3D structure of the C3bB complex provides insights into the activation and regulation of the complement alternative pathway convertase

Torreira, Eva; Tortajada, Agustín; Montes, Tamara; Córdoba, Santiago Rodrı́guez de; Llorca, Óscar

doi:10.1073/pnas.0810860106

Cited by 73 publications

(93 citation statements)

References 33 publications

(46 reference statements)

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“…We further illustrate our method by using experimental negative-stain and cryo-EM class averages as restraints to build accurate models for three additional protein assemblies in the Electron Microscopy Data Bank (EMDB): the human protoconvertase C3bB (EMDB ID code 1583) (19), the bovine mitochondrial supercomplex I 1 III 2 IV 1 (EMDB ID code 1876) (20), and the type I restriction modification complex EcoR124I from E. coli (EMDB ID code 1890) (21) ( Table 1 and Fig. S4).…”

Section: Resultsmentioning

confidence: 99%

“…The results demonstrate that accurate models for various types of macromolecular assemblies can be obtained by using only a limited number of class averages in combination with other restraints not containing direct 3D information. Next, as an example of the utility of the approach, we use it to compute models for the human transferrin receptor-transferrin (TfR-Tf) complex (18), the human C3bB protoconvertase complex (19), the bovine mitochondrial supercomplex I 1 III 2 IV 1 (20), and the type I restriction modification complex EcoR124I from Escherichia coli (21). Finally, the applicability of the method and possible improvements are discussed.…”

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confidence: 99%

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Assembly of macromolecular complexes by satisfaction of spatial restraints from electron microscopy images

Velázquez-Muriel

Lasker

Russel

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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To obtain a structural model of a macromolecular assembly by single-particle EM, a large number of particle images need to be collected, aligned, clustered, averaged, and finally assembled via reconstruction into a 3D density map. This process is limited by the number and quality of the particle images, the accuracy of the initial model, and the compositional and conformational heterogeneity. Here, we describe a structure determination method that avoids the reconstruction procedure. The atomic structures of the individual complex components are assembled by optimizing a match against 2D EM class-average images, an excluded volume criterion, geometric complementarity, and optional restraints from proteomics and chemical cross-linking experiments. The optimization relies on a simulated annealing Monte Carlo search and a divide-and-conquer message-passing algorithm. Using simulated and experimentally determined EM class averages for 12 and 4 protein assemblies, respectively, we show that a few class averages can indeed result in accurate models for complexes of as many as five subunits. Thus, integrative structural biology can now benefit from the relative ease with which the EM class averages are determined.integrative modeling | structural determination | computational biology E M is an increasingly useful approach for structural characterization of macromolecular assemblies (1-3). Different flavors of EM include electron crystallography, single-particle EM, and electron tomography (4), although tomography is generally limited to resolutions worse than 20 Å. Single-particle EM can be used with negative-stained or cryogenically frozen (cryo-EM) samples. Cryo-EM particularly presents some attractive advantages: It preserves a near-native conformation of the molecules, it can be applied to the study of large assemblies, and it can theoretically achieve atomic resolution (5). Currently, the standard way to analyze single-particle EM data is to align collected 2D single-particle images, cluster the images, calculate a 2D classaverage image for each cluster, and finally perform 3D reconstruction to obtain a 3D density map. Pseudoatomic models for many assemblies have been generated by fitting X-ray crystallographic structures and/or comparative models of the individual components into a density map of the whole assembly (6).Obtaining a high-resolution density map requires a large number of single-particle images and depends critically on determining an initial low-resolution density map as a template for reconstruction, as well as a high signal-to-noise ratio (SNR) in the particle images (7-10). Several methods exist to obtain the template map: randomconical reconstruction (11), common lines determination (12)(13)(14), and maximization of the posterior probability of observing the set of class averages (15). A challenge for template construction arises when the available class averages do not provide significant coverage of all the orientations of the complex; in such a case, an accurate template map cannot be compute...

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Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

Assembly of macromolecular complexes by satisfaction of spatial restraints from electron microscopy images

Velázquez-Muriel

Lasker

Russel

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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“…Three positively charged amino acids in the MG1 domain (Arg80, Arg72, and Lys82) form the thioester bond with four negative amino acids in the TED domain (Asp1007, Glu1008, Glu1010, Glu1013). The C3F variant, containing neutral glycine (instead of positively charged arginine), has a weaker ability to bind to CFH, which may impair the downregulation of the AP convertase, thus altering the C3 function [14,46,47]. The frequency of F allele varies among different populations, and it is the highest in Caucasian (18%) and the lowest in Asian (1%) [6,48].…”

Section: The Genetic Background Of the Ap Abnormalities In Glomerularmentioning

confidence: 99%

“…As rs1047286 is located in the MG3 domain of C3 (binding site of CFB), polymorphic variant HAV4-1+ has stronger ability to bind to CFB (Fig. 1) [46,50].…”

Section: The Genetic Background Of the Ap Abnormalities In Glomerularmentioning

confidence: 99%

“…Carries of C3F allele are at risk for the development of age-related macular degeneration (AMD) [46], partial lipodystrophy (PD) [51], and various types of GN: membranoproliferative glomerulonephritis type II (MPGN II, presently known as dense deposit disease, DDD) [51,52], IgA nephropathy (IgAN) [53,54] and systemic vasculitis (SV) [55,56]. Surprisingly, C3F allele has been shown to have a protective effect on transplant kidney, and its presence in donor's kidney may prolong the graft survival [57].…”

Section: The Genetic Background Of the Ap Abnormalities In Glomerularmentioning

confidence: 99%

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The role of the alternative pathway of complement activation in glomerular diseases

2018

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The complement system (CS) has recently been recognized as a bridge between innate and adaptive immunity that constitutes a very complex mechanism controlling the clearance of pathogens, cellular debris, and immune complexes. Out of three known pathways of complement activation, the alternative pathway (AP) plays a critical role in host defense by amplifying the complement response, independently of initiation pathway and continuously maintaining low-level activity in a process called 'thick-over.' A key molecule of the CS is C3, in which the AP is constantly activated. To prevent host cell destruction, a group of the AP regulators tightly controls this pathway of the CS activation. Acquired and genetic abnormalities of the CS may alter the delicate balance between enhancing and inhibiting the AP cascade. These can lead to the uncontrolled CS activation, inflammatory response, and subsequent tissue damage. Since complement components are locally produced and activated in the kidney, the abnormalities targeting the AP may cause glomerular injury. C3 glomerulopathy is a new entity, in which the AP dysregulation has been well established. However, recent studies indicate that the AP may also contribute to a wide range of kidney pathologies, including immune-complex-mediated glomerulonephritis (GN), pauci-immune GN, and primary membranous nephropathy (PMN). This article provides insight into current knowledge on the role of the AP in the pathogenesis of glomerular diseases, focusing mainly on various types of primary and secondary GN and PMN.

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Glycopolymer Brushes Presenting Sugars in Their Natural Form: Synthesis and Applications

Kizhakkedathu

2017

Polymer and Biopolymer Brushes

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3D structure of the C3bB complex provides insights into the activation and regulation of the complement alternative pathway convertase

Cited by 73 publications

References 33 publications

Assembly of macromolecular complexes by satisfaction of spatial restraints from electron microscopy images

Assembly of macromolecular complexes by satisfaction of spatial restraints from electron microscopy images

The role of the alternative pathway of complement activation in glomerular diseases

Glycopolymer Brushes Presenting Sugars in Their Natural Form: Synthesis and Applications

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