Your search keyword '"Complement system"' showing total 23,162 results

1. Leptospira Leptolysin Contributes to Serum Resistance but Is Not Essential for Acute Infection.

Author

Santos Courrol, Daniella, Santos, Cassia Moreira, Chura‐Chambi, Rosa Maria, Morganti, Lígia, Avelar, Kátia Eliane Santos, Moraes Maia, Fernanda, Rodrigues‐da‐Silva, Rodrigo Nunes, Wunder, Elsio Augusto Jr, and Barbosa, Angela Silva

Subjects

*RECOMBINANT proteins, *LEPTOSPIRA interrogans, *COMPLEMENT activation, *MUTANT proteins, *METALLOPROTEINASES

Abstract

ABSTRACT Previous in vitro works focusing on virulence determinants of the spirochete Leptospira implicated metalloproteinases as putative contributing factors to the pathogenicity of these bacteria. Those proteins have the capacity to degrade extracellular matrix components (ECM) and proteins of host's innate immunity, notably effectors of the complement system. In this study, we gained further knowledge on the role of leptolysin, one of the leptospiral‐secreted metalloproteinases, previously described as having a broad substrate specificity. We demonstrated that a proportion of human patients with mild leptospirosis evaluated in the current study produced antibodies that recognize leptolysin, thus indicating that the protease is expressed during host infection. Using recombinant protein and a knockout mutant strain, Manilae leptolysin−, we determined that leptolysin contributes to Leptospira interrogans serum resistance in vitro, likely by proteolysis of complement molecules of the alternative, the classical, the lectin, and the terminal pathways. Furthermore, in a hamster model of infection, the mutant strain retained virulence; however, infected animals had lower bacterial loads in their kidneys. Further studies are necessary to better understand the role and potential redundancy of metalloproteinases on the pathogenicity of this important neglected disease. [ABSTRACT FROM AUTHOR]

Published

2024

2. Vascularites immunologiques des petits et moyens vaisseaux : physiopathologie et diagnostic biologique.

Author

Kolopp Sarda, Marie-Nathalie, Dumestre-Pérard, Chantal, and Clavarino, Giovanna

Abstract

Les vascularites sont définies par une inflammation des endothéliums vasculaires, elles sont rares et de diagnostic difficile. Cet article n'évoquera que les vascularites primitives non infectieuses, comme cela est fait dans la nomenclature internationale de Chapel Hill dont la deuxième version impose le remplacement des dénominations éponymes des maladies par des expressions en lien avec leur mécanisme physiopathologique ou leurs caractéristiques histologiques. Cette nomenclature des vascularites prend en compte la taille des vaisseaux et les mécanismes physiopathologiques qui, dans l'atteinte des petits et moyens vaisseaux, sont des mécanismes immunologiques. Il s'agit d'une part des vascularites à dépôts de complexes immuns, comprenant les vascularites cryoglobulinémiques, les vascularites à dépôts d'IgA, les vascularites urticariennes hypocomplémentémiques (maladie de McDuffie) et les vascularites à Acs anti-membrane basale glomérulaire (maladie de Goodpasture), et d'autre part des vascularites à Acs anticytoplasme des polynucléaires neutrophiles (ANCA pour Anti-Neutrophil Cytoplasmic Antibodies), qui comprennent la granulomatose avec polyangéite (ex-syndrome de Wegener), la granulomatose à éosinophiles avec polyangéite (ex-syndrome de Churg et Strauss) et la polyangéite microscopique. Dans cet article, les mécanismes physiopathologiques de ces vascularites immunologiques et les outils biologiques seront développés, permettant aux biologistes de participer au diagnostic de ces maladies rares et fréquemment sévères. Vasculitis is defined by inflammation of the vascular endothelium, it is rare and difficult to diagnose. This article will only discuss primary non-infectious vasculitis, as is done in the international nomenclature of Chapel Hill, the second version of which aimed to replace the eponymous names of diseases with expressions related to their pathophysiological mechanism or their histological characteristics. This nomenclature of vasculitis takes into account the size of the vessels and the pathophysiological mechanisms which, in the involvement of small and medium-sized vessels, are immunological mechanisms. These are first, vasculitis with immune complex deposition, including cryoglobulinemic vasculitis, vasculitis with IgA deposits, hypocomplementemic urticarial vasculitis (McDuffie's disease) and vasculitis with anti-glomerular basement membrane Abs (Goodpasture's disease), and second, vasculitis with anti-neutrophil cytoplasmic Abs (ANCA), including granulomatosis with polyangiitis (formerly Wegener's syndrome), eosinophilic granulomatosis with polyangiitis (formerly Churg-Strauss syndrome) and microscopic polyangiitis. In this article, the pathophysiological mechanisms of these immunological vasculitides and the biological diagnostic tools will be developed, allowing biologists to participate in the diagnosis of these rare and frequently severe diseases. [ABSTRACT FROM AUTHOR]

Published

2024

3. The dysfunction of complement and coagulation in diseases: the implications for the therapeutic interventions.

Author

Jiang, Honghong, Guo, Yiming, Wang, Qihang, Wang, Yiran, Peng, Dingchuan, Fang, Yigong, Yan, Lei, Ruan, Zhuolin, Zhang, Sheng, Zhao, Yong, Zhang, Wendan, Shang, Wei, and Feng, Zhichun

Abstract

The complement system, comprising over 30 proteins, is integral to the immune system, and the coagulation system is critical for vascular homeostasis. The activation of the complement and coagulation systems involves an organized proteolytic cascade, and the overactivation of these systems is a central pathogenic mechanism in several diseases. This review describes the role of complement and coagulation system activation in critical illness, particularly sepsis. The complexities of sepsis reveal significant knowledge gaps that can be compared to a profound abyss, highlighting the urgent need for further investigation and exploration. It is well recognized that the inflammatory network, coagulation, and complement systems are integral mechanisms through which multiple factors contribute to increased susceptibility to infection and may result in a disordered immune response during septic events in patients. Given the overlapping pathogenic mechanisms in sepsis, immunomodulatory therapies currently under development may be particularly beneficial for patients with sepsis who have concurrent infections. Herein, we present recent findings regarding the molecular relationships between the coagulation and complement pathways in the advancement of sepsis, and propose potential intervention targets related to the crosstalk between coagulation and complement, aiming to provide more valuable treatment of sepsis. [ABSTRACT FROM AUTHOR]

Published

2024

4. Antibody density on bacteria regulates C1q recruitment by monoclonal IgG but not IgM.

Author

Aymerich, Nathan, Schlotheuber, Luca J., Bucheli, Olivia T. M., Portmann, Kevin, Baudry, Jean, and Eyer, Klaus

Subjects

BORDETELLA pertussis, BACTERIAL cells, NATURAL immunity, NEISSERIA meningitidis, COMPLEMENT activation

Abstract

Antibodies that trigger the complement system play a pivotal role in the immune defense against pathogenic bacteria and offer potential therapeutic avenues for combating antibiotic‐resistant bacterial infections, a rising global concern. To gain a deeper understanding of the key parameters regulating complement activation by monoclonal antibodies, we developed a novel bioassay for quantifying classical complement activation at the monoclonal antibody level, and employed this assay to characterize rare complement‐activating antibacterial antibodies on the single‐antibody level in postimmunization murine antibody repertoires. We characterized monoclonal antibodies from various antibody isotypes against specific pathogenic bacteria (Bordetella pertussis and Neisseria meningitidis) to broaden the scope of our findings. We demonstrated activation of the classical pathway by individual IgM‐ and IgG‐secreting cells, that is, monoclonal IgM and IgG2a/2b/3 subclasses. Additionally, we could observe different epitope density requirements for efficient C1q binding depending on antibody isotype, which is in agreement with previously proposed molecular mechanisms. In short, we found that antibody density most crucially regulated C1q recruitment by monoclonal IgG isotypes, but not IgM isotypes. This study provides additional insights into important parameters for classical complement initiation by monoclonal antibodies, a knowledge that might inform antibody screening and vaccination efforts. [ABSTRACT FROM AUTHOR]

Published

2024

5. The complement model disease paroxysmal nocturnal hemoglobinuria.

Author

Schmidt, Christoph Q., Höchsmann, Britta, and Schrezenmeier, Hubert

Subjects

COMPLEMENT inhibition, BLOOD diseases, COMPLEMENT activation, MEDICAL research, PATIENT experience, PAROXYSMAL hemoglobinuria

Abstract

We describe initial, current, and future aspects of complement activation and inhibition in the rare hematological disease paroxysmal nocturnal hemoglobinuria (PNH). PNH is a rare but severe hematological disorder characterized by complement‐mediated intravascular hemolysis resulting in anemia and severe thrombosis. Insights into the complement‐mediated pathophysiology ultimately led to regulatory approval of the first‐in‐class complement inhibitor, eculizumab, in 2007. This anti‐complement C5 therapy resulted in the stabilization of many hematologic parameters and dramatically reduced the often fatal, coagulant‐resistant thrombotic events. Despite the remarkable clinical success, a substantial proportion of PNH patients experience suboptimal clinical responses during anti‐C5 therapy. We describe the identification and mechanistic dissection of four unexpected processes responsible for such suboptimal clinical responses: (1) pharmacokinetic and (2) pharmacodynamic intravascular breakthrough hemolysis, (3) continuing low‐level residual intravascular hemolysis, and (4) extravascular hemolysis. Novel complement therapeutics mainly targeting different complement proteins proximal in the cascade attempt to address these remaining problems. With five approved complement inhibitors in the clinic and many more being evaluated in clinical trials, PNH remains one of the complement diseases with the highest intensity of clinical research. Mechanistically unexpected breakthrough events occur not only with C5 inhibitors but also with proximal pathway inhibitors, which require further mechanistic elaboration. [ABSTRACT FROM AUTHOR]

Published

2024

6. Circulating levels of endogenous complement inhibitors correlate inversely with complement consumption in systemic lupus erythematosus.

Author

van der Meulen, Stef, Monahan, Rory C., Gelderman, Kyra A., van Kooten, Cees, Teng, Y.K. Onno, Huizinga, Tom W.J., Steup‐Beekman, Gerda M., and Trouw, Leendert A.

Subjects

COMPLEMENT inhibition, COMPLEMENT activation, SYSTEMIC lupus erythematosus, CENTRAL nervous system, BIOMARKERS

Abstract

Systemic lupus erythematosus (SLE) is marked by excessive complement activation, contributing to tissue damage. Complement activation can be detected in many organs including the skin, kidney, and brain. The involvement of the central nervous system is particularly relevant to understanding neuropsychiatric SLE (NPSLE), one of the poorest understood manifestations of SLE for which no biomarkers are available. We studied the levels of complement inhibitors in SLE in relation to disease activity and as possible biomarkers to identify NPSLE. Serum levels of complement inhibitors C1‐inhibitor (C1‐INH), C4b‐binding protein (C4BP), Factor I, and Factor H were measured in 345 SLE patients (including 102 with NPSLE) and 108 healthy controls. Compared with controls, SLE patients had higher C1‐INH and C4BP but lower Factor I and H levels. All inhibitors positively correlated with total C3 and C4 levels. While correlating with the SLE Disease Activity Index (SLEDAI), no distinction in inhibitor levels was found between SLE and NPSLE patients. Over time, C1‐INH and Factor H levels normalized, but no significant changes were observed for C4BP and Factor I. In SLE the levels of circulating complement inhibitors are inversely correlated to complement consumption but do not serve as biomarkers for NPSLE. [ABSTRACT FROM AUTHOR]

Published

2024

7. Understanding the Role of the Complement System in Insulin Resistance and Metabolic Syndrome in Patients With Rheumatoid Arthritis.

