Your search keyword '"eculizumab"' showing total 7,743 results

51. Eculizumab in Hypertensive Emergency-associated Hemolytic Uremic Syndrome (HYPERSHU)

Published

2024

52. Therapeutic challenges and unmet needs in the management of myasthenia gravis: an Italian expert opinion.

Author

Mantegazza, Renato, Saccà, Francesco, Antonini, Giovanni, Bonifati, Domenico Marco, Evoli, Amelia, Habetswallner, Francesco, Liguori, Rocco, Pegoraro, Elena, Rodolico, Carmelo, Schenone, Angelo, Sgarzi, Manlio, and Pappagallo, Giovanni

Subjects

*CHOLINERGIC receptors, *THERAPEUTICS, *PROTEIN-tyrosine kinases, *IMMUNOSUPPRESSIVE agents, *COMPLEMENT activation, *ECULIZUMAB, *MYASTHENIA gravis, *OFF-label use (Drugs)

Abstract

Myasthenia gravis (MG) is a rare, autoimmune, neurological disorder. Most MG patients have autoantibodies against acetylcholine receptors (AChRs). Some have autoantibodies against muscle-specific tyrosine kinase (MuSK) or lipoprotein-receptor-related protein 4 (LRP4), and some are seronegative. Standard of care, which includes anti-cholinesterase drugs, thymectomy, corticosteroids (CS), and off-label use of non-steroidal immunosuppressive drugs (NSISTs), is bounded by potential side effects and limited efficacy in refractory generalized MG (gMG) patients. This highlights the need for new therapeutic approaches for MG. Eculizumab, a monoclonal antibody that inhibits the complement system, has been recently approved in Italy for refractory gMG. A panel of 11 experts met to discuss unmet therapeutic needs in the acute and chronic phases of the disease, as well as the standard of care for refractory patients. Survival was emphasized as an acute phase outcome. In the chronic phase, persistent remission and early recognition of exacerbations to prevent myasthenic crisis and respiratory failure were considered crucial. Refractory patients require treatments with fast onset of action, improved tolerability, and the ability to slow disease progression and increase life expectancy. The Panel agreed that eculizumab would presumably meet the therapeutic needs of many refractory gMG patients. The panel concluded that the unmet needs of current standard of care treatments for gMG are significant. Evaluating new therapeutic options accurately is essential to find the best balance between efficacy and tolerability for each patient. Collecting real-world data on novel molecules in routine clinical practice is necessary to address unmet needs. [ABSTRACT FROM AUTHOR]

Published

2024

53. Protein-losing enteropathy as a new phenotype in atypical hemolytic uremic syndrome caused by CD46 gene mutation.

Author

Wang, Chunyan, Chen, Jing, Han, Xinli, Sun, Manqing, Fang, Xiaoyan, Zhai, Yihui, Miao, Qianfan, Zhang, Zhiqing, Tang, Xiaoshan, Liu, Jiaojiao, Shen, Qian, and Xu, Hong

Subjects

*THERAPEUTIC use of monoclonal antibodies, *PROTEIN-losing enteropathy, *HEMOLYTIC-uremic syndrome, *GENE expression, *MOLECULAR structure, *DRUG efficacy, *GENETIC mutation, *PHENOTYPES, *GENETIC testing

