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

McLean, W. H. Irwin; Pulkkinen, Leena; Smith, Frances J.D.; Rugg, Elizabeth L.; Lane, E.B.; Bullrich, Florencia; Burgeson, Robert E.; Amano, Sadao; Hudson, David L.; Owaribe, Katsushi; McGrath, John A.; McMillan, James R.; Eady, R.A.J.; Leigh, Irene M.; Christiano, Angela M.; Uitto, Jouni

doi:10.1101/gad.10.14.1724

Cited by 285 publications

(220 citation statements)

References 52 publications

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“…We speculate that these multiple linkage systems play synergistic roles in maintaining the firm anchorage of keratin bundles to the hemidesmosome plaque. This idea is supported by studies that reveal that ablation of either plectin or BP230 in keratinocytes results in loss of keratin bundle association with the plaque of the hemidesmosome (Guo et al, 1995;Gache et al, 1996;McLean et al, 1996;Smith et al, 1996). These complex interconnections may enhance further the stability of keratin interaction with the cell surface and not only modulate cell-matrix association but also facilitate signal transduction at the site of the hemidesmosome (Giancotti, 1996).…”

Section: Discussionmentioning

confidence: 93%

The N Terminus of the Transmembrane Protein BP180 Interacts with the N-terminal Domain of BP230, Thereby Mediating Keratin Cytoskeleton Anchorage to the Cell Surface at the Site of the Hemidesmosome

Hopkinson

Jones

2000

MBoC

106

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In epidermal cells, the keratin cytoskeleton interacts with the elements in the basement membrane via a multimolecular junction called the hemidesmosome. A major component of the hemidesmosome plaque is the 230-kDa bullous pemphigoid autoantigen (BP230/BPAG1), which connects directly to the keratin-containing intermediate filaments of the cytoskeleton via its C terminus. A second bullous pemphigoid antigen of 180 kDa (BP180/BPAG2) is a type II transmembrane component of the hemidesmosome. Using yeast two-hybrid technology and recombinant proteins, we show that an N-terminal fragment of BP230 can bind directly to an N-terminal fragment of BP180. We have also explored the consequences of expression of the BP230 N terminus in 804G cells that assemble hemidesmosomes in vitro. Unexpectedly, this fragment disrupts the distribution of BP180 in transfected cells but has no apparent impact on the organization of endogenous BP230 and ␣6␤4 integrin. We propose that the BP230 N terminus competes with endogenous BP230 protein for BP180 binding and inhibits incorporation of BP180 into the cell surface at the site of the hemidesmosome. These data provide new insight into those interactions of the molecules of the hemidesmosome that are necessary for its function in integrating epithelial and connective tissue types.

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Section: Discussionmentioning

confidence: 93%

The N Terminus of the Transmembrane Protein BP180 Interacts with the N-terminal Domain of BP230, Thereby Mediating Keratin Cytoskeleton Anchorage to the Cell Surface at the Site of the Hemidesmosome

Hopkinson

Jones

2000

MBoC

106

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“…Similar structures were found in cells of the mouse TA3/Ha carcinoma cell line that normally grows in suspension because the large amount of the mucin epiglycanin on their surface prevents attachment of the cells to the substratum (Kemperman 1992), and therefore these molecules may also associate in other cell types to form a complex for anchoring other cytoskeleton components to the plasma membrane. Recent evidence indicates that HD1 and plectin are similar or identical proteins (Gache et al, 1996;McLean et al, 1996;Smith et al, 1996). Plectin is considered to be a general cross-linker of cytoskeletal networks (Foisner and Wiche, 1991), and in COS-7 cells plectin has been shown to associate with the vimentin and keratin networks (Wiche et al, 1993).…”

Section: Discussionmentioning

confidence: 99%

“…The structure of HD1 has not yet been determined but its apparent molecular mass and tissue distribution are similar to fhose of plectin (Gache et al, 1996). In addition, mutations in the plectin gene correlate with a loss of immunoreactivity not only of plectin but also of HD1 (McLean et al, 1996;Smith et al 1996). Together, these data suggest that HD1 and plectin are identical or related molecules.…”

Section: Introductionmentioning

confidence: 99%

Integrin alpha 6 beta 4 forms a complex with the cytoskeletal protein HD1 and induces its redistribution in transfected COS-7 cells.