Author

Rodríguez-González, Dara, García-González, María, Gómez-Bernal, Fuensanta, Quevedo-Abeledo, Juan C., González-Rivero, Agustín F., González-López, Elena, Ocejo-Vinyals, J. Gonzalo, González-Gay, Miguel Á., and Ferraz-Amaro, Iván

Subjects

COMPLEMENT activation, METABOLIC syndrome, INSULIN resistance, RHEUMATOID arthritis, CELL physiology

Abstract

Objective. The complement system has been associated with the etiopathogenesis of rheumatoid arthritis (RA). Insulin resistance (IR) and metabolic syndrome (MetS) are prevalent among patients with RA. The aim of this study was to explore the relationship between a comprehensive evaluation of the complement system and IR, as well as MetS, in patients with RA. Methods. A total of 339 nondiabetic patients with RA were recruited. Functional assays of the 3 complement pathways were assessed. Additionally, serum levels of the following individual components of the complement system were measured: C1q (classical); lectin (lectin); C2, C4, and C4b (classical lectin); factor D and properdin (alternative); C3 and C3a (common); C5, C5a, and C9 (terminal); as well as the factor I and C1 inhibitor regulators. IR and β cell function indices were calculated using the homeostatic model assessment. Criteria for MetS were applied. Multivariable linear regression analysis was performed to investigate the association between the complement system and IR in patients with RA. Results. Many elements of the upstream and common complement pathways, but not the functional tests of the 3 routes, correlated positively with higher levels of IR and β cell function. However, after multivariable adjustment for factors associated with IR, these relationships were lost. Conversely, the presence of MetS in patients with RA maintained a relationship with higher levels of C1q, C4, C3, properdin, and factor I after adjusting for confounders. Conclusion. There is a positive correlation between the complement system and MetS among nondiabetic patients with RA. This association is independent of traditional IR factors. [ABSTRACT FROM AUTHOR]

Published

2024

8. Dysregulated C1q and CD47 in the aging monkey brain: association with myelin damage, microglia reactivity, and cognitive decline.

Author

DeVries, Sarah A., Dimovasili, Christina, Medalla, Maria, Moore, Tara L., and Rosene, Douglas L.

Subjects

MYELIN basic protein, WHITE matter (Nerve tissue), MYELIN sheath, RHESUS monkeys, MIDDLE age

Abstract

Normal aging, though lacking widespread neurodegeneration, is nevertheless characterized by cognitive impairment in learning, memory, and executive function. The aged brain is spared from neuron loss, but white matter is lost and damage to myelin sheaths accumulates. This myelin damage is strongly associated with cognitive impairment. Although the cause of the myelin damage is not known, microglia dysregulation is a likely contributor. Immunologic proteins interact with microglial receptors to modulate microglia-mediated phagocytosis, which mediates myelin damage clearance and turn-over. Two such proteins, "eat me" signal C1q and "don't eat me" signal CD47, act in opposition with microglia. Both C1q and CD47 have been implicated in Multiple Sclerosis, a demyelinating disease, but whether they play a role in age-related myelin pathology is currently unknown. The present study investigates C1q and CD47 in relation to age-related myelin degeneration using multilabel immunofluorescence, RNAscope, and confocal microscopy in the cingulum bundle of male and female rhesus monkeys across the lifespan. Our findings showed significant age-related elevation in C1q localized to myelin basic protein, and this increase is associated with more severe cognitive impairment. In contrast, CD47 localization to myelin decreased in middle age and oligodendrocyte expression of CD47 RNA decreased with age. Lastly, microglia reactivity increased with age in association with the changes in C1q and CD47. Together, these results suggest disruption in the balance of "eat me" and "don't eat me" signals during normal aging, biasing microglia toward increased reactivity and phagocytosis of myelin, resulting in cognitive deficits. [ABSTRACT FROM AUTHOR]

Published

2024

9. The prognostic role of activation of the complement pathways in the progression of advanced IgA nephropathy to end-stage renal disease.

Author

Wang, Ying, Jiang, Shimin, Di, Dingxin, Zou, Guming, Gao, Hongmei, Shang, Shunlai, and Li, Wenge

Subjects

COMPLEMENT (Immunology), COMPLEMENT activation, IGA glomerulonephritis, CHRONIC kidney failure, KIDNEY physiology

Abstract

Introduction: The role of complement system in late stage of IgA nephropathy (IgAN) remains unknown. We therefore investigated the effects of complement system on worsening kidney function in advanced (stage 4 CKD) IgAN. Methods: Renal specimens of 69 IgAN patients who underwent renal biopsy during stage 4 CKD between 2010 and 2021, were stained using immunofluorescence (IF) and immunohistochemistry (IHC) for glomerular complement components. The primary outcome was progression to end-stage renal disease (ESRD). Associations of complement components with baseline clinicopathological characteristics and outcomes were assessed using multivariable Cox regression and Spearman analyses. Results: During a median follow-up of 18.0 months, 26 (37.7%) patients progressed to ESRD and none died. C1q and C3 deposition were detected in 12 and 66 patients, respectively. Higher eGFR [hazards ratio (HR), 0.852, 95% confidence interval (CI), 0.756–0.959; P = 0.008], higher C3 intensity (HR, 2.955, 95%CI, 1.063–8.220; P = 0.038) and T1-2 score (HR, 2.576, 95%CI, 1.205–5.576, P = 0.015) were predictive of time to ESRD in CKD 4 stage IgAN. Significant expressions of C1q (P = 0.005), C4d (P < 0.001), factor B (P < 0.001), C3 (P = 0.042) and C5b-9 (P = 0.004) were identified in ESRD group than in non-ESRD group by IHC, while MBL expression was low. Although they were not associated with baseline 24 h-UP, higher factor B and C1q expressions were both correlated with a lower baseline eGFR (P < 0.001 and = 0.04, respectively) and the deterioration of kidney function during follow-up (P = 0.046 and 0.015, respectively). Conclusion: Complement deposition in IgAN patients with stage 4 CKD portends a faster deterioration of kidney function. Activation of classical and alternative complement pathways plays a major role in this stage. [ABSTRACT FROM AUTHOR]

Published

2024

10. Long-term Elevation of Complement Factors in Cerebrospinal Fluid of Patients With Borna Disease Virus 1 Encephalitis.

Author

Bauswein, Markus, Zoubaa, Saida, Toelge, Martina, Eidenschink, Lisa, Riemenschneider, Markus J, Neumann, Bernhard, Lee, De-Hyung, Eid, Ehab, Tappe, Dennis, Niller, Hans Helmut, Gessner, André, Schmidt, Barbara, Bülow, Sigrid, and Angstwurm, Klemens

Subjects

*CENTRAL nervous system viral diseases, *BORNA disease virus, *COMPLEMENT activation, *ENCEPHALITIS viruses, *CEREBROSPINAL fluid

Abstract

Background Borna disease virus 1 (BoDV-1) causes rare but severe zoonotic infections in humans, presenting as encephalitis. The case-fatality risk is very high and no effective countermeasures have been established so far. An immunopathology is presumed, while data on immune responses in humans are limited. Evidence of a role of the complement system in various neurological disorders and in viral infections of the central nervous system is increasing and specific inhibitors are available as therapeutic options. Methods In this study, we investigated factors of the complement system in the cerebrospinal fluid (CSF) of patients with BoDV-1 infections (n = 17) in comparison to noninflammatory control CSF samples (n = 11), using a bead-based multiplex assay. In addition, immunohistochemistry was performed using postmortem brain tissue samples. Results We found an intrathecal elevation of complement factors of all complement pathways and an active cascade during human BoDV-1 infections. The increase of certain complement factors such as C1q was persistent, and C3 complement deposits were detected in postmortem brain sections. Intrathecal complement levels were negatively correlated with survival. Conclusions Further investigations are warranted to clarify whether targeting the complement cascade by specific inhibitors might be beneficial for patients suffering from severe BoDV-1 encephalitis. [ABSTRACT FROM AUTHOR]

Published

2024

11. The complement system as a target in cancer immunotherapy.

Author

Merle, Nicolas S. and Roumenina, Lubka T.

Subjects

COMPLEMENT (Immunology), COMPLEMENT activation, GENETIC overexpression, TUMOR microenvironment, CYTOTOXINS

Abstract

Malignant cells are part of a complex network within the tumor microenvironment, where their interaction with host cells and soluble mediators, including complement components, is pivotal. The complement system, known for its role in immune defense and homeostasis, exhibits a dual effect on cancer progression. This dichotomy arises from its antitumoral opsonophagocytosis and cytotoxicity versus its protumoral chronic inflammation mediated by the C5a/C5aR1 axis, influencing antitumor T‐cell responses. Recent studies have revealed distinct co‐expression patterns of complement genes in various cancer types, correlating with prognosis. Notably, some cancers exhibit co‐regulated overexpression of complement genes associated with poor prognosis, while others show favorable outcomes. However, significant intra‐patient heterogeneity further complicates this classification. Moreover, the involvement of locally produced and intracellular complement proteins adds complexity to the tumor microenvironment dynamics. This review highlights the unique interplay of complement components within different cancers and patient cohorts, showing that "one size does not fit all", for complement in cancer. It summarizes the clinical trials for complement targeting in cancer, emphasizing the need for tailored therapeutic approaches. By elucidating the mechanistic basis of complement's context‐dependent role, this review aims to facilitate the development of personalized cancer therapies, ultimately improving patient care and outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

12. Case report: Timing of eculizumab treatment in catastrophic antiphospholipid syndrome.

Author

Carrara, Camillo, Mataj, Blerina, Gastoldi, Sara, Ruggenenti, Piero, Sciascia, Savino, and Roccatello, Dario

Subjects

COMPLEMENT activation, COMPLEMENT inhibition, PHOSPHOLIPID antibodies, DISEASE remission, KIDNEY failure

Abstract

Catastrophic antiphospholipid syndrome (CAPS) is a life-threatening condition of small-vessel thrombosis with acute multiple-organ involvement and visceral damage. In this report, we present a case of a patient with CAPS who is refractory to conventional therapy. For the first time in a patient with CAPS, marked C5b-9 formation was demonstrated on microvascular endothelial cells, suggesting the usefulness of therapeutic complement inhibition in this setting. Eculizumab, a C5-blocking monoclonal antibody, is remarkably effective in the treatment of different forms of thrombotic microangiopathy by controlling complement system hyperactivation. It halted the "thrombotic storm" and promptly achieved full recovery of thrombocytopenia. However, kidney function did not recover, possibly because eculizumabwas administered too late. Conceivably, the timing of treatment is crucial to achieving disease remission before irreversible structural damage occurs in target organs, thereby preventing their complete functional recovery. [ABSTRACT FROM AUTHOR]

