Deficiency Mutations of Alpha-1 Antitrypsin. Effects on Folding, Function, and Polymerization

Haq, Imran Ul; Irving, James A.; Saleh, Aarash; Dron, Louis; Regan-Mochrie, Gemma L.; Motamedi-Shad, Neda; Hurst, John R.; Gooptu, Bibek; Lomas, David A.

doi:10.1165/rcmb.2015-0154oc

Cited by 35 publications

(30 citation statements)

References 48 publications

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“…Therefore, temperature can be used as a probe of mechanism: deviations from this trend indicate effects on other characteristics of the polymerisation pathway [22,39,62]. A comparison of polymerisation half-life interpolated at 55°C (Figure 1D) and stability determined by thermal unfolding (Figure 1E, left) is shown in Figure 1E (right).…”

Section: Resultsmentioning

confidence: 99%

An antibody that prevents serpin polymerisation acts by inducing a novel allosteric behaviour

Motamedi-Shad

Jagger

Liedtke

et al. 2016

Biochemical Journal

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Serpins are important regulators of proteolytic pathways with an antiprotease activity that involves a conformational transition from a metastable to a hyperstable state. Certain mutations permit the transition to occur in the absence of a protease; when associated with an intermolecular interaction, this yields linear polymers of hyperstable serpin molecules, which accumulate at the site of synthesis. This is the basis of many pathologies termed the serpinopathies. We have previously identified a monoclonal antibody (mAb4B12) that, in single-chain form, blocks α1-antitrypsin (α1-AT) polymerisation in cells. Here, we describe the structural basis for this activity. The mAb4B12 epitope was found to encompass residues Glu32, Glu39 and His43 on helix A and Leu306 on helix I. This is not a region typically associated with the serpin mechanism of conformational change, and correspondingly the epitope was present in all tested structural forms of the protein. Antibody binding rendered β-sheet A — on the opposite face of the molecule — more liable to adopt an ‘open’ state, mediated by changes distal to the breach region and proximal to helix F. The allosteric propagation of induced changes through the molecule was evidenced by an increased rate of peptide incorporation and destabilisation of a preformed serpin–enzyme complex following mAb4B12 binding. These data suggest that prematurely shifting the β-sheet A equilibrium towards the ‘open’ state out of sequence with other changes suppresses polymer formation. This work identifies a region potentially exploitable for a rational design of ligands that is able to dynamically influence α1-AT polymerisation.

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Section: Resultsmentioning

confidence: 99%

An antibody that prevents serpin polymerisation acts by inducing a novel allosteric behaviour

Motamedi-Shad

Jagger

Liedtke

et al. 2016

Biochemical Journal

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“…Human M and Z α 1 -antitrypsin were purified from donor plasma, and recombinant α 1 -antitrypsin was purified from Escherichia coli as previously described ( 24 , 40 ). Monoclonal antibodies were purified from hybridomas according to published methods ( 12 ) and stored in phosphate-buffered saline (PBS) with 0.02% (w/v) sodium azide.…”

Section: Methodsmentioning

confidence: 99%

The structural basis for Z α ₁ -antitrypsin polymerization in the liver

et al. 2020

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The serpinopathies are among a diverse set of conformational diseases that involve the aberrant self-association of proteins into ordered aggregates. α1-Antitrypsin deficiency is the archetypal serpinopathy and results from the formation and deposition of mutant forms of α1-antitrypsin as “polymer” chains in liver tissue. No detailed structural analysis has been performed of this material. Moreover, there is little information on the relevance of well-studied artificially induced polymers to these disease-associated molecules. We have isolated polymers from the liver tissue of Z α1-antitrypsin homozygotes (E342K) who have undergone transplantation, labeled them using a Fab fragment, and performed single-particle analysis of negative-stain electron micrographs. The data show structural equivalence between heat-induced and ex vivo polymers and that the intersubunit linkage is best explained by a carboxyl-terminal domain swap between molecules of α1-antitrypsin.

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“…Hexahistidine-tagged human A1AT introduced into the pQE-30 vector (QIAGEN) was expressed in the XL1-Blue strain of E. coli (Thermo Fisher Scientific), purified by nickel-affinity and ion-exchange chromatography, as described previously (43), and its purity was assessed by SDS-PAGE and nondenaturing PAGE. Plasma M, Z, and S A1AT were purified using Antitrypsin Select affinity resin (GE Healthcare) and ion-exchange chromatography, as described previously (44). Heat polymers were generated by incubating 21 μM of A1AT in phosphate saline buffer pH 7.4 (PBS) at 55°C (WT M) or 50°C (Z A1AT) for 16 hours (16), with removal of residual monomer by ion-exchange chromatography.…”

Section: Methodsmentioning

confidence: 99%

Intrahepatic heteropolymerization of M and Z alpha-1-antitrypsin

et al. 2020

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Deficiency Mutations of Alpha-1 Antitrypsin. Effects on Folding, Function, and Polymerization

Cited by 35 publications

References 48 publications

An antibody that prevents serpin polymerisation acts by inducing a novel allosteric behaviour

An antibody that prevents serpin polymerisation acts by inducing a novel allosteric behaviour

The structural basis for Z α ₁ -antitrypsin polymerization in the liver

Intrahepatic heteropolymerization of M and Z alpha-1-antitrypsin

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Deficiency Mutations of Alpha-1 Antitrypsin. Effects on Folding, Function, and Polymerization

Cited by 35 publications

References 48 publications

An antibody that prevents serpin polymerisation acts by inducing a novel allosteric behaviour

An antibody that prevents serpin polymerisation acts by inducing a novel allosteric behaviour

The structural basis for Z α 1 -antitrypsin polymerization in the liver

Intrahepatic heteropolymerization of M and Z alpha-1-antitrypsin

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The structural basis for Z α ₁ -antitrypsin polymerization in the liver