Your search keyword '"WANG Jun-ling"' showing total 6 results

1. Paroxysmal kinesigenic dyskinesia: Clinical and genetic analyses of 110 patients.

Author

Huang XJ, Wang T, Wang JL, Liu XL, Che XQ, Li J, Mao X, Zhang M, Bi GH, Wu L, Zhang Y, Wang JY, Shen JY, Tang BS, Cao L, and Chen SD

Subjects

Adolescent, Adult, Age of Onset, Child, Child, Preschool, Chorea etiology, Chorea physiopathology, Dystonia complications, Dystonia etiology, Dystonia physiopathology, Female, Genetic Association Studies, Homozygote, Humans, Infant, Male, Mutation, Severity of Illness Index, Time Factors, Uniparental Disomy, Young Adult, Chorea genetics, Dystonia genetics, Membrane Proteins genetics, Nerve Tissue Proteins genetics

Abstract

Objective: We aimed to investigate the clinical and genetic features of paroxysmal kinesigenic dyskinesia (PKD) in a large population and to analyze the genotype-phenotype correlation of PKD., Methods: We analyzed clinical manifestations and conducted PRRT2 screening in 110 patients with PKD. Clinical data were compared between 91 probands with and without PRRT2 mutations., Results: Among the enrolled participants (45 from 26 families, 65 sporadic cases), 8 PRRT2 mutations were detected in 20 PKD families (76.9%) and 14 sporadic cases (21.5%), accounting for 37.4% (34/91) of the study population. Five mutations (c.649dupC, c.649delC, c.487C>T, c.573dupT, c.796C>T) were already reported, while 3 mutations (c.787C>T, c.797G>A, c.931C>T) were undocumented. A patient harboring a homozygous c.931C>T mutation was shown to have inherited the mutation via uniparental disomy. Compared with non-PRRT2 mutation carriers, the PRRT2 mutation carriers were younger at onset, experienced longer attacks, and tended to present with complicated PKD, combined phenotypes of dystonia and chorea, and a positive family history. A good response was shown in 98.4% of the patients prescribed with carbamazepine., Conclusions: PRRT2 mutations are common in patients with PKD and are significantly associated with an earlier age at onset, longer duration of attacks, a complicated form of PKD, combined phenotypes of dystonia and chorea, and a tendency for a family history of PKD. A patient with uniparental disomy resulting in a homozygous c.931C>T mutation is identified in the present study. Carbamazepine is the first-choice drug for patients with PKD, but an individualized treatment regimen should be developed., (© 2015 American Academy of Neurology.)

Published

2015

2. Mutation analysis of PRRT2 in two Chinese BFIS families and nomenclature of PRRT2 related paroxysmal diseases.

Author

Wang JL, Mao X, Hu ZM, Li JD, Li N, Guo JF, Jiang H, Shen L, Li J, Shi YT, Xia K, Liu JY, Liao WP, and Tang BS

Subjects

Dystonia, Female, Genetic Linkage, Genetic Predisposition to Disease genetics, Humans, Male, Mutation, Pedigree, Vault Ribonucleoprotein Particles genetics, Asian People genetics, Chorea genetics, Dyskinesias genetics, Epilepsy, Benign Neonatal genetics, Membrane Proteins genetics, Nerve Tissue Proteins genetics, Seizures genetics

Abstract

Benign familial infantile seizure (BFIS) and paroxysmal kinesigenic dyskinesia (PKD) are autosomal-dominant inherited self-limited neurological disorders. BFIS is characterized by clusters of epileptic seizures in infancy while, in some cases, infantile seizures and adolescent-onset paroxysmal kinesigenic choreoathetosis co-occurred, which is called infantile convulsions and choreoathetosis (ICCA) syndrome. We and other researchers have reported the proline-rich transmembrane protein 2 (PRRT2) as the causative gene of PKD. We and our collaborators also identified PRRT2 mutations in ICCA and other phenotypes. Here we collected two BFIS families of Chinese Han origin. The linkage analysis has mapped the BFIS-causing locus to 16p12.1-q12.2, where PRRT2 is located. We then performed mutation analysis of PRRT2 by direct sequencing and identified c.649-650insC mutation in all BFIS patients. We also noticed that paroxysmal diseases (such as BFIS, PKD and ICCA) with PRRT2 mutations, instead of other forms, share some characteristics like being responded well to anti-epiletic treatment, we thus suggest to name them as PRRT2-related paroxysmal diseases (PRPDs) in order to assist clinical diagnosis and treatment., (Copyright © 2013 Elsevier Ireland Ltd. All rights reserved.)