Published

2024

13. Role of factor H-related protein 3 in Pseudomonas aeruginosa bloodstream infections.

Author

González-Alsina, Alex, Martín-Merinero, Héctor, Mateu-Borrás, Margalida, Verd, María, Doménech-Sánchez, Antonio, Goldberg, Joanna B., Rodríguez de Córdoba, Santiago, and Albertí, Sebastián

Subjects

PSEUDOMONAS aeruginosa infections, COMPLEMENT factor H, BLOOD proteins, BACTERIAL cell surfaces, COMPLEMENT activation

Abstract

Pseudomonas aeruginosa is a leading cause of nosocomial bloodstream infections. The outcome of these infections depends on the virulence of the microorganism as well as host-related conditions and factors. The complement system plays a crucial role in defense against bloodstream infections. P. aeruginosa counteracts complement attack by recruiting Factor H (FH) that inhibits complement amplification on the bacterial surface. Factor H-related proteins (FHRs) are a group of plasma proteins evolutionarily related to FH that have been postulated to interfere this bacterial evasion mechanism. In this study, we demonstrate that FHR-3 competes with purified FH for binding to P. aeruginosa and identify EF-Tu as a common bacterial target for both complement regulator factors. Importantly, elevated levels of FHR-3 in human serum promote complement activation, leading to increased opsonization and killing of P. aeruginosa. Conversely, physiological concentrations of FHR-3 have no significant effect. Our findings suggest that FHR-3 may serve as a protective host factor against P. aeruginosa infections. [ABSTRACT FROM AUTHOR]

Published

2024

14. Autoimmune Hemolytic Anemias: Challenges in Diagnosis and Therapy.

Author

Barcellini, Wilma and Fattizzo, Bruno

Subjects

*HEMATOLOGIC agents, *PHYSICAL diagnosis, *BLOOD testing, *IMMUNOSUPPRESSIVE agents, *COMPUTED tomography, *IMMUNOLOGY technique, *DECISION making, *DIAGNOSIS, *DECISION making in clinical medicine, *FEVER, *ROUTINE diagnostic tests, *AUTOIMMUNE hemolytic anemia, *IMMUNOSUPPRESSION, *SYMPTOMS

Abstract

Background: Autoimmune hemolytic anemia (AIHA) is a rare disease due to increased destruction of erythrocytes by autoantibodies, with or without complement activation. Summary: AIHA is usually classified in warm AIHA (wAIHA) and cold agglutinin disease (CAD), based on isotype and thermal amplitude of the autoantibody. The direct antiglobulin test (DAT) or Coombs test is the cornerstone of AIHA diagnosis, as it is positive with anti-IgG in wAIHA, and with anti-C3d/IgM antisera plus high titer cold agglutinins in CAD. Therapy is quite different, as steroids and rituximab are effective in the former, but have a lower response rate and duration in the latter. Splenectomy, which is still a good option for young/fit wAIHA, is contraindicated in CAD, and classic immunosuppressants are moving to further lines. Several new drugs are increasingly used or are in trials for relapsed/refractory AIHAs, including B-cell (parsaclisib, ibrutinib, rilzabrutinib), and plasma cell target therapies (bortezomib, daratumumab), bispecific agents (ianalumab, obexelimab, povetacicept), neonatal Fc receptor blockers (nipocalimab), and complement inhibitors (sutimlimab, riliprubart, pegcetacoplan, iptacopan). Clinically, AIHAs are highly heterogeneous, from mild/compensated to life-threatening/fulminant, and may be primary or associated with infections, neoplasms, autoimmune diseases, transplants, immunodeficiencies, and drugs. Along with all these variables, there are rare forms like mixed (wAIHA plus CAD), atypical (IgA or warm IgM driven), and DAT negative, where the diagnosis and clinical management are particularly challenging. Key Messages: This article covers the classic clinical features, diagnosis, and therapy of wAIHA and CAD, and focuses, with the support of clinical vignettes, on difficult diagnosis and refractory/relapsing cases requiring novel therapies. [ABSTRACT FROM AUTHOR]

Published

2024

15. Therapeutic targeting of factor D and MASP3 in complement‐mediated diseases: Lessons learned from mouse studies.

Author

Mohammadyari, Eshagh, Miwa, Takashi, Golla, Madhu, and Song, Wen‐Chao

Abstract

The alternative pathway (AP) plays a major role in many complement‐mediated human diseases. Factor D (FD), a rate‐limiting enzyme in AP complement activation, is an attractive therapeutic target. Unlike other complement proteins, FD is synthesized primarily in adipose tissue, and its levels in human blood are relatively low. However, because of FD's high turnover rate, therapeutic targeting with monoclonal antibodies and chemical inhibitors has been challenging. The recent discovery that FD activity is regulated by mannose‐binding lectin‐associated serine protease 3 (MASP3), through conversion of a zymogen to mature FD, has sparked interest in MASP3 inhibition as a new way to block FD function and AP complement activity. Here, we review studies of mouse models of FD and MASP3 inhibition. We additionally discuss the lessons learned from these studies and their implications for therapeutic targeting of human FD and MASP3. [ABSTRACT FROM AUTHOR]

Published

2024

16. Association of Endothelial Cell Activation with Acute Kidney Injury during Coronary Angiography and the Influence of Recombinant Human C1 Inhibitor—A Secondary Analysis of a Randomized, Placebo-Controlled, Double-Blind Trial.

Author

Moser, Stephan, Araschmid, Laura, Panagiotou, Anneza, Bonati, Leo H., Breidthardt, Tobias, Fahrni, Gregor, Kaiser, Christoph, Jeger, Raban, Trendelenburg, Marten, and Osthoff, Michael

Subjects

CD54 antigen, CELL adhesion molecules, POISONS, ACUTE kidney failure, CONTRAST media, VASCULAR cell adhesion molecule-1, RADIOGRAPHIC contrast media

Abstract

Background: Acute kidney injury (AKI) as a result of iodinated contrast media (CM) has been linked to CM-induced renal ischemia and toxic effects on endothelial cells (EC). The recombinant human C1 inhibitor (rhC1INH) has been shown to influence EC activation. Methods: Secondary analysis of 74/77 (96%) participants of a double-blind, randomized, and placebo-controlled study that assessed the effect of rhC1INH on AKI. E-selectin, intercellular adhesion molecule-1 (ICAM-1), vascular cell adhesion molecule (VCAM-1), and CC-chemokin-ligand-5 (CCL5) were determined in frozen blood samples over 48 h and analyzed according to the treatment group and renal outcomes. Results: The mean age was 76.7 years, and 37 patients each received rhC1INH and placebo, respectively. In the entire study population, minor differences in median EC activation markers/CCL5 concentrations during the first 48 h compared to baseline were observed (e.g., E-selectin 27.5 ng/mL at baseline vs. 29.7 ng/mL on day 1, CCL5: 17.7 ng/mL at baseline vs. 32.2 ng/mL on day 2). Absolute changes in ICAM-1/E-selectin concentrations correlated with a higher peak change in urinary NGAL concentrations. However, AKI was not associated with significant changes in EC markers/CCL5. Last, no significant differences in serum concentrations of EC activation markers/CCL5 were evident between the placebo and the rhC1INH group. Conclusions: CM administration during coronary angiography only mildly activated ECs within the first 48 h, which does not explain subsequent AKI. The administration of rhC1INH was not associated with a reduction of EC activation or CCL5. [ABSTRACT FROM AUTHOR]

Published

2024

17. Anti-Poly(ethylene glycol) (PEG) Antibodies: From Where Are We Coming and Where Are We Going.

Author

Simberg, Dmitri and Moghimi, S. Moein

Subjects

IMMUNE response, COMPLEMENT activation, POLYETHYLENE glycol, IMMUNOGLOBULINS, DRUGS

Abstract

PEGylation technology confers stability and modulates the biological performance of a broad range of preclinical and clinical nanopharmaceuticals. However, the emerging PEG immunogenicity in the general population is thought to impact the efficacy and safety of PEGylated medicines. Despite this, the clinical significance of PEG immunogenicity is still not clear and remains debatable. By considering the strategic importance of the PEGylation technology in nanopharmaceutical engineering, we raise a number of critical questions and briefly discuss gaps in the knowledge of PEG immunogenicity and its clinical significance. [ABSTRACT FROM AUTHOR]

Published

2024

18. The prognostic role of activation of the complement pathways in the progression of advanced IgA nephropathy to end-stage renal disease

Author

Ying Wang, Shimin Jiang, Dingxin Di, Guming Zou, Hongmei Gao, Shunlai Shang, and Wenge Li

Subjects

IgA nephropathy, Complement system, C1q, Factor B, C3, Prognosis, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Abstract Introduction The role of complement system in late stage of IgA nephropathy (IgAN) remains unknown. We therefore investigated the effects of complement system on worsening kidney function in advanced (stage 4 CKD) IgAN. Methods Renal specimens of 69 IgAN patients who underwent renal biopsy during stage 4 CKD between 2010 and 2021, were stained using immunofluorescence (IF) and immunohistochemistry (IHC) for glomerular complement components. The primary outcome was progression to end-stage renal disease (ESRD). Associations of complement components with baseline clinicopathological characteristics and outcomes were assessed using multivariable Cox regression and Spearman analyses. Results During a median follow-up of 18.0 months, 26 (37.7%) patients progressed to ESRD and none died. C1q and C3 deposition were detected in 12 and 66 patients, respectively. Higher eGFR [hazards ratio (HR), 0.852, 95% confidence interval (CI), 0.756–0.959; P = 0.008], higher C3 intensity (HR, 2.955, 95%CI, 1.063–8.220; P = 0.038) and T1-2 score (HR, 2.576, 95%CI, 1.205–5.576, P = 0.015) were predictive of time to ESRD in CKD 4 stage IgAN. Significant expressions of C1q (P = 0.005), C4d (P

Published

2024

19. Complement activation and lung injury in Japanese patients with COVID-19: a prospective observational study

Author

Kentaro Seki, Koichiro Sueyoshi, Yukari Miyoshi, Yuki Nakamura, Tadashi Ishihara, Yutaka Kondo, Yoko Kuroda, Ayumi Yonekura, Kazuhisa Iwabuchi, Ken Okamoto, and Hiroshi Tanaka

Subjects

Complement system, COVID-19, Invasive mechanical ventilation, Syndecan-1, Medicine, Science

Abstract

Abstract Background The production of inflammatory cytokines is reportedly increased in patients with coronavirus disease 2019 (COVID-19), causing the migration of neutrophils and monocytes to lung tissues. This disrupts the air–blood barrier by damaging the bronchial epithelial and vascular endothelial cells. As multiorgan dysfunction in sepsis is considered to be partly caused by complement activation, which can cause lung injury in patients with COVID-19. There are limited studies examining the link between complement activation in patients with COVID-19. This study aimed to AQinvestigate the association of complement activation with the pathophysiology of COVID-19. Twenty-seven patients with COVID-19 were enrolled in this study and classified into two groups depending on the indication for mechanical ventilation. Plasma complement factors (C3a, C5a, Ba, and sC5b-9), complement regulators (sCD59 and factor H), interleukin-6 (IL-6), and syndecan-1 levels were measured using Enzyme-linked immunosorbent assay (ELISA). Results: All complement factors and regulators, IL-6, and syndecan-1 levels were significantly elevated in patients with COVID-19 compared with those in healthy controls. C5a and sC5b-9 levels were decreased significantly in the invasive mechanical ventilation (IMV) group compared with those in the non-IMV group. Syndecan-1 levels were significantly increased in the IMV group compared with those in the non-IMV group. Conclusions: Complement activation is an exacerbating factor for lung injury in patients with COVID-19. Complement factors are nonessential predictors of mechanical ventilation; however, syndecan-1 could be a biomarker of COVID-19 severity in patients.

