Identification of HSP47 Binding Site on Native Collagen and Its Implications for the Development of HSP47 Inhibitors

Cai, Haiyan; Sasikumar, Parvathy; Little, Gemma; Bihan, Dominique; Hamaia, Samir; Zhou, Aiwu; Gibbins, Jonathan M.; Farndale, Richard W.

doi:10.3390/biom11070983

Cited by 10 publications

(8 citation statements)

References 35 publications

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“…In contrast to structures available to date of proteins in complex with collagen peptides, which all involve a collagen residue with a long side chain, i.e. phenylalanine (VWF-A3 20 , SPARC 17 , and OSCAR 21 ), glutamate (α 2 β 1 40 ), or arginine (Hsp47 41,42 ), our structures reveal a novel collagen-binding mode employing the interaction of a rather flat surface across the D1 β-sheet of GPVI with several modestly-sized hydroxyprolines in collagen.…”

Section: Discussionmentioning

confidence: 99%

Structural insights into collagen binding by platelet receptor glycoprotein VI

Feitsma

Brondijk

Jarvis

et al. 2022

Blood

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Glycoprotein VI (GPVI) mediates collagen-induced platelet activation after vascular damage, and is an important contributor to the onset of thrombosis, heart attack and stroke. Animal models of thrombosis have identified GPVI as a promising target for antithrombotic therapy. Although for many years the crystal structure of GPVI has been known, the essential details of its interaction with collagen have remained elusive. Here, we present crystal structures of the GPVI ectodomain bound to triple-helical collagen peptides, which reveal a collagen-binding site across the β-sheet of the D1-domain. Mutagenesis and binding studies confirm the observed binding site, and identify Trp76, Arg38 and Glu40 as essential residues for binding to fibrillar collagens and collagen-related peptide (CRP). GPVI binds a site on collagen comprising two collagen chains with the core formed by the sequence motif OGPOGP. Potent GPVI-binding peptides from Toolkit-III all contain OGPOGP, weaker binding peptides frequently contain a partial motif varying at either terminus. Alanine-scanning of peptide III-30 also identified two AGPOGP motifs that contribute to GPVI-binding, but steric hindrance between GPVI-molecules restricts the maximum binding capacity. We further show that no cooperative interactions could occur between two GPVI-monomers binding to a stretch of (GPO)5, and that binding of two or more GPVI-molecules to a fibril-embedded helix requires non-overlapping OGPOGP-motifs. Our structure confirms the previously suggested similarity in collagen binding between GPVI and Leukocyte-Associated Immunoglobulin-like Receptor 1 (LAIR-1), but also indicates significant differences that may be exploited for the development of receptor-specific therapeutics.

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Section: Discussionmentioning

confidence: 99%

Structural insights into collagen binding by platelet receptor glycoprotein VI

Feitsma

Brondijk

Jarvis

et al. 2022

Blood

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“…SERPINH1, normally resides in the endoplasmic and plays a role in collagen biosynthesis and its folding as a molecular chaperone. 61,62 The protein level of SERPINH1 was not altered. THY1, also known as CD90, is a heavily glycosylated protein with a GPI anchor, which is present on the cell membrane of several cell types including fibroblasts.…”

Section: Discussionmentioning

confidence: 92%

“…Several other proteins also showed the downregulation at their glycosylation levels such as SERPINH, THY1, and HAPLN1. SERPINH1, normally resides in the endoplasmic and plays a role in collagen biosynthesis and its folding as a molecular chaperone 61,62 . The protein level of SERPINH1 was not altered.…”

Section: Discussionmentioning

confidence: 93%

N‐glycoproteomics reveals distinct glycosylation alterations in NGLY1‐deficient patient‐derived dermal fibroblasts

Budhraja

Saraswat

Graef

et al. 2022

J of Inher Metab Disea

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Congenital disorders of glycosylation are genetic disorders that occur due to defects in protein and lipid glycosylation pathways. A deficiency of N-glycanase 1, encoded by the NGLY1 gene, results in a congenital disorder of deglycosylation. The NGLY1 enzyme is mainly involved in cleaving N-glycans from misfolded, retrotranslocated glycoproteins in the cytosol from the endoplasmic reticulum before their proteasomal degradation or activation. Despite the essential role of NGLY1 in deglycosylation pathways, the exact consequences of NGLY1 deficiency on global cellular protein glycosylation have not yet been investigated. We undertook a multiplexed tandem mass tags-labeling-based quantitative glycoproteomics and proteomics analysis of fibroblasts from NGLY1-deficient individuals carrying different biallelic pathogenic variants in NGLY1. This quantitative mass spectrometric analysis detected 8041 proteins and defined a proteomic signature of differential expression across affected individuals and controls. Proteins that showed significant differential expression included phospholipid phosphatase 3, stromal cellderived factor 1, collagen alpha-1 (IV) chain, hyaluronan and proteoglycan link protein 1, and thrombospondin-1. We further detected a total of 3255 Nglycopeptides derived from 550 glycosylation sites of 407 glycoproteins by multiplexed N-glycoproteomics. Several extracellular matrix glycoproteins and adhesion molecules showed altered abundance of N-glycopeptides. Overall, we observed distinct alterations in specific glycoproteins, but our data revealed no global accumulation of glycopeptides in the patient-derived fibroblasts, despite the genetic defect in NGLY1. Our findings highlight new molecular and system-level insights for understanding NGLY1-CDDG.

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“…Hsp47 binding sites are predominantly located towards the N-terminal half of collagens type I, II and III. ( 12, 20, 70 ) Given the C- to N-terminal propagation, the implication is that Hsp47 binds these collagens after half the triple-helix has already folded. Hsp47 also does not recognize or does so only weakly collagens type XI, XIV, XXII.…”

Section: Discussionmentioning

confidence: 99%

“…By comparison, only a few binding sites for Hsp47 have formally been identified in human type II and III collagens. ( 20 ) Importantly, incorrect alignment of the chains in the respective triple helices dramatically decreases the number of possible salt bridges in all collagen subtypes. We also find that non-collagenous interruptions are frequently flanked by a higher density of salt bridges.…”

Section: Introductionmentioning

confidence: 99%

Code for Collagen Folding Deciphered

Malcor,

Ferruz,

Romero-Romero

et al. 2024

Preprint

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Collagen triple helix folds in two steps: nucleation of three polypeptides at the C-termini followed by zip-chain like propagation. The triple helices found in all domains of life as well as viruses contain upto 6000 amino acids in each polypeptide that are also frequently interrupted with non-helical sequences that disrupt folding and reduce stability. Given the length of polypeptide and the disruptive interruptions, compensating mechanisms that stabilize against local unfolding during propagation and offset the entropic cost of folding the long polypeptides are not fully understood. Here, we show that the information for correct folding of collagen triple helices is encoded in their sequence as interchain electrostatic interactions. In case of humans, disrupting these interactions causes severe to lethal diseases.Key ResultCollagen triple helices found in all the three domains of life as well as viruses have converged on similar mechanism to fold correctly.

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Identification of HSP47 Binding Site on Native Collagen and Its Implications for the Development of HSP47 Inhibitors

Cited by 10 publications

References 35 publications

Structural insights into collagen binding by platelet receptor glycoprotein VI

Structural insights into collagen binding by platelet receptor glycoprotein VI

N‐glycoproteomics reveals distinct glycosylation alterations in NGLY1‐deficient patient‐derived dermal fibroblasts

Code for Collagen Folding Deciphered

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