Published

2013

3. PRRT2 gene mutations in familial and sporadic paroxysmal kinesigenic dyskinesia cases.

Author

Shi CH, Sun SL, Wang JL, Liu AQ, Miao W, Avinash C, Mao X, Tang BS, and Xu YM

Subjects

Asian People genetics, Cohort Studies, Dystonia, Female, Humans, Male, Chorea genetics, Family Health, Membrane Proteins genetics, Mutation genetics, Nerve Tissue Proteins genetics

Published

2013

4. Identification of PRRT2 as the causative gene of paroxysmal kinesigenic dyskinesias.

Author

Wang JL, Cao L, Li XH, Hu ZM, Li JD, Zhang JG, Liang Y, San-A, Li N, Chen SQ, Guo JF, Jiang H, Shen L, Zheng L, Mao X, Yan WQ, Zhou Y, Shi YT, Ai SX, Dai MZ, Zhang P, Xia K, Chen SD, and Tang BS

Subjects

Adolescent, Adult, Aged, Child, Chromosome Mapping, Female, Genetic Association Studies, Genetic Linkage, Genetic Loci, Genotype, Haplotypes, Humans, Male, Middle Aged, Mutation, Pedigree, Chorea genetics, Membrane Proteins genetics, Nerve Tissue Proteins genetics

Abstract

Paroxysmal kinesigenic dyskinesias is a paroxysmal movement disorder characterized by recurrent, brief attacks of abnormal involuntary movements induced by sudden voluntary movements. Although several loci, including the pericentromeric region of chromosome 16, have been linked to paroxysmal kinesigenic dyskinesias, the causative gene has not yet been identified. Here, we identified proline-rich transmembrane protein 2 (PRRT2) as a causative gene of paroxysmal kinesigenic dyskinesias by using a combination of exome sequencing and linkage analysis. Genetic linkage mapping with 11 markers that encompassed the pericentromeric of chromosome 16 was performed in 27 members of two families with autosomal dominant paroxysmal kinesigenic dyskinesias. Then, the whole-exome sequencing was performed in three patients from these two families. By combining the defined linkage region (16p12.1-q12.1) and the results of exome sequencing, we identified an insertion mutation c.649_650InsC (p.P217fsX7) in one family and a nonsense mutation c.487C>T (p.Q163X) in another family. To confirm our findings, we sequenced the exons and flanking introns of PRRT2 in another three families with paroxysmal kinesigenic dyskinesias. The c.649_650InsC (p.P217fsX7) mutation was identified in two of these families, whereas a missense mutation, c.796C>T (R266W), was identified in another family with paroxysmal kinesigenic dyskinesias. All of these mutations completely co-segregated with the phenotype in each family. None of these mutations was identified in 500 normal unaffected individuals of matched geographical ancestry. Thus, we have identified PRRT2 as the first causative gene of paroxysmal kinesigenic dyskinesias, warranting further investigations to understand the pathogenesis of this disorder.

