nmol/(mg·h). Sequencing analysis revealed 14 sequence variants, including 2 novel mutations (Q81X and c.1355_1356delC), 2 pseudodeficiency alleles (G576S and E689K), 8 polymorphic loci, and 2 sequence variants previously related with glycogen storage disease type Ⅱ pathogenesis (W746C and D645E). Conclusions Due to the apparently diagnostic delay, prognosis of patients with glycogen storage disease type Ⅱ could be improved by increasing the clinician's awareness of the disease. It is essential to combine clinical history with GAA activity and GAA gene analysis when we make a definitive diagnosis of glycogen storage disease type Ⅱ. Though siblings share the same set of GAA mutations, the phenotype regarding the course and severity of disease could vary substantially. doi: 10.3969/j.issn.1672-6731.2014.05.008

Published

2014

3. Detection of α-globin gene deletion and duplication using quantitative multiplex PCR of short fluorescent fragments

Author

Gui Ling Mo, Wenli Feng, Yi Xin Zhan, Ya Juan Li, Zong Ping Mo, Zheng Yu Zeng, Chaohui Hu, Chang Shun Yu, and Wei Xi Cao

Subjects

Genetics, Biochemistry (medical), Clinical Biochemistry, DNA Mutational Analysis, Reproducibility of Results, General Medicine, Biology, Molecular biology, Polymerase Chain Reaction, law.invention, alpha-Globins, alpha-Thalassemia, law, hemic and lymphatic diseases, Gene Duplication, Gene duplication, Multiplex polymerase chain reaction, Multiplex, Copy-number variation, Multiplex ligation-dependent probe amplification, Allele, Gene, Polymerase chain reaction, Gene Deletion, Fluorescent Dyes

Abstract

Background The aim of this study was to establish a sensitive method that can detect the presence of not only the common but also the unusual or unknown α-globin gene deletions for screening of α-thalassemia. We used quantitative multiplex PCR of short fluorescent fragments (QMPSF) for the α-globin genes (HBA) to screen α-thalassemia deletions. Methods We set up and validated HBA-QMPSF using 50 negative and 100 positive controls of deletional α-thalassemia. To evaluate its ability to detect the presence of the common and unusual or unknown α-globin gene deletions, 579 unrelated samples were simultaneously analyzed using this assay and multiplex Gap polymerase chain reaction (Gap-PCR). The inconsistent results were further confirmed by multiplex ligation-dependent probe amplification (MLPA). Results HBA-QMPSF was capable of detecting α-globin gene deletions with an acceptable variability as shown by mean values (SD) of allele dosage for the heterozygous deleted control obtained from intra- and inter-experimental replicates [0.63 (0.01) and 0.61 (0.03)]. In 572 out of the 579 unrelated subjects, HBA-QMPSF and multiplex Gap-PCR gave consistent results. In seven cases which were finally proved to be composed of one rare deletion--Thai/-α3.7, one novel deletion--SEA/-α2.8, four αααanti3.7/αα and one αααanti4.2/αα triplications, HBA-QMPSF showed deletion or duplication in the α-globin gene while multiplex Gap-PCR failed to give the correct diagnosis. Conclusions HBA-QMPSF is able to detect the presence of the common and unusual or unknown α-thalassemia deletions and duplications. It can be used as an initial screening test for α-thalassemia caused by HBA gene copy number alteration.

Published

2011

4. [Study on clinical manifestation, genotype and genetic characteristics of two Kennedy disease pedigrees]

Author

Juan, Yang, Cheng, Zhang, Zhao-hui, Hu, Yi-xin, Zhan, Ji-qing, Cao, and Hui, Ren

Subjects

Adult, Male, Adolescent, Base Sequence, Genotype, Electromyography, Biopsy, Muscles, Molecular Sequence Data, Bulbo-Spinal Atrophy, X-Linked, Exons, Middle Aged, Pedigree, Young Adult, Receptors, Androgen, Child, Preschool, Humans, Female, Child, Aged, Ultrasonography

Abstract

To investigate the clinical manifestations, genotypes, and genetic characteristics of two pedigrees with Kennedy disease.The clinical data of the patients from two Kennedy disease families were collected. The numbers of trinucleotide CAG repeats in exon 1 of the androgen receptor gene were determined by DNA sequencing and repeat fragment analysis.Family A was composed of 58 individuals in 4 generations. The proband had onset at 39 years old. There were two Kennedy disease patients in family B which included 61 individuals in 5 generations. The two patients had onset at 39 and 41 years old, respectively. All the three patients displayed limbs and bulbar muscular weakness because of the damage of lower motor neurons. They had androgen insensitivity syndrome in common, and showed mild or moderate increase in serum creatine kinase level. The electromyogram showed wild damage in anterior horn of spinal cord. Muscle biopsy displayed neurogenic muscular atrophy. The numbers of the CAG repeat expansion in the androgen receptor gene of the three patients were 49, 48, and 47, respectively. X-linked recessive mode of inheritance was demonstrated by pedigree analysis in the two families.Kennedy disease usually occurs in mid-adulthood man. The clinical features are the weakness and wasting of limbs and bulbar muscles. Genetic analysis contributes to diagnosis and identification of carriers, and is beneficial to genetic counseling and prenatal diagnosis.

Published

2010