Your search keyword '"HisRS"' showing total 7 results

1. Mechanistic perspectives on anti-aminoacyl-tRNA synthetase syndrome.

Author

Kanaji, Sachiko, Chen, Wenqian, Morodomi, Yosuke, Shapiro, Ryan, Kanaji, Taisuke, and Yang, Xiang-Lei

Subjects

*TRANSFER RNA, *AMINOACYL-tRNA synthetases, *TOLL-like receptors, *LIGASES, *PNEUMONIA, *IMMUNE response, *AUTOANTIBODIES, *MYELOID differentiation factor 88

Abstract

Antisynthetase syndrome (ASSD) is an autoimmune disease characterized by circulating autoantibodies against one of eight aminoacyl-tRNA synthetases (aaRSs). Although these autoantibodies are believed to play critical roles in ASSD pathogenesis, the nature of their roles remains unclear. Here we describe ASSD pathogenesis and discuss ASSD-linked aaRSs – from the WHEP domain that may impart immunogenicity to the role of tRNA in eliciting the innate immune response and the secretion of aaRSs from cells. Through these explorations, we propose that ASSD pathogenesis involves the tissue-specific secretion of aaRSs and that extracellular tRNAs or tRNA fragments and their ability to engage Toll-like receptor signaling may be important disease factors. Antisynthetase syndrome (ASSD) autoantibodies target one of eight cytoplasmic tRNA synthetases, which is usually not associated with the multisynthetase complex and most likely to be a class IIa tRNA synthetase. Tissue-specific secretion of tRNA synthetases and their cognate tRNA may contribute to their selective involvement in ASSD. Histidyl-tRNA synthetase (HisRS) is the predominant autoantigen in ASSD, and the major epitope resides in the evolutionarily new WHEP domain, which is not found in most other ASSD-linked aminoacyl-tRNA synthetases. The HisRS WHEP domain (with different C-terminus) reportedly can elicit either immune activation or immune-suppressive activities. The immune-suppressive activity of an HisRS WHEP-containing splice variant is being developed at clinical phases for treating lung inflammation. [ABSTRACT FROM AUTHOR]

Published

2023

2. Anti‐Jo1 autoantibodies, from clinic to the bench

Author

Angeles S. Galindo‐Feria, Begum Horuluoglu, and Ingrid E. Lundberg

Subjects

anti‐Jo1 autoantibodies, ASyS, HisRS, IIM, myositis, Immunologic diseases. Allergy, RC581-607, Diseases of the musculoskeletal system, RC925-935

Abstract

Abstract Introduction Idiopathic inflammatory myopathies (IIM) also known as myositis, is a chronic autoimmune disease which affects muscles, skin, joints and lung. One of the most common autoantibodies with a prevalence of 25‐35%, is the anti‐Jo‐1 autoantibodies, targeting the histidyl‐transfer RNA synthetase (HisRS). These autoantibodies are strongly associated with a distinct clinical phenotype called anti‐synthetase syndrome (ASyS) that includes interstitial lung disease (ILD), myositis, arthritis and Raynaud's phenomenon. The mechanism of how autoantibodies are produced and how they contribute to disease pathogenesis is unclear. Areas Covered In this review we will discuss the clinical manifestations associated with Jo‐1 autoantibodies, and the association with clinical features. Moreover, we will also review the molecular characteristics of the antibodies and how they affect the cells of the immune system in order to understand possible disease mechanisms.

Published

2022

3. Longitudinal assessment of reactivity and affinity profile of anti-Jo1 autoantibodies to distinct HisRS domains and a splice variant in a cohort of patients with myositis and anti-synthetase syndrome

Author

Antonella Notarnicola, Charlotta Preger, Susanna L. Lundström, Nuria Renard, Edvard Wigren, Eveline Van Gompel, Angeles S. Galindo-Feria, Helena Persson, Maryam Fathi, Johan Grunewald, Per-Johan Jakobsson, Susanne Gräslund, Ingrid E. Lundberg, and Cátia Fernandes-Cerqueira

Subjects

Anti-Jo1, HisRS, Longitudinal samples, ILD, Autoantibodies, Affinity, Diseases of the musculoskeletal system, RC925-935

