Molecular properties of the Goodpasture epitope

Gunnarsson, Andreas; Hellmark, Thomas; Wieslander, Jörgen

Molecular properties of the Goodpasture epitope

Mark

Gunnarsson, Andreas ; Hellmark, Thomas ^LU

and Wieslander, Jörgen ^LU (2000) In Journal of Biological Chemistry 275(40). p.30844-30848

Abstract: Goodpasture disease fulfils all criteria for a classical autoimmune disease, where autoantibodies targeted against the non-collagenous domain of the alpha3-chain of collagen IV initiates an inflammatory destruction of the basement membrane in kidney glomeruli and lung alveoli. This leads to a rapidly progressive glomerulonephritis and severe pulmonary hemorrhage. Previous studies have indicated a limited epitope for the toxic antibodies in the N-terminal part of the non-collagenous domain. The epitope has been partially characterized by recreating the epitope in the non-reactive alpha1-chain by exchanging nine residues to the corresponding ones of alpha3. In this study we have investigated to what extent each of these amino acids... (More); Goodpasture disease fulfils all criteria for a classical autoimmune disease, where autoantibodies targeted against the non-collagenous domain of the alpha3-chain of collagen IV initiates an inflammatory destruction of the basement membrane in kidney glomeruli and lung alveoli. This leads to a rapidly progressive glomerulonephritis and severe pulmonary hemorrhage. Previous studies have indicated a limited epitope for the toxic antibodies in the N-terminal part of the non-collagenous domain. The epitope has been partially characterized by recreating the epitope in the non-reactive alpha1-chain by exchanging nine residues to the corresponding ones of alpha3. In this study we have investigated to what extent each of these amino acids contribute to the antibody binding in different patient sera. The results show that seven of the nine substitutions are enough to get an epitope that is recognized equally well as the native alpha3-chain by all sera from 20 clinically verified Goodpasture patients. Furthermore, the patient sera reactivity against the different recombinant chains used in the study are very similar, with some minor exceptions, strongly supporting a highly defined and restricted epitope. We are convinced that the restriction of the epitope is of significant importance for the understanding of the etiology of the disease. Thereby also making every step on the way to characterization of the epitope a crucial step on the way to specific therapy for the disease. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1116535

author

Gunnarsson, Andreas ; Hellmark, Thomas ^LU

and Wieslander, Jörgen ^LU

organization

Nephrology

publishing date

2000

type

Contribution to journal

publication status

published

subject

Urology and Nephrology

in

Journal of Biological Chemistry

volume

275

issue

40

pages

30844 - 30848

publisher

American Society for Biochemistry and Molecular Biology

external identifiers

pmid:10896942
scopus:0034613171

ISSN

1083-351X

DOI

10.1074/jbc.M004717200

language

English

LU publication?

yes

id

3156d49f-f26a-445b-90d3-4e70f1ec64a2 (old id 1116535)

date added to LUP

2016-04-01 11:42:46

date last changed

2022-02-18 03:45:45

@article{3156d49f-f26a-445b-90d3-4e70f1ec64a2,
  abstract     = {{Goodpasture disease fulfils all criteria for a classical autoimmune disease, where autoantibodies targeted against the non-collagenous domain of the alpha3-chain of collagen IV initiates an inflammatory destruction of the basement membrane in kidney glomeruli and lung alveoli. This leads to a rapidly progressive glomerulonephritis and severe pulmonary hemorrhage. Previous studies have indicated a limited epitope for the toxic antibodies in the N-terminal part of the non-collagenous domain. The epitope has been partially characterized by recreating the epitope in the non-reactive alpha1-chain by exchanging nine residues to the corresponding ones of alpha3. In this study we have investigated to what extent each of these amino acids contribute to the antibody binding in different patient sera. The results show that seven of the nine substitutions are enough to get an epitope that is recognized equally well as the native alpha3-chain by all sera from 20 clinically verified Goodpasture patients. Furthermore, the patient sera reactivity against the different recombinant chains used in the study are very similar, with some minor exceptions, strongly supporting a highly defined and restricted epitope. We are convinced that the restriction of the epitope is of significant importance for the understanding of the etiology of the disease. Thereby also making every step on the way to characterization of the epitope a crucial step on the way to specific therapy for the disease.}},
  author       = {{Gunnarsson, Andreas and Hellmark, Thomas and Wieslander, Jörgen}},
  issn         = {{1083-351X}},
  language     = {{eng}},
  number       = {{40}},
  pages        = {{30844--30848}},
  publisher    = {{American Society for Biochemistry and Molecular Biology}},
  series       = {{Journal of Biological Chemistry}},
  title        = {{Molecular properties of the Goodpasture epitope}},
  url          = {{http://dx.doi.org/10.1074/jbc.M004717200}},
  doi          = {{10.1074/jbc.M004717200}},
  volume       = {{275}},
  year         = {{2000}},
}

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Molecular properties of the Goodpasture epitope