Published

2024

20. Pathophysiological dynamics in the contact, coagulation, and complement systems during sepsis: Potential targets for nafamostat mesilate

Author

Qiaolan He, Yilin Wei, Yiqi Qian, and Ming Zhong

Subjects

Sepsis, Nafamostat, Contact system, Coagulation system, Complement system, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Sepsis is a life-threatening syndrome resulting from a dysregulated host response to infection. It is the primary cause of death in the intensive care unit, posing a substantial challenge to human health and medical resource allocation. The pathogenesis and pathophysiology of sepsis are complex. During its onset, pro-inflammatory and anti-inflammatory mechanisms engage in intricate interactions, possibly leading to hyperinflammation, immunosuppression, and long-term immune disease. Of all critical outcomes, hyperinflammation is the main cause of early death among patients with sepsis. Therefore, early suppression of hyperinflammation may improve the prognosis of these patients. Nafamostat mesilate is a serine protease inhibitor, which can inhibit the activation of the complement system, coagulation system, and contact system. In this review, we discuss the pathophysiological changes occurring in these systems during sepsis, and describe the possible targets of the serine protease inhibitor nafamostat mesilate in the treatment of this condition.

Published

2024

21. Exploring the hub Genes and Potential Mechanisms of Complement system-related Genes in Parkinson Disease: Based on Transcriptome Sequencing and Mendelian Randomization.

Author

Wang, Xin, Yang, Gaoming, Lai, Yali, Li, Yuanyuan, and Liu, Xindong

Abstract

An accurate diagnosis of Parkinson’s disease (PD) remains challenging and the exact cause of the disease is unclean. The aims are to identify hub genes associated with the complement system in PD and to explore their underlying molecular mechanisms. Initially, differentially expressed genes (DEGs) and key module genes related to PD were mined through differential expression analysis and WGCNA. Then, differentially expressed CSRGs (DE-CSRGs) were obtained by intersecting the DEGs, key module genes and CSRGs. Subsequently, MR analysis was executed to identify genes causally associated with PD. Based on genes with significant MR results, the expression level and diagnostic performance verification were achieved to yield hub genes. Functional enrichment and immune infiltration analyses were accomplished to insight into the pathogenesis of PD. qRT-PCR was employed to evaluate the expression levels of hub genes. After MR analysis and related verification, CD93, CTSS, PRKCD and TLR2 were finally identified as hub genes. Enrichment analysis indicated that the main enriched pathways for hub genes. Immune infiltration analysis found that the hub genes showed significant correlation with a variety of immune cells (such as myeloid-derived suppressor cell and macrophage). In the qRT-PCR results, the expression levels of CTSS, PRKCD and TLR2 were consistent with those we obtained from public databases. Hence, we mined four hub genes associated with complement system in PD which provided novel perspectives for the diagnosis and treatment of PD. [ABSTRACT FROM AUTHOR]

Published

2024

22. Complement C3a/C3aR inhibition alleviates the formation of aortic aneurysm in Marfan syndrome mice

Author

Fan Zhang, Kexin Yao, Yan Liu, Mei Zhou, Yanhong Zhang, Shiyao Hong, Jian Wu, and Congcong Zhang

Subjects

Marfan syndrome, Aortic aneurysm, Complement system, Inflammation, MMPs activities, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Mutations in fibrillin 1 (FBN1) is the main cause of Marfan syndrome (MFS) with thoracic aortic aneurysm (TAA) as the main complication. Activation of the complement system plays a key role in the formation of thoracic and abdominal aortic aneurysms. However, the role of the complement system in MFS-associated aortic aneurysms remains unclear. In this study, we observed increased levels of complement C3a and C5a in the plasma of MFS patients and mouse, and the increased deposition of the activated complement system product C3b/iC3b was also observed in the elastic fiber rupture zone of 3-month-old MFS mice. The expression of C3a receptor (C3aR) was increased in MFS aortas, and recombinant C3a promoted the expression of cytokines in macrophages. The administration of a C3aR antagonist (C3aRA) attenuated the development of thoracic aortic aneurysms in MFS mice. The increased inflammation response and matrix metalloproteinases activities were also attenuated by C3aRA treatment in MFS mice. Therefore, these findings indicate that the complement C3a/C3aR inhibition alleviates the formation of aortic aneurysm in Marfan syndrome mice.

Published

2024

23. Anti-Poly(ethylene glycol) (PEG) Antibodies: From Where Are We Coming and Where Are We Going

Author

Dmitri Simberg and S. Moein Moghimi

Subjects

antibodies, complement system, immunogenicity, poly(ethylene glycol), Medical technology, R855-855.5

Abstract

PEGylation technology confers stability and modulates the biological performance of a broad range of preclinical and clinical nanopharmaceuticals. However, the emerging PEG immunogenicity in the general population is thought to impact the efficacy and safety of PEGylated medicines. Despite this, the clinical significance of PEG immunogenicity is still not clear and remains debatable. By considering the strategic importance of the PEGylation technology in nanopharmaceutical engineering, we raise a number of critical questions and briefly discuss gaps in the knowledge of PEG immunogenicity and its clinical significance.

Published

2024

24. The Relationship between the complement system and subclinical carotid atherosclerosis in patients with rheumatoid arthritis

Author

Marta Hernández-Díaz, Dara Rodríguez-González, Elena Heras-Recuero, Fuensanta Gómez-Bernal, Juan Carlos Quevedo-Abeledo, Agustín F. González-Rivero, Elena González-López, J. Gonzalo Ocejo-Vinyals, Alejandro Jimenez-Sosa, Miguel Ángel González-Gay, and Iván Ferraz-Amaro

Subjects

Rheumatoid arthritis, Complement system, Carotid plaque, Intima media thickness, Atherosclerosis, Cardiovascular disease, Diseases of the musculoskeletal system, RC925-935

Abstract

Abstract Background Patients with rheumatoid arthritis (RA) have an increased risk of cardiovascular (CV) events and CV mortality. Subclinical carotid atherosclerosis is independently associated with rates of incident CV events among patients with RA. The complement system has been related to both the etiopathogenesis of RA and CV disease. In this study, we aimed to evaluate the association between a comprehensive assessment of the complement system and carotid intima media thickness and carotid plaque in patients with RA. Methods 430 patients with RA were recruited. Functional assays of the three pathways of the complement system, utilizing new-generation techniques, were assessed. Additionally, serum levels of individual components of the complement system belonging to the three pathways were measured: C1q (classical), lectin (lectin), C2, C4, and C4b (classical and lectin), factor D and properdin (alternative), C3 and C3a (common), C5, C5a, and C9 (terminal), as well as regulators factor I and C1-inhibitor. Subclinical carotid atherosclerosis was evaluated by ultrasonography. Multivariable linear regression analysis was conducted to investigate the association between the complement system and carotid intima media thickness and carotid plaque. Results After multivariable adjustment, which included traditional CV risk factors and disease-related data, C3a and C5a exhibited significant positive correlations with carotid intima media thickness. Additionally, higher values of C1-inhibitor, properdin, C3, C5, and C5a were independently associated with the presence of carotid plaque. Conclusion The complement system and subclinical carotid atherosclerosis are linked in patients with RA.

Published

2024

25. Sphingolipid Signaling and Complement Activation in Glioblastoma: A Promising Avenue for Therapeutic Intervention

Author

Alhaji H. Janneh

Subjects

glioblastoma, sphingolipids, complement system, tumor microenvironment, therapeutics, Therapeutics. Pharmacology, RM1-950, Biochemistry, QD415-436

Abstract

Glioblastoma is the most common and aggressive type of malignant brain tumor with a poor prognosis due to the lack of effective treatment options. Therefore, new treatment options are required. Sphingolipids are essential components of the cell membrane, while complement components are integral to innate immunity, and both play a critical role in regulating glioblastoma survival signaling. This review focuses on recent studies investigating the functional roles of sphingolipid metabolism and complement activation signaling in glioblastoma. It also discusses how targeting these two systems together may emerge as a novel therapeutic approach.

Published

2024

26. Unbiased Proteomic Exploration Suggests Overexpression of Complement Cascade Proteins in Plasma from Patients with Psoriasis Compared with Healthy Individuals.

Author

Kromann, Bjørn, Niu, Lili, Møller, Line B. P., Sølberg, Julie, Sulek, Karolina, Gyldenløve, Mette, Dyring-Andersen, Beatrice, Skov, Lone, and Løvendorf, Marianne B.

Subjects

*BLOOD proteins, *COMPLEMENT activation, *PERIOSTIN, *PROTEOMICS, *PSORIASIS

Abstract

Knowledge about the molecular mechanisms underlying the systemic inflammation observed in psoriasis remains incomplete. In this study, we applied mass spectrometry-based proteomics to compare the plasma protein levels between patients with psoriasis and healthy individuals, aiming to unveil potential systemically dysregulated proteins and pathways associated with the disease. Plasma samples from adult patients with moderate-to-severe psoriasis vulgaris (N = 59) and healthy age- and sex-matched individuals (N = 21) were analyzed using liquid chromatography–tandem mass spectrometry. Patients did not receive systemic anti-psoriatic treatment for four weeks before inclusion. A total of 776 protein groups were quantified. Of these, 691 were present in at least 60% of the samples, providing the basis for the downstream analysis. We identified 20 upregulated and 22 downregulated proteins in patients with psoriasis compared to controls (p < 0.05). Multiple proteins from the complement system were upregulated, including C2, C4b, C5, and C9, and pathway analysis revealed enrichment of proteins involved in complement activation and formation of the terminal complement complex. On the other end of the spectrum, periostin was the most downregulated protein in sera from patients with psoriasis. This comprehensive proteomic investigation revealed significantly elevated levels of complement cascade proteins in psoriatic plasma, which might contribute to increased systemic inflammation in patients with psoriasis. [ABSTRACT FROM AUTHOR]

Published

2024

27. Factor H-related protein 1 in systemic lupus erythematosus.

Author

Kleer, Jessica S., Klehr, Juliane, Dubler, Denise, Infanti, Laura, Chizzolini, Carlo, Huynh-Do, Uyen, Ribi, Camillo, and Trendelenburg, Marten

Subjects

SYSTEMIC lupus erythematosus, COMPLEMENT inhibition, COMPLEMENT activation, AUTOANTIBODIES, WESTERN immunoblotting