Published

2011

5. Identification of PRRT2 as the causative gene of paroxysmal kinesigenic dyskinesias.

Author

Wang, Jun-Ling, Cao, Li, Li, Xun-Hua, Hu, Zheng-Mao, Li, Jia-Da, Zhang, Jian-Guo, Liang, Yu, San-A, Li, Nan, Chen, Su-Qin, Guo, Ji-Feng, Jiang, Hong, Shen, Lu, Zheng, Lan, Mao, Xiao, Yan, Wei-Qian, Zhou, Ying, Shi, Yu-Ting, Ai, San-Xi, and Dai, Mei-Zhi

Subjects

*MOVEMENT disorders, *CHROMOSOMES, *GENETICS, *MEMBRANE proteins, *LINKAGE (Genetics), *PHENOTYPES, *GENETIC mutation

Abstract

Paroxysmal kinesigenic dyskinesias is a paroxysmal movement disorder characterized by recurrent, brief attacks of abnormal involuntary movements induced by sudden voluntary movements. Although several loci, including the pericentromeric region of chromosome 16, have been linked to paroxysmal kinesigenic dyskinesias, the causative gene has not yet been identified. Here, we identified proline-rich transmembrane protein 2 (PRRT2) as a causative gene of paroxysmal kinesigenic dyskinesias by using a combination of exome sequencing and linkage analysis. Genetic linkage mapping with 11 markers that encompassed the pericentromeric of chromosome 16 was performed in 27 members of two families with autosomal dominant paroxysmal kinesigenic dyskinesias. Then, the whole-exome sequencing was performed in three patients from these two families. By combining the defined linkage region (16p12.1–q12.1) and the results of exome sequencing, we identified an insertion mutation c.649_650InsC (p.P217fsX7) in one family and a nonsense mutation c.487C>T (p.Q163X) in another family. To confirm our findings, we sequenced the exons and flanking introns of PRRT2 in another three families with paroxysmal kinesigenic dyskinesias. The c.649_650InsC (p.P217fsX7) mutation was identified in two of these families, whereas a missense mutation, c.796C>T (R266W), was identified in another family with paroxysmal kinesigenic dyskinesias. All of these mutations completely co-segregated with the phenotype in each family. None of these mutations was identified in 500 normal unaffected individuals of matched geographical ancestry. Thus, we have identified PRRT2 as the first causative gene of paroxysmal kinesigenic dyskinesias, warranting further investigations to understand the pathogenesis of this disorder. [ABSTRACT FROM PUBLISHER]

Published

2011

6. A sensitive and reversible staining of proteins on blot membranes.

Author

Wang, Jun-Ling, Zhao, Li, Li, Mei-Qi, Chen, Wei-Guang, and Xu, Chao-Jin

Subjects

*WESTERN immunoblotting, *MEMBRANE proteins, *CONGO red (Staining dye), *PEROXIDASE, *MOLECULAR docking, *POLYVINYLIDENE fluoride

Abstract

A modified, sensitive and reversible method for protein staining on nitrocellulose (NC) and polyvinylidine fluoride (PVDF) membranes was developed in Western blotting. The method employed Congo red staining to visualize proteins on different blot membranes. Staining of proteins with Congo red dye is more faster procedures. According to the experimental results, approximate 20 ng proteins could be detected in 3 min in room temperature. The staining on the proteins is easily reversible with Congo red destaining solution for NC and PVDF membranes, so that the blot membranes can be reused for Western blotting. In addition, we confirmed that the staining method is fully compatible with Western blot detection. NC and PVDF membranes treatment with Congo red staining does not interfere with conventional chemiluminescent substrates of peroxidase. As compared to MemCode reversible protein stain kits from Pirece Biotechnology, the staining technique is more sensitive, lower of cost, convenient and not adversely affecting subsequent Western blotting results. On the other hand, the stain is more sensitive than the Ponceau S staining. Therefore, Congo red staining is a promising and ideal alternative for current protein stain. Besides, the binding modes of Congo red or Ponceau S stain were investigated using various 2D and 3D molecular docking and demonstrated potential molecular basis for sensitivity of Congo red staining are higher than Ponceau S. Image 1 • We developed a sensitive and reversible method for protein staining on NC and PVDF membranes. • About 20 ng proteins could be detected in 3 min on NC and PVDF membranes by Congo red staining. • Congo red staining is much cheaper and more convenient compared to commercial MemCode kit. [ABSTRACT FROM AUTHOR]

Published

2020