Abstract

Background: Atypical hemolytic uremic syndrome (aHUS) is a life-threatening thrombotic microangiopathy. Genetic defects in the alternative complement (AP) pathway have been identified in 60–70% of individuals. Eculizumab is recommended as a first-line therapy. Methods: We collected the clinical data of a pediatric patient with aHUS accompanied by protein-losing enteropathy (PLE). Genetic testing was performed. Related literature on aHUS combined with PLE was reviewed. Results: A 15-year-old Chinese girl was diagnosed with aHUS at 3.7 years of age and experienced five episodes; her symptoms completely resolved with plasma treatment. Severe gastrointestinal symptoms and hypoalbuminemia presented after the first episode, and PLE was diagnosed. A novel homozygous CD46 variant was identified, and FACS revealed significantly decreased CD46 expression. She presented at a recent relapse with persistent GI symptoms and headache and progressed to chronic kidney failure; peritoneal dialysis was initiated. Eculizumab was given 8 months after the last recurrence. Surprisingly, PLE was cured. Afterward, dialysis was discontinued, and eGFR recovered to 44.8 ml/min/1.73 m2. A review of the literature indicated that PLE with thrombosis was caused by CD55 variants via hyperactivation of the AP system. We report an aHUS patient with PLE caused by CD46 variants. Symptoms of both PLE and aHUS were significantly alleviated in our patient and patients with CD55 variants treated with eculizumab, indicating that PLE was a new symptom of aHUS in our patient with a CD46 variant. Conclusions: Our case expands the phenotype of aHUS caused by a CD46 mutation and provides evidence of the efficacy of eculizumab after a long phase of chronic kidney failure. [ABSTRACT FROM AUTHOR]

Published

2024

54. Risk–Benefit Analysis of Novel Treatments for Patients with Generalized Myasthenia Gravis.

Author

Smith, A. Gordon, Wolfe, Gil I., Habib, Ali A., Qi, Cynthia Z., Yang, Hongbo, Du, Mandy, Chen, Xin, Gelinas, Deborah, Brauer, Edward, Phillips, Glenn, and Saccà, Francesco

Abstract

Introduction: This study used network meta-analysis (NMA) to inform and compare the number needed to treat (NNT), number needed to harm (NNH), and cost per improved outcome (CPIO) associated with more recently approved treatments for anti-acetylcholine receptor antibody-positive (anti-AChR Ab+) generalized myasthenia gravis (gMG). Methods: Clinical trials of neonatal Fc receptor (FcRn) inhibitors, efgartigimod intravenous (IV) and rozanolixizumab, and complement inhibitors, ravulizumab and zilucoplan, versus placebo (with background conventional treatment) were included in the primary NMA to compare efficacy and safety outcomes. The outputs from the NMAs were used to estimate NNT and NNH of each treatment versus placebo. CPIO (2024 USD) was estimated for a ≥ 3- or ≥ 5-point reduction from baseline in Quantitative Myasthenia Gravis (QMG) and Myasthenia Gravis-Activities of Daily Living (MG-ADL) scores. Sensitivity analyses were performed adding efgartigimod PH20 subcutaneous (SC) and eculizumab to the NMA. Results: Efgartigimod IV had the lowest NNT versus placebo for achieving a ≥ 3- and ≥ 5-point reduction in QMG, as well as a ≥ 5-point reduction in MG-ADL, whereas rozanolixizumab had the lowest NNT for a ≥ 3-point reduction in MG-ADL. The NNH versus placebo was similar across comparator treatments. Efgartigimod IV had the lowest CPIO among all treatments for all assessed efficacy outcomes. Sensitivity analyses yielded results consistent with primary analysis and indicated that efgartigimod PH20 SC had comparable NNT and CPIO values to efgartigimod IV, whereas eculizumab had comparable NNT and higher CPIO values compared to other complement inhibitors. Conclusions: FcRn inhibitors and complement inhibitors assessed in this study all demonstrated clinical benefit in terms of NNT as well as an acceptable safety profile in terms of NNH. Within the limitations of this meta-analysis, efgartigimod was associated with a favorable benefit–risk profile as well as a better economic value compared to ravulizumab, rozanolixizumab, and zilucoplan as treatments for anti-AChR Ab+ gMG. [ABSTRACT FROM AUTHOR]

Published

2024

55. Annual trends in atypical haemolytic uremic syndrome management in Japan and factors influencing early diagnosis and treatment: a retrospective study

Author

Yoshitaka Tatematsu, Takahiro Imaizumi, Nobuaki Michihata, Noritoshi Kato, Ryosuke Kumazawa, Hiroki Matsui, Kiyohide Fushimi, Hideo Yasunaga, and Shoichi Maruyama

