Your search keyword '"Lane, E. B."' showing total 8 results

1. Plectin deficiency results in muscular dystrophy with epidermolysis bullosa.

Author

Smith FJ, Eady RA, Leigh IM, McMillan JR, Rugg EL, Kelsell DP, Bryant SP, Spurr NK, Geddes JF, Kirtschig G, Milana G, de Bono AG, Owaribe K, Wiche G, Pulkkinen L, Uitto J, McLean WH, and Lane EB

Subjects

Amino Acid Sequence, Animals, Base Sequence, Chromosome Mapping, Chromosomes, Human, Pair 8, DNA Primers chemistry, Desmosomes metabolism, Genes, Recessive, Haplotypes, Humans, Intercellular Junctions physiology, Intermediate Filament Proteins deficiency, Molecular Sequence Data, Muscles metabolism, Pedigree, Plectin, Point Mutation, Rats, Sequence Alignment, Sequence Homology, Amino Acid, Skin metabolism, Cell Adhesion Molecules genetics, Epidermolysis Bullosa genetics, Intermediate Filament Proteins genetics, Muscular Dystrophies genetics

Abstract

We report that mutation in the gene for plectin, a cytoskeleton-membrane anchorage protein, is a cause of autosomal recessive muscular dystrophy associated with skin blistering (epidermolysis bullosa simplex). The evidence comes from absence of plectin by antibody staining in affected individuals from four families, supportive genetic analysis (localization of the human plectin gene to chromosome 8q24.13-qter and evidence for disease segregation with markers in this region) and finally the identification of a homozygous frameshift mutation detected in plectin cDNA. Absence of the large multifunctional cytoskeleton protein plectin can simultaneously account for structural failure in both muscle and skin.

Published

1996

2. Loss of plectin causes epidermolysis bullosa with muscular dystrophy: cDNA cloning and genomic organization.

Author

McLean WH, Pulkkinen L, Smith FJ, Rugg EL, Lane EB, Bullrich F, Burgeson RE, Amano S, Hudson DL, Owaribe K, McGrath JA, McMillan JR, Eady RA, Leigh IM, Christiano AM, and Uitto J

Subjects

Actins metabolism, Adult, Amino Acid Sequence, Base Sequence, Chromosome Mapping, Chromosomes, Human, Pair 8 genetics, Cloning, Molecular, Epidermolysis Bullosa pathology, Female, Frameshift Mutation, Humans, Male, Molecular Sequence Data, Muscular Dystrophies pathology, Pedigree, Phenotype, Plectin, Polymerase Chain Reaction, DNA, Complementary genetics, Epidermolysis Bullosa complications, Epidermolysis Bullosa genetics, Intermediate Filament Proteins deficiency, Intermediate Filament Proteins genetics, Muscular Dystrophies complications, Muscular Dystrophies genetics

Abstract

Plectin is a widely expressed high molecular weight protein that is involved in cytoskeleton-membrane attachment in epithelial cells, muscle, and other tissues. The human autosomal recessive disorder epidermolysis bullosa with muscular dystrophy (MD-EBS) shows epidermal blister formation at the level of the hemidesmosome and is associated with a myopathy of unknown etiology. Here, plectin was found to be absent in skin and cultured keratinocytes from an MD-EBS patient by immunofluorescence and immunoprecipitation, suggesting that plectin is a candidate gene/protein system for MD-EBS mutation. The 14800-bp human plectin cDNA was cloned and sequenced. The predicted 518-kD polypeptide has homology to the actin-binding domain of the dystrophin family at the amino terminus, a central rod domain, and homology to the intermediate filament-associated protein desmoplakin at the carboxyl terminus. The corresponding human gene (PLEC1), consisting of 33 exons spanning >26 kb of genomic DNA was cloned, sequenced, and mapped to chromosomal band 8q24. Homozygosity by descent was observed in the consanguineous MD-EBS family with intragenic plectin polymorphisms. Direct sequencing of PCR-amplified plectin cDNA from the patient's keratinocytes revealed a homozygous 8-bp deletion in exon 32 causing a frameshift and a premature termination codon 42 bp downstream. The clinically unaffected parents of the proband were found to be heterozygous carriers of the mutation. These results establish the molecular basis of MD-EBS in this family and clearly demonstrate the important structural role for plectin in cytoskeleton-membrane adherence in both skin and muscle.