Niessen

Hulsman

Rots

et al. 1997

MBoC

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The integrin a6134 is a major component of hemidesmosomes, in which it is linked to intermediate filaments. Its Subsequent immunoblot analysis revealed that the 500-kDa protein is in fact HD1. In COS-7 cells, which do not express a6f34 or the hemidesmosomal components BP230 and BP180, HD1 is associated with the cytoskeleton, but after transfecting the cells with cDNAs for human a6 and 134, it was, instead, colocalized with a6,64 at the basal side of the cells. The organization of the vimentin, keratin, actin, and tubulin cytoskeletal networks was not affected by the expression of a6f34 in COS-7 cells. The localization of HD1 at the basal side of the cells depends on the same region of 134 that forms a complex containing HD1 in vitro, since the expression of a6 with a mutant 134 subunit that lacks the four fibronectin type III repeats and the connecting segment did not alter the distribution of HD1. The results indicate that for association of a6134 with HD1, the cytoplasmic domain of 134 is essential. We suggest that this association may be crucial for hemidesmosome assembly.

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“…Initial examination of biochemical and synthetic properties of cultured keratinocytes from patients with EB-MD using antibodies against plectin showed that this protein was completely absent in the cells of several patients with EB-MD, and subsequently, mutations in the plectin gene (PLEC1) could be demonstrated in a number of families [46][47][48][49]. While EB-MD is a rare autosomal recessive disorder, most of the mutations reported thus far result in premature termination codons on both alleles of plectin, either by nonsense, insertion/deletion or splicing mutations, and the phenotype in these patients is remarkably consistent manifesting with neonatal blistering and progressive muscle weakness from the first or second decade of life on.…”

Section: The Paradigm Of Plectin Disordersmentioning

confidence: 99%

Diseases of epidermal keratins and their linker proteins

Uitto

Richard

McGrath³

2007

Experimental Cell Research

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Epidermal keratins, a diverse group of structural proteins, form intermediate filament networks responsible for the structural integrity of keratinocytes. The networks extend from the nucleus of the epidermal cells to the plasma membrane where the keratins attach to linker proteins which are part of desmosomal and hemidesmosomal attachment complexes. The expression of specific keratin genes is regulated by differentiation of the epidermal cells within the stratifying squamous epithelium. Progress in molecular characterization of the epidermal keratins and their linker proteins has formed the basis to identify mutations which are associated with distinct cutaneous manifestations in patients with genodermatoses. The precise phenotype of each disease apparently reflects the spatial level of expression of the mutated genes, as well as the types and positions of the mutations and their consequences at mRNA and protein levels. Identification of specific mutations in keratinization disorders has provided the basis for improved diagnosis and subclassification with prognostic implications and has formed the platform for prenatal testing and preimplantation genetic diagnosis. Finally, precise knowledge of the mutations is a prerequisite for development of gene therapy approaches to counteract, and potentially cure, these often devastating and currently intractable diseases. KeywordsEpidermal keratins; intermediate filaments; epidermal differentiation; hemidesmosomes; desmosomes; genodermatoses; skin fragility; epidermolysis bullosa; epidermolytic hyperkeratosis; ichthyosis Publisher's Disclaimer: This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final citable form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. BIOLOGY OF EPIDERMAL KERATINSKeratins NIH Public Access Author ManuscriptExp Cell Res. Author manuscript; available in PMC 2008 November 4. Published in final edited form as:Exp Cell Res. 2007 June 10; 313(10): 1995-2009. doi:10.1016/j.yexcr.2007.03.029. NIH-PA Author ManuscriptNIH-PA Author Manuscript NIH-PA Author Manuscript dimensional and highly dynamic cytoskeleton spanning between the nucleus and the cell membrane, where they are anchored by interactions with desmosomal and hemidesmosomal linker proteins (Fig. 1). This organization provides both structural stability and flexibility, and ensures the mechanical integrity of different epithelial tissues. Keratins are expressed as obligate heterodimers of acidic (type I) and basic (type II) proteins, which assemble, through a multi-step process, into intermediate filaments (Fig. 2). The genes encoding type I and type II keratins cluster on chromosomal regions 17q12-q21 and 12q11-q13, respectively. Keratin ...

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

Cited by 285 publications

References 52 publications

The N Terminus of the Transmembrane Protein BP180 Interacts with the N-terminal Domain of BP230, Thereby Mediating Keratin Cytoskeleton Anchorage to the Cell Surface at the Site of the Hemidesmosome

The N Terminus of the Transmembrane Protein BP180 Interacts with the N-terminal Domain of BP230, Thereby Mediating Keratin Cytoskeleton Anchorage to the Cell Surface at the Site of the Hemidesmosome

Integrin alpha 6 beta 4 forms a complex with the cytoskeletal protein HD1 and induces its redistribution in transfected COS-7 cells.

Diseases of epidermal keratins and their linker proteins

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