Abstract

Background: Factor H (FH) is a major soluble inhibitor of the complement system and part of a family comprising five related proteins (FHRs 1-5). Deficiency of FHR1 was described to be linked to an elevated risk of systemic lupus erythematosus (SLE). As FHR1 can partially antagonize the functionality of FH, an altered FHR1/FH ratio could not only enhance SLE vulnerability but also affect the disease expression. This study focuses on the analysis of FH and FHR1 at a protein level, and the occurrence of anti-FH autoantibodies (anti-FH) in a large cohort of SLE patients to explore their association with disease activity and/or expression. Methods: We assessed FH and FHR1 levels in plasma from 378 SLE patients compared to 84 healthy controls (normal human plasma, NHP), and sera from another cohort of 84 healthy individuals (normal human serum, NHS), using RayBio® CFH and CFHR1 ELISA kits. Patients were recruited by the Swiss SLE Cohort Study (SSCS). Unmeasurable FHR1 levels were all confirmed by Western blot, and in a subgroup of patients by PCR. Anti-FH were measured in SLE patients with non-detectable FHR1 levels and matched control patients using Abnova's CFH IgG ELISA kit. Results: Overall, FH and FHR1 levels were significantly higher in healthy controls, but there was no significant difference in FHR1/FH ratios between SLE patients and NHPs. However, SLE patients showed a significantly higher prevalence of undetectable FHR1 compared to all healthy controls (35/378 SLE patients versus 6/168 healthy controls; p= 0.0214, OR=2.751, 95% CI = 1.115 - 8.164), with a consistent trend across all ethnic subgroups. Levels of FH and FHR1, FHR1/FH ratios and absence of FHR1 were not consistently associated with disease activity and/or specific disease manifestations, but absence of FHR1 (primarily equivalent to CFHR1 deficiency) was linked to the presence of anti-FH in SLE patients (p=0.039). Conclusions: Deficiency of FHR1 is associated with a markedly elevated risk of developing SLE. A small proportion of FHR1-deficient SLE patients was found to have autoantibodies against FH but did not show clinical signs of microangiopathy. [ABSTRACT FROM AUTHOR]

Published

2024

28. Complement C3a/C3aR inhibition alleviates the formation of aortic aneurysm in Marfan syndrome mice.

Author

Zhang, Fan, Yao, Kexin, Liu, Yan, Zhou, Mei, Zhang, Yanhong, Hong, Shiyao, Wu, Jian, and Zhang, Congcong

Subjects

THORACIC aneurysms, ABDOMINAL aortic aneurysms, COMPLEMENT activation, AORTIC aneurysms, COMPLEMENT inhibition

Abstract

Mutations in fibrillin 1 (FBN1) is the main cause of Marfan syndrome (MFS) with thoracic aortic aneurysm (TAA) as the main complication. Activation of the complement system plays a key role in the formation of thoracic and abdominal aortic aneurysms. However, the role of the complement system in MFS-associated aortic aneurysms remains unclear. In this study, we observed increased levels of complement C3a and C5a in the plasma of MFS patients and mouse, and the increased deposition of the activated complement system product C3b/iC3b was also observed in the elastic fiber rupture zone of 3-month-old MFS mice. The expression of C3a receptor (C3aR) was increased in MFS aortas, and recombinant C3a promoted the expression of cytokines in macrophages. The administration of a C3aR antagonist (C3aRA) attenuated the development of thoracic aortic aneurysms in MFS mice. The increased inflammation response and matrix metalloproteinases activities were also attenuated by C3aRA treatment in MFS mice. Therefore, these findings indicate that the complement C3a/C3aR inhibition alleviates the formation of aortic aneurysm in Marfan syndrome mice. [ABSTRACT FROM AUTHOR]

Published

2024

29. Soluble terminal complement complex blood levels are elevated in schizophrenia.

Author

Savukoski, Susa, Mannes, Marco, Wohlgemuth, Lisa, Schultze, Anke, Guest, Paul C., Meyer-Lotz, Gabriela, Dobrowolny, Henrik, Relja, Borna, Huber-Lang, Markus, and Steiner, Johann

Subjects

*SCHIZOPHRENIA, *ENZYME-linked immunosorbent assay, *COMPLEMENT activation, *BLOOD serum analysis, *C-reactive protein

Abstract

The role of the complement system in schizophrenia (Sz) is inconclusive due to heterogeneity of the disease and study designs. Here, we assessed the levels of complement activation products and functionality of the classical pathway in acutely ill unmedicated Sz patients at baseline and after 6 weeks of treatment versus matched controls. The study included analyses of the terminal complement complex (sTCC) and C5a in plasma from 96 patients and 96 controls by enzyme-linked immunosorbent assay. Sub-group analysis of serum was conducted for measurement of C4 component and activity of the classical pathway (28 and 24 cases per cohort, respectively). We found no differences in levels of C5a, C4 and classical pathway function in patients versus controls. Plasma sTCC was significantly higher in patients [486 (392–659) ng/mL, n = 96] compared to controls [389 (304–612) ng/mL, n = 96] (p = 0.027, δ = 0.185), but not associated with clinical symptom ratings or treatment. The differences in sTCC between Sz and controls were confirmed using an Aligned Rank Transformation model considering the covariates age and sex (p = 0.040). Additional analysis showed that sTCC was significantly associated with C-reactive protein (CRP; p = 0.006). These findings suggest that sTCC plays a role in Sz as a trait marker of non-specific chronic immune activation, as previously described for CRP. Future longitudinal analyses with more sampling time points from early recognition centres for psychoses may be helpful to better understand the temporal dynamics of innate immune system changes during psychosis development. [ABSTRACT FROM AUTHOR]

Published

2024

30. Complete Description of the Three Pathways of the Complement System in a Series of 430 Patients with Rheumatoid Arthritis.

Author

Rodríguez-González, Dara, García-González, María, Gómez-Bernal, Fuensanta, Quevedo-Abeledo, Juan C., González-Rivero, Agustín F., Fernández-Cladera, Yolanda, González-López, Elena, Ocejo-Vinyals, J. Gonzalo, Jiménez-Sosa, Alejandro, González-Toledo, Beatriz, González-Gay, Miguel Á., and Ferraz-Amaro, Iván

Subjects

*ACUTE phase proteins, *RHEUMATOID factor, *COMPLEMENT activation, *C-reactive protein, *RHEUMATOID arthritis

Abstract

The complement (C) system is implicated in the etiopathogenesis of rheumatoid arthritis (RA). However, there is a lack of studies characterizing all three C pathways in RA patients. This study aimed to evaluate the association between an in-depth examination of the C system and RA patient characteristics, focusing on disease activity and the presence of rheumatoid factor and anti-citrullinated protein autoantibodies (ACPA). In a cohort of 430 RA patients, functional assays of the three C pathways (classical, alternative, and lectin) and serum levels of their components were assessed. Components included C1q (classical); factor D and properdin (alternative); lectin (lectin); C1-inhibitor; C2, C4, and C4b (classical and lectin); C3, C3a, and C4b (common); and C5, C5a, and C9 (terminal). A multivariable linear regression analysis showed significant positive correlations between C-reactive protein and C system proteins and functional assays, especially in the terminal and common pathways. Disease activity, measured by scores with or without acute phase reactants, positively correlated with the classical pathway functional test and terminal pathway products. Conversely, rheumatoid factor or ACPA presence was associated with lower classical pathway values and decreased C3a and C4b levels, suggesting complement depletion. In conclusion, RA disease activity increases C molecules and functional complement assays, while rheumatoid factor or ACPA positivity is linked to C consumption. Our study offers a detailed analysis of the complement system's role in RA, potentially guiding the development of more targeted and effective treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2024

31. The Establishment of Complement System Is from Gene Duplication and Domain Shuffling.

Author

Sun, Jiejie, Liu, Chang, Wang, Lingling, and Song, Linsheng

Subjects

*COMPLEMENT (Immunology), *COMPLEMENT activation, *CHROMOSOME duplication, *TUNICATA, *SPONGES (Invertebrates)

Abstract

The mammalian complement system constitutes a highly sophisticated body defense machinery. The evolutionary origin of the complement system can be traced to Coelenterata as the presence of the central component C3 and two activation proteases BF and MASP. In the present study, the main complement components were screened and analyzed from the genomes of different species in metazoan subphyla/phyla. C1q with classical domains can be traced to Annelida, and ficolin and MBL to Urochordata. C1r and C1s are only found in Chondrichthyes and even higher species, and MASP is traced to Coelenterata. In the evolutionary tree, C1r from Vertebrates is close to MASP1/2/3 from Deuterostomia and Coelenterata, and C1s from Vertebrates is close to MASP-like protease (MASPL) from Arthropoda, Mollusca, and Annelida. C2, BF, and DF can be traced to Mollusca, Coelenterata, and Porifera, respectively. There are no clear C2 and BF branches in the evolutionary tree. C3 can be traced to Coelenterata, and C4 and C5 are only in Chondrichthyes and even higher species. There are three clear C3, C4, and C5 branches in the evolutionary tree. C6-like (C6L) and C8 can be traced to Urochordata, and C7-like (C7L) can be traced to Cephalochordara. C6L, C7L, and C8 from Urochordata and Cephalochordara provide the structural conditions for the formation of Vertebrate MAC components. The findings unveil the evolutionary principles of the complement system and provide insight into its sophistication. [ABSTRACT FROM AUTHOR]

Published

2024

32. Serum amyloid P component: Structure, biological activity, and application in diagnosis and treatment of immune-associated diseases.

Author

Wang, Haixia, Nie, Yadan, Sun, Zuoli, He, Yi, and Yang, Jian

Subjects

*THERAPEUTICS, *AMYLOID, *TISSUE remodeling, *DIAGNOSIS, *NEUROBEHAVIORAL disorders, *CARDIOVASCULAR development

Abstract

Serum amyloid P component (SAP) is a member the innate immune humoral arm and participated in various processes, including the innate immune responses, tissue remodeling, and the pathogenesis of inflammatory diseases. Remarkably, SAP is a highly versatile immunomodulatory factor that can serve as a drug target for treating amyloid diseases and reduce inflammation, fibrosis degree, and respiratory disease. In this review, we focus on the biological activities of SAP and its application in different systemic immune-associated diseases. First, we reviewed the regulatory effects of SAP on innate immune cells and possible mechanisms. Second, we emphasized SAP as a diagnostic marker and therapeutic target for immune-associated diseases, including the neuropsychiatric disorders. Third, we presented several recommendations for regulating SAP in immune cell function and potential areas for future research. Some authorities consider SAP to be a pattern recognition molecule that plays multiple roles in the innate immune system and inflammation. Developing therapeutics that target SAP or its associated signaling pathways may be a promising strategy for treating immune-associated diseases. • This review highlights the effects of SAP as a multifunctional immunomodulator on inflammation, pathogenic infections, and tissue remodeling. • This review summarizes the use of SAP as a diagnostic marker and therapeutic target in immune-related diseases such as amyloidosis, fibrosis, cardiovascular, respiratory, and neuropsychiatric disorders. • This review presents the potential of SAP in the study of the mechanism of action in the central nervous system and hopes to carry out targeted interventions based on SAP. [ABSTRACT FROM AUTHOR]