Published

1996

3. Intermediate filaments in disease.

Author

McLean WH and Lane EB

Subjects

DNA genetics, Genetic Code, Genetic Linkage, Humans, Keratins genetics, Mutation, Protein Structure, Tertiary, Epidermolysis Bullosa genetics, Intermediate Filaments physiology

Abstract

Intermediate filaments are major structural proteins encoded by a large multigene family. Their tissue-specific expression makes them important in studies of development, differentiation and pathology. Most intermediate filaments are keratins; recent discoveries of keratin mutations in a range of genetic skin disorders have clarified their role as providing essential structural support for cells in different physical settings.

Published

1995

4. Mutations in the genes for epidermal keratins in epidermolysis bullosa and epidermolytic hyperkeratosis.

Author

Leigh IM and Lane EB

Subjects

Epidermolysis Bullosa pathology, Humans, Hyperkeratosis, Epidermolytic pathology, Epidermis pathology, Epidermolysis Bullosa genetics, Genes genetics, Hyperkeratosis, Epidermolytic genetics, Keratins genetics, Mutation genetics

Abstract

Background: Clues from clinicopathologic studies of epidermolysis bullosa simplex (EBS) and epidermolytic hyperkeratosis (EH) have implicated abnormalities in keratin filaments as possibly underlying the pathogenesis of these diseases. Multiple avenues of study have now converged, which confirm this hypothesis., Observations: The clinical spectrum of EBS and EH is reviewed together with classic histologic, electron microscopic, and immuno-electron microscopic studies. Linkage analyses have shown in EBS and EH that the disease traits are linked to the keratin gene clusters on chromosomes 12 and 17. Transgenic mice bearing mutations or deletions in genes coding for basal cell keratin K14 express the phenotype of EBS, and transgenic mice bearing abnormal K1/K10 genes resemble EH. Increasing numbers of point mutations in the human keratin genes have been found in both sporadic and familial cases of EBS in keratins 5/14 and EH in keratins K1/K10 genes, respectively, particularly in highly conserved subdomains of the keratin proteins., Conclusions: The recent and rapid progress in understanding the molecular biology of EBS and EH will also enhance knowledge about intermediate filament structure and function. Further studies of the effects of these mutations on the control of keratinocyte growth and differentiation are required. They will lead the way to rational pharmacologic or gene therapy.

Published

1993

5. Functional improvement of mutant keratin cells on addition of desmin: an alternative approach to gene therapy for dominant diseases.

Author

D'Alessandro, M., Morley, S. M., Ogden, P. H., Liovic, M., Porter, R. M., and Lane, E. B.

Subjects

KERATIN, CELLS, GENE therapy, GENE silencing, EPIDERMOLYSIS bullosa, KERATINOCYTES, CELL migration

Abstract

A major challenge to the concept of gene therapy for dominant disorders is the silencing or repairing of the mutant allele. Supplementation therapy is an alternative approach that aims to bypass the defective gene by inducing the expression of another gene, with similar function but not susceptible to the disrupting effect of the mutant one. Epidermolysis bullosa simplex (EBS) is a genetic skin fragility disorder caused by mutations in the genes for keratins K5 or K14, the intermediate filaments present in the basal cells of the epidermis. Keratin diseases are nearly all dominant in their inheritance. In cultured keratinocytes, mutant keratin renders cells more sensitive to a variety of stress stimuli such as osmotic shock, heat shock or scratch wounding. Using a ‘severe’ disease cell culture model system, we demonstrate reversion towards wild-type responses to stress after transfection with human desmin, an intermediate filament protein normally expressed in muscle cells. Such a supplementation therapy approach could be widely applicable to patients with related individual mutations and would avoid some of the financial obstacles to gene therapy for rare diseases.Gene Therapy (2004) 11, 1290-1295. doi:10.1038/sj.gt.3302301 Published online 24 May 2004 [ABSTRACT FROM AUTHOR]

Published

2004

6. Novel and recurrent mutations in keratin 10 causing bullous congenital ichthyosiform erythroderma.

Author

McLean, W H. I., Morley, S. M., Higgins, C., Bowden, P. E., White, M., Leigh, I. M., and Lane, E. B.