Abstract

Abstract Background To address the reactivity and affinity against histidyl-transfer RNA synthetase (HisRS) autoantigen of anti-Jo1 autoantibodies from serum and bronchoalveolar lavage fluid (BALF) in patients with idiopathic inflammatory myopathies/anti-synthetase syndrome (IIM/ASSD). To investigate the associations between the reactivity profile and clinical data over time. Methods Samples and clinical data were obtained from (i) 25 anti-Jo1+ patients (19 sera with 16 longitudinal samples and 6 BALF/matching sera at diagnosis), (ii) 29 anti-Jo1− patients (25 sera and 4 BALF/matching sera at diagnosis), and (iii) 27 age/gender-matched healthy controls (24 sera and 3 BALF/matching sera). Reactivity towards HisRS full-length (HisRS-FL), three HisRS domains (WHEP, antigen binding domain (ABD), and catalytic domain (CD)), and the HisRS splice variant (SV) was tested. Anti-Jo1 IgG reactivity was evaluated by ELISA and western blot using IgG purified from serum by affinity chromatography. In paired serum-BALF, anti-Jo1 IgG and IgA reactivity was analyzed by ELISA. Autoantibody affinity was measured by surface plasmon resonance using IgG purified from sera. Correlations between autoantibody reactivity and clinical data were evaluated at diagnosis and longitudinally. Results Anti-Jo1 IgG from serum and BALF bound HisRS-FL, WHEP, and SV with high reactivity at the time of diagnosis and recognized both conformation-dependent and conformation-independent HisRS epitopes. Anti-HisRS-FL IgG displayed high affinity early in the disease. At the time of IIM/ASSD diagnosis, the highest autoantibody levels against HisRS-FL were found in patients ever developing interstitial lung disease (ILD) and arthritis, but with less skin involvement. Moreover, the reactivity of anti-WHEP IgG in BALF correlated with poor pulmonary function. Levels of autoantibodies against HisRS-FL, HisRS domains, and HisRS splice variant generally decreased over time. With some exceptions, longitudinal anti-HisRS-FL antibody levels changed in line with ILD activity. Conclusion High levels and high-affinity anti-Jo1 autoantibodies towards HisRS-FL were found early in disease in sera and BALF. In combination with the correlation of anti-HisRS-FL antibody levels with ILD and ILD activity in longitudinal samples as well as of anti-WHEP IgG in BALF with poor pulmonary function, this supports the previously raised hypothesis that the lung might have a role in the immune reaction in anti-Jo1-positive patients.

Published

2022

4. Longitudinal assessment of reactivity and affinity profile of anti-Jo1 autoantibodies to distinct HisRS domains and a splice variant in a cohort of patients with myositis and anti-synthetase syndrome

Author

Notarnicola, Antonella, Preger, Charlotta, Lundström, Susanna L., Renard, Nuria, Wigren, Edvard, Van Gompel, Eveline, Galindo-Feria, Angeles S., Persson, Helena, Fathi, Maryam, Grunewald, Johan, Jakobsson, Per-Johan, Gräslund, Susanne, Lundberg, Ingrid E., and Fernandes-Cerqueira, Cátia

Published

2022

5. Longitudinal assessment of reactivity and affinity profile of anti-Jo1 autoantibodies to distinct HisRS domains and a splice variant in a cohort of patients with myositis and anti-synthetase syndrome

Author

Per-Johan Jakobsson, Angeles Shunashy Galindo-Feria, Eveline Van Gompel, C. Preger, Helena Persson, Ingrid E. Lundberg, Cátia Fernandes-Cerqueira, A. Notarnicola, Maryam Fathi, E. Wigren, Susanna L. Lundström, Susanne Gräslund, Johan Grunewald, and Nuria Renard

Subjects

EPITOPES, DISEASE-ACTIVITY, Histidine-tRNA Ligase, Ligases, Rheumatology, INCLUSION-BODY MYOSITIS, Medicine, Humans, Reactivity (chemistry), TRANSFER-RNA-SYNTHETASE, HisRS, Myositis, Autoantibodies, Science & Technology, business.industry, Longitudinal samples, MORTALITY, Alternative splicing, Reactivity, Autoantibody, respiratory system, medicine.disease, respiratory tract diseases, Anti-Jo1, BALF, Affinity, POLYMYOSITIS, TISSUE, Immunology, Cohort, Anti-synthetase syndrome, AUTOANTIGEN, business, Lung Diseases, Interstitial, ILD, Idiopathic inflammatory myopathies, Life Sciences & Biomedicine, LUNG