Published

2024

33. Relationship between the complement system and serum lipid profile in patients with rheumatoid arthritis.

Author

Rodríguez-González, Dara, García-González, María, Gómez-Bernal, Fuensanta, Quevedo-Abeledo, Juan C., González-Rivero, Agustín F., Jiménez-Sosa, Alejandro, González-López, Elena, Heras-Recuero, Elena, Ocejo-Vinyals, J. Gonzalo, González-Gay, Miguel Á., and Ferraz-Amaro, Iván

Subjects

COMPLEMENT activation, BLOOD lipids, RHEUMATOID arthritis, COMPLEMENT (Immunology), LOW density lipoproteins, DYSLIPIDEMIA, ECULIZUMAB, LIPOPROTEIN A

Abstract

Background: The complement system has been linked to the etiopathogenesis of rheumatoid arthritis (RA). Patients with RA exhibit a dysregulated profile of lipid molecules, which has been attributed to the inflammation present in the disease. In this study, we aimed to evaluate the association between a comprehensive assessment of the complement system and the lipid profile of patients with RA. Methods: 430 patients with RA were recruited. New-generation techniques were employed to conduct functional assays of the three pathways of the complement system. Serum levels of various complement components such as C1q, factor D, properdin, lectin, C1-inhibitor, C2, C4, C4b, C3, C3a, C5, C5a, and C9 were assessed. Furthermore, a complete pattern of lipid molecules was measured including high (HDL), low-density lipoproteins (LDL), and lipoprotein (a). Multivariable linear regression analysis was conducted to investigate the association between the complement system and lipid profile in RA patients. Results: After multivariable analysis, several noteworthy associations emerged between the complement system and lipid molecules. Notably, complement components most strongly linked to the lipid profile were C1q and properdin, representing the upstream classical and alternative pathways, along with C3 from the common cascade. These associations demonstrated significance and positivity concerning total cholesterol, LDL, atherogenic index, apolipoprotein B, and lipoprotein(a), suggesting a connection with an unfavorable lipid profile. Interestingly, complement functional assays of the three pathways and activated products such as C3a and C5a showed no correlation with the lipid pattern. Conclusion: The correlation between the complement system and lipid molecule patterns is pronounced in patients with RA. This relationship is predominantly positive and primarily associated with upstream complement components rather than activated ones. [ABSTRACT FROM AUTHOR]

Published

2024

34. Dysregulated complement activation during acute myocardial infarction leads to endothelial glycocalyx degradation and endothelial dysfunction via the C5a:C5a-Receptor1 axis.

Author

Vahldieck, Carl, Löning, Samuel, Hamacher, Constantin, Fels, Benedikt, Rudzewski, Bettina, Nickel, Laura, Weil, Joachim, Nording, Henry, Baron, Lasse, Kleingarn, Marie, Karsten, Christian Marcel, and Kusche-Vihrog, Kristina

Subjects

MYOCARDIAL infarction, ENDOTHELIUM diseases, COMPLEMENT activation, ST elevation myocardial infarction, GLYCOCALYX

Abstract

Introduction: Complement-mediated damage to the myocardium during acute myocardial infarction (AMI), particularly the late components of the terminal pathway (C5-convertase and C5b-9), have previously been characterized. Unfortunately, only few studies have reported a direct association between dysregulated complement activation and endothelial function. Hence, little attention has been paid to the role of the anaphylatoxin C5a. The endothelial glycocalyx (eGC) together with the cellular actin cortex provide a vasoprotective barrier against chronic vascular inflammation. Changes in their nanomechanical properties (stiffness and height) are recognized as hallmarks of endothelial dysfunction as they correlate with the bioavailability of vasoactive substances, such as nitric oxide (NO). Here, we determined how the C5a:C5aR1 axis affects the eGC and endothelial function in AMI. Methods: Samples of fifty-five patients with ST-elevation myocardial infarction (STEMI) vs. healthy controls were analyzed in this study. eGC components and C5a levels were determined via ELISA; NO levels were quantified chemiluminescence-based. Endothelial cells were stimulated with C5a or patient sera (with/without C5a-receptor1 antagonist “PMX53”) and the nanomechanical properties of eGC quantified using the atomic force microscopy (AFM)-based nanoindentation technique. To measure actin cytoskeletal tension regulator activation (RhoA and Rac1) G-LISA assays were applied. Vascular inflammation was examined by quantifying monocyteendothelium interaction via AFM-based single-cell-force spectroscopy. Results: Serum concentrations of eGC components and C5a were significantly increased during STEMI. Serum and solely C5a stimulation decreased eGC height and stiffness, indicating shedding of the eGC. C5a enhanced RhoA activation, resulting in increased cortical stiffness with subsequent reduction in NO concentrations. Monocyte adhesion to the endothelium was enhanced after both C5a and stimulation with STEMI serum. eGC degradation- and RhoAinduced cortical stiffening with subsequent endothelial dysfunction were attenuated after administering PMX53. Conclusion: This study demonstrates that dysregulated C5a activation during AMI results in eGC damage with subsequent endothelial dysfunction and reduced NO bioavailability, indicating progressively developing vascular inflammation. This could be prevented by antagonizing C5aR1, highlighting the role of the C5a:C5a-Receptor1 axis in vascular inflammation development and endothelial dysfunction in AMI, offering new therapeutic approaches for future investigations. [ABSTRACT FROM AUTHOR]

Published

2024

35. Summary of the Therapeutic Options for Patients with Dry and Neovascular AMD.

Author

Śpiewak, Dorota, Drzyzga, Łukasz, Dorecka, Mariola, and Wyględowska-Promieńska, Dorota

Subjects

*MACULAR degeneration, *DRUG delivery systems, *ENDOTHELIAL growth factors, *STEM cell treatment, *INTRAVITREAL injections

Abstract

Age-related macular degeneration (AMD) is the leading cause of irreversible blindness worldwide and a severe medical and social problem. The steadily increasing number of patients is related to the aging of the population. So far, many factors affecting the development of AMD have been identified, which can be divided into non-modifiable, including genetic factors, age, and sex, and modifiable or environmental factors, such as smoking, poor diet, and hypertension. Early stages of age-related macular degeneration are characterized by fundus drusen and abnormalities in the retinal pigment epithelium. In late stages, geographic atrophy and choroidal neovascularization (CNV) are observed. The treatment of AMD, especially its advanced forms, is very challenging. Intensive research has made it possible to treat advanced stages of the dry form of AMD with pegcetacoplan and avacincaptad pegol, new drugs approved for use in the US. Pegcetacoplan targets the C3 and avacincaptad pegol targets the C5, the pivotal proteins of the complement cascade. The drugs are administered by intravitreal injection. The gold standard for neovascular AMD (nAMD) consists of intravitreal injections of anti-vascular endothelial growth factor (anti-VEGF) drugs such as bevacizumab, ranibizumab, aflibercept, brolucizumab, and faricimab. Treatment can be administered according to the fixed, pro-re-nata, and treat-and-extend regimens. The latter seems to have the best effect on improving visual acuity (VA) and the maximum therapeutic benefit. The search continues for the best ways to deliver intravitreal drugs. Current methods include sustained-release implants and hydrogel platforms for drug release, while the most promising future pathways for treating dry and nAMD are stem cell and gene therapy. [ABSTRACT FROM AUTHOR]

Published

2024

36. Proangiogenic properties of complement protein C1q can contribute to endometriosis.

Author

Agostinis, Chiara, Toffoli, Miriam, Zito, Gabriella, Balduit, Andrea, Pegoraro, Silvia, Spazzapan, Mariagiulia, Pascolo, Lorella, Romano, Federico, Di Lorenzo, Giovanni, Mangogna, Alessandro, Santin, Aurora, Spedicati, Beatrice, Valencic, Erica, Girotto, Giorgia, Ricci, Giuseppe, Kishore, Uday, and Bulla, Roberta

Subjects

ENDOMETRIOSIS, ENDOTHELIAL cells, UTERUS, COMPLEMENT activation, IMMUNOHISTOCHEMISTRY, PELVIC pain

Abstract

Endometriosis (EM) is defined as the engraftment and proliferation of functional endometrial-like tissue outside the uterine cavity, leading to a chronic inflammatory condition. While the precise etiology of EM remains elusive, recent studies have highlighted the crucial involvement of a dysregulated immune system. The complement system is one of the predominantly altered immune pathways in EM. Owing to its involvement in the process of angiogenesis, here, we have examined the possible role of the first recognition molecule of the complement classical pathway, C1q. C1q plays seminal roles in several physiological and pathological processes independent of complement activation, including tumor growth, placentation, wound healing, and angiogenesis. Gene expression analysis using the publicly available data revealed that C1q is expressed at higher levels in EM lesions compared to their healthy counterparts. Immunohistochemical analysis confirmed the presence of C1q protein, being localized around the blood vessels in the EM lesions. CD68+ macrophages are the likely producer of C1q in the EM lesions since cultured EM cells did not produce C1q in vitro. To explore the underlying reasons for increased C1q expression in EM, we focused on its established pro-angiogenic role. Employing various angiogenesis assays on primary endothelial endometriotic cells, such as migration, proliferation, and tube formation assays, we observed a robust proangiogenic effect induced by C1q on endothelial cells in the context of EM. C1q promoted angiogenesis in endothelial cells isolated from EM lesions (as well as healthy ovary that is also rich in C1q). Interestingly, endothelial cells from EM lesions seem to overexpress the receptor for the globular heads of C1q (gC1qR), a putative C1q receptor. Experiments with siRNA to silence gC1qR resulted in diminished capacity of C1q to perform its angiogenic functions, suggesting that C1q is likely to engage gC1qR in the pathophysiology of EM. gC1qR can be a potential therapeutic target in EM patients that will disrupt C1q-mediated proangiogenic activities in EM. [ABSTRACT FROM AUTHOR]

Published

2024

37. Mannose Binding Lectin and C3 Serum Levels in Coronary Artery Disease: A Cross-Sectional Study.

Author

Meneghetti da Rosa, Juliana, Lidani, Kárita Cláudia Freitas, Andrade, Fabiana Antunes, Sena, Léia, Nisihara, Renato, Ambrosio, Altair Rogerio, and Messias-Reason, Iara J.