Subjects

GENETIC mutation, EPIDERMOLYSIS bullosa, KERATIN, BLISTERS, NEWBORN infants, GENETICS, AMINO acids

Abstract

Bullous congenital ichthyosiform erythroderma (BCIE) is a dominantly inherited keratinizing disorder characterized by erythroderma and blistering in neonates and generalized epidermolytic hyperkeratosis (EH) in adulthood. Previously, it has been shown that BCIE can be caused by mutations in either of the genes encoding K1 or K10, the keratins predominantly expressed in suprabasal layers of the epidermis. Using direct sequencing of genomic PCR fragments, we have analyzed 4 British families with BCIE, all of whom were found to carry mutations in K10. In 1 family, the affected person was found to have an unusual dinucleotide transversion mutation, 2138CC ??? AA, causing two amino acid substitutions, D155E and R156S, also in the 1A domain of the K10 polypeptide. In 2 further kindreds, the previously reported "hotspot" mutations 2139C ??? T and 2140G ??? A were found. These mutations predict amino acid substitutions in the helix 1A domain of K10, designated R156C and R156H respectively. The proband in the fourth family was found to carry a novel mutation 4724T ??? C, predicting the amino acid change L452P in the helix 2B domain of K10. All mutations were confirmed in the affected persons and were excluded from a population of 50 normal, unrelated individuals by restriction enzyme analysis. The location of these mutations in the highly conserved helix boundary motif sequences of K10 are consistent with previously reported dominant negative mutations in K10 and other keratins. Despite the unusual nature of two of these mutations, in particular the double missense mutation, the phenotypes of the affected individuals in these 4 families were entirely typical of BCIE. [ABSTRACT FROM AUTHOR]

Published

1999

7. Recessive epidermolysis bullosa simplex associated with plectin mutations: infantile respiratory complications in two unrelated cases.

Author

Mellerio, J. E., Smith, F. J. D., McMillan, J. R., McLean, W. H. I., McGrath, J. A., Morrison, G. A. J., Tierney, P., Albert, D. M., Wiche, G., Leigh, I. M., Geddes, J. F., Lane, E. B., Uitto, J., and Jeady, R. A.

Subjects

PROTEINS, CYTOSKELETON, CELL membranes, TISSUES, EPIDERMOLYSIS bullosa, RESPIRATORY distress syndrome, MUSCULAR dystrophy

Abstract

Plectin is a 500kDa protein involved in cytoskeleton-plasma membrane attachment with a wide tissue distribution including cutaneous and airway epithelia, muscle and neuronal tissue. Recently, mutations in the gene encoding plectin (PLEC1) have been implicated in the pathogenesis of an autosomal recessive variant of epidermolysis bullosa simplex in which cutaneous blistering starting in the neonatal period is associated with muscular dystrophy in later life. In this study, we report two unrelated patients, both of consanguineous parentage, who presented with cutaneous blistering and a hoarse cry from birth. Both experienced respiratory stridor and respiratory distress, necessitating emergency tracheostomy in one case, immunoreactivity to monoclonal antibodies against plectin was absent or markedly reduced in skin biopsies from both patients. Electron microscopy revealed a low intraepidermal plane of cleavage and hypoplastic hemidesmosomes with a reduced association with keratin intermediate filaments. Direct sequencing of PLEC1 in each case demonstrated two novel homozygous frameshift deletion mutations. 5069del19 and 5905Sdel2, which both create downstream premature termination codons. Although currently neither patient has symptoms of muscle disease, the identification of mutations in PLEC1 may be predictive for the future development of muscular dystrophy. Recessive epidermolysis bullosa simplex resulting from abnormalities in plectin should be considered in the differential diagnosis of cutaneous blistering, hoarseness and stridor in infancy. [ABSTRACT FROM AUTHOR]

Published

1997

8. Abnormalities of keratinocyte culture morphology in epidermolysis bullosa.

Author

Leigh, I. M., Lane, E. B., Tidman, M. J., and Eady, R. A. J.

Subjects

EPITHELIAL cells, CELL adhesion, EPIDERMOLYSIS bullosa, KERATINOCYTES, COLLAGEN, EPITHELIUM

Abstract

This article focuses on a study conducted to investigate abnormalities of epithelial adhesion in epidermolysis bullosa (EB) an in vitro system involving keratinocyte culture has been used. Samples of non-blistered, non-scarred skin were taken from one adult and three children with junctional EB, two children with recessive dystrophic EB and one child with generalized EB simplex. Keratinocyte cultures were prepared in the presence of 3T3 feeder cells on collagen-coated dishes using a previous technique.

Published

1983