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Literature DB >> 20410306

Complement protein C1q forms a complex with cytotoxic prion protein oligomers.

Paul Erlich¹, Chantal Dumestre-Pérard, Wai Li Ling, Catherine Lemaire-Vieille, Guy Schoehn, Gérard J Arlaud, Nicole M Thielens, Jean Gagnon, Jean-Yves Cesbron.

Abstract

A growing number of studies have investigated the interaction between C1q and PrP, but the oligomeric form of PrP involved in this interaction remains to be determined. Aggregation of recombinant full-length murine PrP in the presence of 100 mm NaCl allowed us to isolate three different types of oligomers by size-exclusion chromatography. In contrast to PrP monomers and fibrils, these oligomers activate the classical complement pathway, the smallest species containing 8-15 PrP protomers being the most efficient. We used Thioflavine T fluorescence to monitor PrP aggregation and showed that, when added to the reaction, C1q has a cooperative effect on PrP aggregation and leads to the formation of C1q-PrP complexes. In these complexes, C1q interacts through its globular domains preferentially with the smallest oligomers, as shown by electron microscopy, and retains the ability to activate the classical complement pathway. Using two cell lines, we also provide evidence that C1q inhibits the cytotoxicity induced by the smallest PrP oligomers. The cooperative interaction between C1q and PrP could represent an early step in the disease, where it prevents elimination of the prion seed, leading to further aggregation.

Entities: Chemical Disease Gene Species

Mesh：

Substances：

Year: 2010 PMID： 20410306 PMCID： PMC2885205 DOI： 10.1074/jbc.M109.071860

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

44 in total

1. Sensitive detection of pathological prion protein by cyclic amplification of protein misfolding.

Authors: G P Saborio; B Permanne; C Soto
Journal: Nature Date: 2001-06-14 Impact factor: 49.962

2. Sequential generation of two structurally distinct ovine prion protein soluble oligomers displaying different biochemical reactivities.

Authors: Human Rezaei; Frédéric Eghiaian; Javier Perez; Bénédicte Doublet; Yvan Choiset; Thomas Haertle; Jeanne Grosclaude
Journal: J Mol Biol Date: 2005-04-01 Impact factor: 5.469

3. C1q binding and complement activation by prions and amyloids.

Authors: Robert B Sim; Uday Kishore; Christian L Villiers; Patrice N Marche; Daniel A Mitchell
Journal: Immunobiology Date: 2007-05-10 Impact factor: 3.144

4. Evidence for stepwise formation of amyloid fibrils by the mouse prion protein.

Authors: Shweta Jain; Jayant B Udgaonkar
Journal: J Mol Biol Date: 2008-07-26 Impact factor: 5.469

5. Prefibrillar transthyretin oligomers and cold stored native tetrameric transthyretin are cytotoxic in cell culture.

Authors: Karin Sörgjerd; Therése Klingstedt; Mikael Lindgren; Katarina Kågedal; Per Hammarström
Journal: Biochem Biophys Res Commun Date: 2008-11-05 Impact factor: 3.575

6. Subunit composition and structure of subcomponent C1q of the first component of human complement.

Authors: K B Reid; R R Porter
Journal: Biochem J Date: 1976-04-01 Impact factor: 3.857

7. Complement component C1q inhibits beta-amyloid- and serum amyloid P-induced neurotoxicity via caspase- and calpain-independent mechanisms.

Authors: Karntipa Pisalyaput; Andrea J Tenner
Journal: J Neurochem Date: 2007-11-06 Impact factor: 5.372

8. Mice devoid of PrP are resistant to scrapie.

Authors: H Büeler; A Aguzzi; A Sailer; R A Greiner; P Autenried; M Aguet; C Weissmann
Journal: Cell Date: 1993-07-02 Impact factor: 41.582

9. Study on the binding of Thioflavin T to beta-sheet-rich and non-beta-sheet cavities.

Authors: Minna Groenning; Lars Olsen; Marco van de Weert; James M Flink; Sven Frokjaer; Flemming S Jørgensen
Journal: J Struct Biol Date: 2006-12-31 Impact factor: 2.867

10. Native, amyloid fibrils and beta-oligomers of the C-terminal domain of human prion protein display differential activation of complement and bind C1q, factor H and C4b-binding protein directly.

Authors: Andreas P Sjöberg; Sofie Nyström; Per Hammarström; Anna M Blom
Journal: Mol Immunol Date: 2008-04-11 Impact factor: 4.407

15 in total

1. Global protein differential expression profiling of cerebrospinal fluid samples pooled from Chinese sporadic CJD and non-CJD patients.

Authors: Cao Chen; Di Xiao; Wei Zhou; Qi Shi; Hui-Fang Zhang; Jin Zhang; Chan Tian; Jian-Zhong Zhang; Xiao-Ping Dong
Journal: Mol Neurobiol Date: 2013-08-04 Impact factor: 5.590

10. Structural and Functional Characterization of a Single-Chain Form of the Recognition Domain of Complement Protein C1q.

Authors: Christophe Moreau; Isabelle Bally; Anne Chouquet; Barbara Bottazzi; Berhane Ghebrehiwet; Christine Gaboriaud; Nicole Thielens
Journal: Front Immunol Date: 2016-03-02 Impact factor: 7.561

Complement protein C1q forms a complex with cytotoxic prion protein oligomers.

1. Sensitive detection of pathological prion protein by cyclic amplification of protein misfolding.

2. Sequential generation of two structurally distinct ovine prion protein soluble oligomers displaying different biochemical reactivities.

3. C1q binding and complement activation by prions and amyloids.

4. Evidence for stepwise formation of amyloid fibrils by the mouse prion protein.

5. Prefibrillar transthyretin oligomers and cold stored native tetrameric transthyretin are cytotoxic in cell culture.

6. Subunit composition and structure of subcomponent C1q of the first component of human complement.

7. Complement component C1q inhibits beta-amyloid- and serum amyloid P-induced neurotoxicity via caspase- and calpain-independent mechanisms.

8. Mice devoid of PrP are resistant to scrapie.

9. Study on the binding of Thioflavin T to beta-sheet-rich and non-beta-sheet cavities.

10. Native, amyloid fibrils and beta-oligomers of the C-terminal domain of human prion protein display differential activation of complement and bind C1q, factor H and C4b-binding protein directly.

1. Global protein differential expression profiling of cerebrospinal fluid samples pooled from Chinese sporadic CJD and non-CJD patients.

2. Formation of Protein Corona on Nanoparticle Affects Different Complement Activation Pathways Mediated by C1q.

3. Posttranslational modifications define course of prion strain adaptation and disease phenotype.

Review 4. The role of genetics in chronic wasting disease of North American cervids.

5. Reaction of complement factors varies with prion strains in vitro and in vivo.

Review 6. Emerging and Novel Functions of Complement Protein C1q.

7. Low activity of complement in the cerebrospinal fluid of the patients with various prion diseases.

8. The human c1q globular domain: structure and recognition of non-immune self ligands.

9. Mechanisms of action of therapeutic amyloidogenic hexapeptides in amelioration of inflammatory brain disease.

10. Structural and Functional Characterization of a Single-Chain Form of the Recognition Domain of Complement Protein C1q.