Subjects

*CORONARY artery disease, *CARDIOVASCULAR diseases risk factors, *CORONARY angiography, *COMPLEMENT activation, *BODY mass index

Abstract

Background: The process of tissue injury in coronary artery disease (CAD) has been associated with activation of the complement system, partly due to the action of mannose-binding lectin (MBL) and C3, which are expressed in atherosclerotic lesions. Objective: The aim of this study was to evaluate the serum levels of MBL and C3 in patients with CAD and to compare them with healthy controls. Additionally, we aim to assess the correlation between MBL and C3 levels and cardiometabolic parameters. Methods: MBL and C3 serum concentration were determined by ELISA and immunoturbidimetry, respectively, in up to 119 patients undergoing coronary angiography for CAD evaluation, comprising 48 individuals diagnosed with acute myocardial infarction (MI) and 71 without MI. A total of 93 paired healthy controls were included in the study. Results: Individuals with CAD had MBL serum concentration higher than controls (p =.002), regardless of the presence of MI (p =.006). In addition, high concentration of MBL (>2000 ng/mL) was more frequent in patients with CAD (p =.007; OR = 2.6; 95% CI = 1.3–5.1). C3 levels were not significantly associated with any of the patient groups but were positively correlated with cardiometabolic parameters such as body mass index (BMI) and triglycerides levels. Conclusions: Higher concentrations of MBL were found to be associated with CAD, whereas C3 levels were found to be associated with cardiovascular risk factors. [ABSTRACT FROM AUTHOR]

Published

2024

38. The complement system and diabetic retinopathy.

Author

Jiang, Feipeng, Lei, Chunyan, Chen, Yingying, Zhou, Nenghua, and Zhang, Meixia

Subjects

*COMPLEMENT activation, *DIABETIC retinopathy, *DIABETES complications, *MILITARY invasion, *MICROBIAL invasiveness, *VISION disorders

Abstract

Diabetic retinopathy (DR) is one of the common microvascular complications of diabetes mellitus and is the main cause of visual impairment in diabetic patients. The pathogenesis of DR is still unclear. The complement system, as an important component of the innate immune system in addition to defending against the invasion of foreign microorganisms, is involved in the occurrence and development of DR through 3 widely recognized complement activation pathways, the complement regulatory system, and many other pathways. Molecules such as C3a, C5a, and membrane attacking complex, as important molecules of the complement system, are involved in the pathologenesus of DR, either through direct damaging effects or by activating cells (microglia, macroglia, etc.) in the retinal microenvironment to contribute to the pathological damage of DR indirectly. We review the integral association of the complement system and DR to further understand the pathogenesis of DR and possibly provide a new strategy for itstreatment. [ABSTRACT FROM AUTHOR]

Published

2024

39. Elevated expression of complement factor I in lung cancer cells associates with shorter survival–Potentially via non-canonical mechanism.

Author

Felberg, Anna, Bieńkowski, Michał, Stokowy, Tomasz, Myszczyński, Kamil, Polakiewicz, Zuzanna, Kitowska, Kamila, Sądej, Rafał, Mohlin, Frida, Kuźniewska, Alicja, Kowalska, Daria, Stasiłojć, Grzegorz, Jongerius, Ilse, Spaapen, Robbert, Mesa-Guzman, Miguel, Montuenga, Luis M., Blom, Anna M., Pio, Ruben, and Okrój, Marcin

Abstract

While numerous membrane-bound complement inhibitors protect the body's cells from innate immunity's autoaggression, soluble inhibitors like complement factor I (FI) are rarely produced outside the liver. Previously, we reported the expression of FI in non-small cell lung cancer (NSCLC) cell lines. Now, we assessed the content of FI in cancer biopsies from lung cancer patients and associated the results with clinicopathological characteristics and clinical outcomes. Immunohistochemical staining intensity did not correlate with age, smoking status, tumor size, stage, differentiation grade, and T cell infiltrates, but was associated with progression-free survival (PFS), overall survival (OS) and disease-specific survival (DSS). Multivariate Cox analysis of low vs. high FI content revealed HR 0.55, 95 % CI 0.32-0.95, p=0.031 for PFS, HR 0.51, 95 % CI 0.25-1.02, p=0.055 for OS, and HR 0.32, 95 % CI 0.12-0.84, p=0.021 for DSS. Unfavorable prognosis might stem from the non-canonical role of FI, as the staining pattern did not correlate with C4d - the product of FI-supported degradation of active complement component C4b. To elucidate that, we engineered three human NSCLC cell lines naturally expressing FI with CRISPR/Cas9 technology, and compared the transcriptome of FI-deficient and FI-sufficient clones in each cell line. RNA sequencing revealed differentially expressed genes engaged in intracellular signaling pathways controlling proliferation, apoptosis, and responsiveness to growth factors. Moreover, in vitro colony-formation assays showed that FI-deficient cells formed smaller foci than FI-sufficient NSCLC cells, but their size increased when purified FI protein was added to the medium. We postulate that a non-canonical activity of FI influences cellular physiology and contributes to the poor prognosis of lung cancer patients. [ABSTRACT FROM AUTHOR]

Published

2024

40. Anti-C1q antibodies: a biomarker for diagnosis and management of lupus nephritis. A narrative review.

Author

Calatroni, Marta, Moroni, Gabriella, Conte, Emanuele, Stella, Matteo, Reggiani, Francesco, and Ponticelli, Claudio

Subjects

LUPUS nephritis, DIAGNOSIS, IMMUNOGLOBULINS, KIDNEY physiology, BIOMARKERS, KIDNEY diseases

Abstract

Nephritis is a frequent and severe complication of Systemic Lupus Erythematous (SLE). The clinical course of lupus nephritis (LN) is usually characterized by alternating phases of remission and exacerbation. Flares of LN can lead to deterioration of kidney function, necessitating timely diagnosis and therapy. The presence of autoantibodies against C1q (anti-C1qAb) in the sera of SLE patients has been reported in various studies. Some research suggests that the presence and changes in the titer of anti-C1qAb may be associated with the development of LN, as well as with LN activity and renal flares. However, the exact role of anti-C1qAb in LN remains a subject of debate. Despite variability in the results of published studies, anti-C1qAb hold promise as noninvasive markers for assessing LN activity in SLE patients. Measuring anti-C1qAb levels could aid in diagnosing and managing LN during periods of both inactive disease and renal flares. Nevertheless, larger controlled trials with standardized laboratory assays are necessary to further establish the utility of anti-C1qAb in predicting the reactivation and remission of LN and guiding treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2024

41. Systematic review of the complement components as potential biomarkers of pre-eclampsia: pitfalls and opportunities.

Author

Balduit, Andrea, Agostinis, Chiara, Mangogna, Alessandro, Zito, Gabriella, Stampalija, Tamara, Ricci, Giuseppe, and Bulla, Roberta

Abstract

The complement system (C) is a crucial component of the innate immune system. An increasing body of research has progressively shed light on the pivotal role of C in immunological tolerance at the feto-maternal interface. Excessive C activation or impaired C regulation may determine the onset of pregnancy-related pathological conditions, including pre-eclampsia (PE). Thus, several studies have investigated the presence of C components or split products in blood matrixes (i.e., plasma, serum), urine, and amniotic fluid in PE. In the current study, we systematically reviewed the currently available scientific literature reporting measurements of C components as circulating biomarkers in PE, based on a literature search using Pubmed, Scopus, and Embase databases. A total of 41 out of 456 studies were selected after full-text analysis. Fourteen studies (34.1%) were identified as measuring the blood concentrations of the classical pathway, 5 (12.1%) for the lectin pathway, 28 (68.3%) for the alternative pathway, 17 (41.5%) for the terminal pathway components, and 16 (39%) for C regulators. Retrieved results consistently reported C4, C3, and factor H reduction, and increased circulating levels of C4d, Bb, factor D, C3a, C5a, and C5b-9 in PE compared to normal pregnancies, depicting an overall scenario of excessive C activation and aberrant C regulation. With evidence of C activation and dysregulation, C-targeted therapy is an intriguing perspective in PE management. Moreover, we also discussed emerging pitfalls in C analysis, mainly due to a lack of experimental uniformity and biased cohort selection among different studies and laboratories, aiming to raise a more comprehensive awareness for future standardization. [ABSTRACT FROM AUTHOR]

Published

2024

42. Revisiting the interaction between complement lectin pathway protease MASP-2 and SARS-CoV-2 nucleoprotein.

Author

Bally, Isabelle, Drumont, Guillaume, Rossi, Véronique, Guseva, Serafima, Botova, Maiia, Reiser, Jean-Baptiste, Thépaut, Michel, Dylon, Sebastian Dergan, Dumestre-Pérard, Chantal, Gaboriaud, Christine, Fieschi, Franck, Blackledge, Martin, Poignard, Pascal, and Thielens, Nicole M.

Subjects

SARS-CoV-2, VIRAL proteins, CATALYTIC domains, PROTEIN domains, COMPLEMENT activation, ECULIZUMAB, LECTINS, IMMUNE reconstitution inflammatory syndrome

Abstract

Complement activation is considered to contribute to the pathogenesis of severe SARS-CoV-2 infection, mainly by generating potent immune effector mechanisms including a strong inflammatory response. Involvement of the lectin complement pathway, a major actor of the innate immune anti-viral defense, has been reported previously. It is initiated by recognition of the viral surface Spike glycoprotein by mannose-binding lectin (MBL), which induces activation of the MBL-associated protease MASP-2 and triggers the proteolytic complement cascade. A role for the viral nucleoprotein (N) has also been reported, through binding to MASP-2, leading to protease overactivation and potentiation of the lectin pathway. In the present study, we reinvestigated the interactions of the SARS-CoV-2 N protein, produced either in bacteria or secreted by mammalian cells, with full-length MASP-2 or its catalytic domain, in either active or proenzyme form. We could not confirm the interaction of the N protein with the catalytic domain of MASP-2 but observed N protein binding to proenzyme MASP-2. We did not find a role of the N protein in MBL-mediated activation of the lectin pathway. Finally, we showed that incubation of the N protein with MASP-2 results in proteolysis of the viral protein, an observation that requires further investigation to understand a potential functional significance in infected patients. [ABSTRACT FROM AUTHOR]

Published

2024

43. Targeting autoimmune mechanisms by precision medicine in Myasthenia Gravis.

Author

Cavalcante, Paola, Mantegazza, Renato, and Antozzi, Carlo

Subjects

MYASTHENIA gravis, INDIVIDUALIZED medicine, COMPLEMENT activation, MYONEURAL junction, B cells, AUTOIMMUNE diseases

Abstract

Myasthenia Gravis (MG) is a chronic disabling autoimmune disease caused by autoantibodies to the neuromuscular junction (NMJ), characterized clinically by fluctuating weakness and early fatigability of ocular, skeletal and bulbar muscles. Despite being commonly considered a prototypic autoimmune disorder, MG is a complex and heterogeneous condition, presenting with variable clinical phenotypes, likely due to distinct pathophysiological settings related with different immunoreactivities, symptoms' distribution, disease severity, age at onset, thymic histopathology and response to therapies. Current treatment of MG based on international consensus guidelines allows to effectively control symptoms, but most patients do not reach complete stable remission and require life-long immunosuppressive (IS) therapies. Moreover, a proportion of them is refractory to conventional IS treatment, highlighting the need for more specific and tailored strategies. Precision medicine is a new frontier of medicine that promises to greatly increase therapeutic success in several diseases, including autoimmune conditions. In MG, B cell activation, antibody recycling and NMJ damage by the complement system are crucial mechanisms, and their targeting by innovative biological drugs has been proven to be effective and safe in clinical trials. The switch from conventional IS to novel precision medicine approaches based on these drugs could prospectively and significantly improve MG care. In this review, we provide an overview of key immunopathogenetic processes underlying MG, and discuss on emerging biological drugs targeting them. We also discuss on future direction of research to address the need for patients' stratification in endotypes according with genetic and molecular biomarkers for successful clinical decision making within precision medicine workflow. [ABSTRACT FROM AUTHOR]

Published

2024

44. The potential application of complement inhibitors-loaded nanosystem for autoimmune diseases via regulation immune balance.