Abstract

BackgroundTo address the reactivity and affinity against histidyl-transfer RNA synthetase (HisRS) autoantigen of anti-Jo1 autoantibodies from serum and bronchoalveolar lavage fluid (BALF) in patients with idiopathic inflammatory myopathies/anti-synthetase syndrome (IIM/ASSD). To investigate the associations between the reactivity profile and clinical data over time.MethodsSamples and clinical data were obtained from (i) 25 anti-Jo1+patients (19 sera with 16 longitudinal samples and 6 BALF/matching sera at diagnosis), (ii) 29 anti-Jo1−patients (25 sera and 4 BALF/matching sera at diagnosis), and (iii) 27 age/gender-matched healthy controls (24 sera and 3 BALF/matching sera). Reactivity towards HisRS full-length (HisRS-FL), three HisRS domains (WHEP, antigen binding domain (ABD), and catalytic domain (CD)), and the HisRS splice variant (SV) was tested. Anti-Jo1 IgG reactivity was evaluated by ELISA and western blot using IgG purified from serum by affinity chromatography. In paired serum-BALF, anti-Jo1 IgG and IgA reactivity was analyzed by ELISA. Autoantibody affinity was measured by surface plasmon resonance using IgG purified from sera. Correlations between autoantibody reactivity and clinical data were evaluated at diagnosis and longitudinally.ResultsAnti-Jo1 IgG from serum and BALF bound HisRS-FL, WHEP, and SV with high reactivity at the time of diagnosis and recognized both conformation-dependent and conformation-independent HisRS epitopes. Anti-HisRS-FL IgG displayed high affinity early in the disease. At the time of IIM/ASSD diagnosis, the highest autoantibody levels against HisRS-FL were found in patients ever developing interstitial lung disease (ILD) and arthritis, but with less skin involvement. Moreover, the reactivity of anti-WHEP IgG in BALF correlated with poor pulmonary function.Levels of autoantibodies against HisRS-FL, HisRS domains, and HisRS splice variant generally decreased over time. With some exceptions, longitudinal anti-HisRS-FL antibody levels changed in line with ILD activity.ConclusionHigh levels and high-affinity anti-Jo1 autoantibodies towards HisRS-FL were found early in disease in sera and BALF. In combination with the correlation of anti-HisRS-FL antibody levels with ILD and ILD activity in longitudinal samples as well as of anti-WHEP IgG in BALF with poor pulmonary function, this supports the previously raised hypothesis that the lung might have a role in the immune reaction in anti-Jo1-positive patients.

