Přejít k obsahu
Merck
  • C1q protein binds to the apoptotic nucleolus and causes C1 protease degradation of nucleolar proteins.

C1q protein binds to the apoptotic nucleolus and causes C1 protease degradation of nucleolar proteins.

The Journal of biological chemistry (2015-08-02)
Yitian Cai, Boon Heng Dennis Teo, Joo Guan Yeo, Jinhua Lu
ANOTACE

In infection, complement C1q recognizes pathogen-congregated antibodies and elicits complement activation. Among endogenous ligands, C1q binds to DNA and apoptotic cells, but whether C1q binds to nuclear DNA in apoptotic cells remains to be investigated. With UV irradiation-induced apoptosis, C1q initially bound to peripheral cellular regions in early apoptotic cells. By 6 h, binding concentrated in the nuclei to the nucleolus but not the chromatins. When nucleoli were isolated from non-apoptotic cells, C1q also bound to these structures. In vivo, C1q exists as the C1 complex (C1qC1r2C1s2), and C1q binding to ligands activates the C1r/C1s proteases. Incubation of nucleoli with C1 caused degradation of the nucleolar proteins nucleolin and nucleophosmin 1. This was inhibited by the C1 inhibitor. The nucleoli are abundant with autoantigens. C1q binding and C1r/C1s degradation of nucleolar antigens during cell apoptosis potentially reduces autoimmunity. These findings help us to understand why genetic C1q and C1r/C1s deficiencies cause systemic lupus erythematosus.

MATERIÁLY
Číslo produktu
Značka
Popis produktu

Sigma-Aldrich
Complement component C1q from human serum, ≥95% (SDS-PAGE)
Sigma-Aldrich
Complement C1, Human, Complement C1, Human Native, is the first component of the classical complement pathway. It is a calcium-dependent complex of C1q, C1r, and C1s subcomponents.