Author

Wei, Yaya, Guo, Jueshuo, Meng, Tingting, Gao, Ting, Mai, Yaping, Zuo, Wenbao, and Yang, Jianhong

Subjects

*AUTOIMMUNE diseases, *COMPLEMENT inhibition, *ECULIZUMAB, *COMPLEMENT activation, *INFLAMMATORY mediators, *IMMUNE system

Abstract

The complement is an important arm of the innate immune system, once activated, the complement system rapidly generates large quantities of protein fragments that are potent mediators of inflammation. Recent studies have shown that over-activated complement is the main proinflammatory system of autoimmune diseases (ADs). In addition, activated complements interact with autoantibodies, immune cells exacerbate inflammation, further worsening ADs. With the increasing threat of ADs to human health, complement-based immunotherapy has attracted wide attention. Nevertheless, efficient and targeted delivery of complement inhibitors remains a significant challenge owing to their inherent poor targeting, degradability, and low bioavailability. Nanosystems offer innovative solutions to surmount these obstacles and amplify the potency of complement inhibitors. This prime aim to present the current knowledge of complement in ADs, analyse the function of complement in the pathogenesis and treatment of ADs, we underscore the current situation of nanosystems assisting complement inhibitors in the treatment of ADs. Considering technological, physiological, and clinical validation challenges, we critically appraise the challenges for successfully translating the findings of preclinical studies of these nanosystem assisted-complement inhibitors into the clinic, and future perspectives were also summarised. (The graphical abstract is by BioRender.) Nanosystem-assisted complement inhibitor strategy. (By BioRender.) [ABSTRACT FROM AUTHOR]

Published

2024

45. Double-Edged Sword: Exploring the Mitochondria–Complement Bidirectional Connection in Cellular Response and Disease.

Author

Lin, Jingfei, Hwang, Sinwoo, Luo, Honglin, and Mohamud, Yasir

Subjects

*COMPLEMENT activation, *CIRCULAR DNA, *ALZHEIMER'S disease, *IMMUNE complexes, *BACTERIAL cells, *MITOCHONDRIAL membranes, *PLANT mitochondria

Abstract

Simple Summary: Complement system is an ancient immune pathway that protects us against harmful invaders. Meanwhile, mitochondria, widely known as the powerhouse of the cell, are essential for producing energy and maintaining healthy cells. Bridging past and present studies, this review aims to elucidate an underexplored yet essential connection between the complement system and mitochondria. These interactions are implicated in different diseases across various tissues and organs, such as Alzheimer's disease and cancer, that are in critical need of cure. Mitochondria release signals that impact the activation of the complement system, leading to tissue damage and inflammation; while the complement system alters mitochondrial functions, forming a vicious cycle. This cycle exacerbates disease progression and health outcomes. We hope to highlight potential targets to alleviate societal healthcare burdens by bringing scientists' attention to this novel bidirectional interaction. Mitochondria serve an ultimate purpose that seeks to balance the life and death of cells, a role that extends well beyond the tissue and organ systems to impact not only normal physiology but also the pathogenesis of diverse diseases. Theorized to have originated from ancient proto-bacteria, mitochondria share similarities with bacterial cells, including their own circular DNA, double-membrane structures, and fission dynamics. It is no surprise, then, that mitochondria interact with a bacterium-targeting immune pathway known as a complement system. The complement system is an ancient and sophisticated arm of the immune response that serves as the body's first line of defense against microbial invaders. It operates through a complex cascade of protein activations, rapidly identifying and neutralizing pathogens, and even aiding in the clearance of damaged cells and immune complexes. This dynamic system, intertwining innate and adaptive immunity, holds secrets to understanding numerous diseases. In this review, we explore the bidirectional interplay between mitochondrial dysfunction and the complement system through the release of mitochondrial damage-associated molecular patterns. Additionally, we explore several mitochondria- and complement-related diseases and the potential for new therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024

46. A 21‐bp deletion in the complement regulator CD55 promotor region is associated with multifocal motor neuropathy and its disease course.

Author

Bos, Jeroen W., Groen, Ewout J. N., Otten, Henny G., Budding, Kevin, van Eijk, Ruben P. A., Curial, Chantall, Kardol‐Hoefnagel, Tineke, Goedee, H. Stephan, van den Berg, Leonard H., and van der Pol, W. Ludo

Subjects

*COMPLEMENT (Immunology), *PROMOTERS (Genetics), *DESCRIPTIVE statistics, *GENETIC polymorphisms, *MEMBRANE glycoproteins, *POLYNEUROPATHIES, *COMPARATIVE studies, *CONFIDENCE intervals, *MOTOR neuron diseases, *SEQUENCE analysis, *GENOTYPES

Abstract

Background and Aims: To further substantiate the role of antibody‐mediated complement activation in multifocal motor neuropathy (MMN) immunopathology, we investigated the distribution of promotor polymorphisms of genes encoding the membrane‐bound complement regulators CD46, CD55, and CD59 in patients with MMN and controls, and evaluated their association with disease course. Methods: We used Sanger sequencing to genotype five common polymorphisms in the promotor regions of CD46, CD55, and CD59 in 133 patients with MMN and 380 controls. We correlated each polymorphism to clinical parameters. Results: The genotype frequencies of rs28371582, a 21‐bp deletion in the CD55 promotor region, were altered in patients with MMN as compared to controls (p.009; Del/Del genotype 16.8% vs. 7.7%, p.005, odds ratio: 2.43 [1.27–4.58]), and patients carrying this deletion had a more favorable disease course (mean difference 0.26 Medical Research Council [MRC] points/year; 95% confidence interval [CI]: 0.040–0.490, p.019). The presence of CD59 rs141385724 was associated with less severe pre‐diagnostic disease course (mean difference 0.940 MRC point/year; 95% CI: 0.083–1.80, p.032). Interpretation: MMN susceptibility is associated with a 21‐bp deletion in the CD55 promotor region (rs2871582), which is associated with lower CD55 expression. Patients carrying this deletion may have a more favorable long‐term disease outcome. Taken together, these results point out the relevance of the pre‐C5 level of the complement cascade in the inflammatory processes underlying MMN. [ABSTRACT FROM AUTHOR]

Published

2024

47. Sphingolipid Signaling and Complement Activation in Glioblastoma: A Promising Avenue for Therapeutic Intervention.

Author

Janneh, Alhaji H.

Subjects

*SPHINGOLIPIDS, *GLIOBLASTOMA multiforme, *BRAIN tumors, *PROGNOSIS, *CELL membranes

Abstract

Glioblastoma is the most common and aggressive type of malignant brain tumor with a poor prognosis due to the lack of effective treatment options. Therefore, new treatment options are required. Sphingolipids are essential components of the cell membrane, while complement components are integral to innate immunity, and both play a critical role in regulating glioblastoma survival signaling. This review focuses on recent studies investigating the functional roles of sphingolipid metabolism and complement activation signaling in glioblastoma. It also discusses how targeting these two systems together may emerge as a novel therapeutic approach. [ABSTRACT FROM AUTHOR]

Published

2024

48. The complement system in the pathogenesis and progression of kidney diseases: What doesn't kill you makes you older.

Author

Stea, Emma Diletta, D'Ettorre, Giuseppina, Mitrotti, Adele, and Gesualdo, Loreto

Subjects

*COMPLEMENT activation, *HEMOLYTIC-uremic syndrome, *DISEASE progression, *COMPLEMENT inhibition, *GLOMERULONEPHRITIS

Abstract

The Complement System is an evolutionarily conserved component of immunity that plays a key role in host defense against infections and tissue homeostasis. However, the dysfunction of the Complement System can result in tissue damage and inflammation, thereby contributing to the development and progression of various renal diseases, ranging from atypical Hemolytic Uremic Syndrome to glomerulonephritis. Therapeutic interventions targeting the complement system have demonstrated promising results in both preclinical and clinical studies. Currently, several complement inhibitors are being developed for the treatment of complement-mediated renal diseases. This review aims to summarize the most recent insights into complement activation and therapeutic inhibition in renal diseases. Furthermore, it offers potential directions for the future rational use of complement inhibitor drugs in the context of renal diseases. [ABSTRACT FROM AUTHOR]

Published

2024

49. The Complement System as a Therapeutic Target in Retinal Disease.

Author

Ong, Joshua, Zarnegar, Arman, Selvam, Amrish, Driban, Matthew, and Chhablani, Jay

Subjects

COMPLEMENT activation, RETINAL diseases, DIABETIC retinopathy, COMPLEMENT inhibition, MACULAR degeneration, HUMAN body

Abstract

The complement cascade is a vital system in the human body's defense against pathogens. During the natural aging process, it has been observed that this system is imperative for ensuring the integrity and homeostasis of the retina. While this system is critical for proper host defense and retinal integrity, it has also been found that dysregulation of this system may lead to certain retinal pathologies, including geographic atrophy and diabetic retinopathy. Targeting components of the complement system for retinal diseases has been an area of interest, and in vivo, ex vivo, and clinical trials have been conducted in this area. Following clinical trials, medications targeting the complement system for retinal disease have also become available. In this manuscript, we discuss the pathophysiology of complement dysfunction in the retina and specific pathologies. We then describe the results of cellular, animal, and clinical studies targeting the complement system for retinal diseases. We then provide an overview of complement inhibitors that have been approved by the Food and Drug Administration (FDA) for geographic atrophy. The complement system in retinal diseases continues to serve as an emerging therapeutic target, and further research in this field will provide additional insights into the mechanisms and considerations for treatment of retinal pathologies. [ABSTRACT FROM AUTHOR]

Published

2024

50. The dysfunction of complement and coagulation in diseases: the implications for the therapeutic interventions

Author

Honghong Jiang, Yiming Guo, Qihang Wang, Yiran Wang, Dingchuan Peng, Yigong Fang, Lei Yan, Zhuolin Ruan, Sheng Zhang, Yong Zhao, Wendan Zhang, Wei Shang, and Zhichun Feng

Subjects

coagulation, complement system, immune response, inflammatory network, sepsis, Medicine

Abstract

Abstract The complement system, comprising over 30 proteins, is integral to the immune system, and the coagulation system is critical for vascular homeostasis. The activation of the complement and coagulation systems involves an organized proteolytic cascade, and the overactivation of these systems is a central pathogenic mechanism in several diseases. This review describes the role of complement and coagulation system activation in critical illness, particularly sepsis. The complexities of sepsis reveal significant knowledge gaps that can be compared to a profound abyss, highlighting the urgent need for further investigation and exploration. It is well recognized that the inflammatory network, coagulation, and complement systems are integral mechanisms through which multiple factors contribute to increased susceptibility to infection and may result in a disordered immune response during septic events in patients. Given the overlapping pathogenic mechanisms in sepsis, immunomodulatory therapies currently under development may be particularly beneficial for patients with sepsis who have concurrent infections. Herein, we present recent findings regarding the molecular relationships between the coagulation and complement pathways in the advancement of sepsis, and propose potential intervention targets related to the crosstalk between coagulation and complement, aiming to provide more valuable treatment of sepsis.

Published

2024