Published

2022

6. Use of biochemical approaches to elucidate substrate recognition by archaeal and eukaryotic Thg1 family enzymes

Author

Roach, Tracy Marie

Subjects

Biochemistry, Thg1, tRNA processing, tRNAHis, HisRS, enzymology

Abstract

In nature, most nucleotide incorporation is catalyzed in the 5'-3' direction. However, evidence of reverse 3'-5' nucleotide incorporation chemistry was first discovered in some eukaryotes where a post-transcriptional 3'-5' nucleotide addition occurs at the 5'-end of tRNAHis in vivo. The enzyme that adds a single guanosine (G-1) to tRNAHis was identified in Saccharomyces cerevisiae and named tRNAHis guanylyltransferase (Thg1). This essential enzyme is responsible for post-transcriptional addition of the G-1 identity element to tRNAHis for proper recognition by histidyl tRNA synthetase (HisRS), a necessary step for proficient translation. Despite its essential role, the molecular basis for Thg1 substrate recognition has not been clearly identified. The work presented in this dissertation has contributed to our understanding of approaches that can be used to better understand Thg1 family enzyme substrate recognition. For tRNAHis, it is known that Thg1 relies on the presence of the GUG anticodon. In addition, the presence of the essential 3'-CCA has proven to increase rates of nucleotide incorporation, binding, and fidelity of G-1 addition to tRNAHis by Thg1. Identifying the biochemical substrate preferences of Thg1 has provided more information about likely physiological requirements for tRNAHis processing pathways that are necessary to signal efficient and accurate G-1 addition by Thg1. The Thg1 substrate recognition mechanism has proven to be particularly challenging to characterize due to the stoichiometry of the Thg1-tRNA complex in systems studied to date. All Thg1 family enzymes studied so far form a homotetramer in their catalytic state, providing a platform for two tRNAs to bind, each contacting three of the four protein monomers. Each identical monomer thus contains residues that contribute to different aspects of substrate recognition and catalysis, and these interactions are therefore dependent on where the residues are located relative to the tRNA substrate. The capability of some Thg1 residues to act in different modes within the same complex makes this a particularly difficult target for biochemical characterization. In this work, we attempted to overcome the aforementioned challenges by characterizing a unique naturally occurring Thg1 gene system found in some green plants. In this system, two genes that each encode tandem Thg1 protein sequence repeats are found in the plant genome. This arrangement predictably conserves the overall four subunit architecture of the eukaryotic Thg1 described previously, but with the possibility of independent active sites involved in different aspects of substrate recognition and catalysis. Members of the larger Thg1 family are found in all three domains of life. Canonical Thg1 enzymes are only encoded in eukaryotes; however, Thg1-like proteins (TLPs) are found in all three domains. Because G-1 is a highly conserved identity element on tRNAHis, it was widely proposed that TLPs in Bacteria and Archaea are responsible for adding G-1 to tRNAHis as well. However, some TLPs in Eukarya have been recently identified as key players in tRNA repair and in catalyzing 5'-nucleotide addition to other small non-coding RNAs. The biological role of TLPs in Archaea has not been investigated until now. To understand if archaeal TLPs are adding G-1 to tRNAHis, we first asked whether these organisms require a G-1 for proper histidyl tRNA synthetase (HisRS) recognition. Biochemical data provides strong evidence that some archaea that encode TLPs do not require G-1 on tRNAHis. In support of this idea, an in vitro analysis provided biochemical evidence that archaeal TLPs do not efficiently catalyze single G-1 addition to cognate tRNAs. These data provide strong evidence that G-1 addition to tRNAHis is not the physiological role of TLPs in Archaea. Instead, these data imply that the role of these TLPs may be more diverse in Archaea and future work will be essential to identify the physiologically relevant substrates for these enzymes.

Published

2020

7. Dynamics of the active site loops in catalyzing aminoacylation reaction in seryl and histidyl tRNA synthetases.

Author

Dutta S, Kundu S, Saha A, and Nandi N

Subjects

Amino Acid Sequence, Binding Sites, Catalysis, Catalytic Domain, Molecular Dynamics Simulation, Protein Conformation, Thermus thermophilus chemistry, Thermus thermophilus enzymology, Amino Acids chemistry, Histidine-tRNA Ligase chemistry, Serine-tRNA Ligase chemistry, Transfer RNA Aminoacylation

Abstract

Aminoacylation reaction is the first step of protein biosynthesis. The catalytic reorganization at the active site of aminoacyl tRNA synthetases (aaRSs) is driven by the loop motions. There remain lacunae of understanding concerning the catalytic loop dynamics in aaRSs. We analyzed the functional loop dynamics in seryl tRNA synthetase from Methanopyrus kandleri ( mk SerRS) and histidyl tRNA synthetases from Thermus thermophilus ( tt HisRS), respectively, using molecular dynamics. Results confirm that the motif 2 loop and other active site loops are flexible spots within the catalytic domain. Catalytic residues of the loops form a network of interaction with the substrates to form a reactive state. The loops undergo transitions between closed state and open state and the relaxation of the constituent residues occurs in femtosecond to nanosecond time scale. Order parameters are higher for constituent catalytic residues which form a specific network of interaction with the substrates to form a reactive state compared to the Gly residues within the loop. The development of interaction is supported from mutation studies where the catalytic domain with mutated loop exhibits unfavorable binding energy with the substrates. During the open-close motion of the loops, the catalytic residues make relaxation by ultrafast librational motion as well as fast diffusive motion and subsequently relax rather slowly via slower diffusive motion. The Gly residues act as a hinge to facilitate the loop closing and opening by their faster relaxation behavior. The role of bound water is analyzed by comparing implicit solvent-based and explicit solvent-based simulations. Loops fail to form catalytically competent geometry in absence of water. The present result, for the first time reveals the nature of the active site loop dynamics in aaRS and their influence on catalysis.

Published

2018