Subjects

Atypical haemolytic uremic syndrome (aHUS), Thrombotic microangiopathy (TMA), Eculizumab, Plasma exchange, A disintegrin-like and metalloproteinase with thrombospondin type 1 motifs 13 (ADAMTS13), Thrombocytopenia, Medicine, Science

Abstract

Abstract Atypical haemolytic uremic syndrome (aHUS) is a rare disorder characterised by complement-mediated thrombotic microangiopathy (TMA). Despite clinical guidelines, the diagnosis and treatment of aHUS in its early stages remains challenging. This study examined the annual trends in aHUS clinical practices in Japan and explored factors influencing early diagnosis and treatment. Using data from the 2011–2020 Diagnosis Procedure Combination database, 3096 cases with the HUS disease code were identified, of which 217 were confirmed as aHUS and treated with eculizumab or plasma exchange. Early initiation, defined as starting eculizumab or plasma exchange within 7 days of admission, was the focus of the study. Our study revealed no significant changes over time in the number of aHUS diagnoses, cases treated with eculizumab, or early initiation cases. Early initiation cases underwent haemodialysis earlier and had ADAMTS13 activity measured earlier, shorter hospital stays, and lower hospitalisation costs than late initiation cases. In conclusion, we found no increase in the number of newly diagnosed aHUS cases or early treatment initiation over time. Early recognition of TMA and differentiation of the causative disease are crucial for identifying potential aHUS cases, which may lead to better patient prognoses.

Published

2024

56. Clinical efficacy and safety of switching from eculizumab to ravulizumab in adult patients with aHUS– real-world data

Author

Kristina Schönfelder, Lucas Kühne, Lena Schulte-Kemna, Jessica Kaufeld, Hana Rohn, Andreas Kribben, Bernd Schröppel, Paul T. Brinkkötter, and Anja Gäckler

Subjects

Atypical hemolytic uremic syndrome, Thrombotic microangiopathy, Eculizumab, Ravulizumab, Kidney transplant recipients, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Abstract Background The complement factor 5 (C5)-inhibitor eculizumab has been established as standard-of-care for the treatment of atypical hemolytic uremic syndrome (aHUS). In 2021, the long-acting C5-inhibitor ravulizumab was approved, extending intervals of intravenous treatment from two to eight weeks resulting in improvement of quality of life for patients and lowering direct and indirect therapy associated costs. Methods This multicenter, retrospective data analysis of 32 adult patients with aHUS (including 10 kidney transplant recipients) treated with eculizumab for at least three months and switched to ravulizumab aims to evaluate the safety and efficacy of switching medication in the real-world setting. Hematologic parameters, kidney function, concurrent therapy and aHUS associated events were evaluated three months before and until up to 12 months after switching to ravulizumab. Results Mean age (range) at ravulizumab initiation was 41 years (19–78 years) and 59% of the patients were female. Genetic analysis was available for all patients with 72% showing a pathogenic variant. Median time (range) on eculizumab before switching was 20 months (3–120 months). No new events of TMA or worsening of renal function were reported during up to 12 months of follow-up during ravulizumab treatment. Conclusions This is the largest, non-industry derived, multi-center retrospective analysis of adult patients with aHUS switching C5-inhibitor treatment from eculizumab to ravulizumab in the real-world setting. Switching to ravulizumab was safe and efficient resulting in sustained hematological stability and preservation of renal function.

Published

2024

57. Eculizumab for Shiga‐toxin‐induced hemolytic uremic syndrome in adults with neurological involvement

Author

Benjamin J. Lee, Zhaohui Arter, Jean Doh, Shawn P. Griffin, Pongthep Vittayawacharin, Steven Atallah, Kevin R. Shieh, Minh‐Ha Tran, Sonata Jodele, Piyanuch Kongtim, and Stefan O. Ciurea

Subjects

eculizumab, hemolytic uremic syndrome, neurological involvement, Shiga‐toxin producing Escherichia coli, STEC‐HUS, Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Abstract The role of eculizumab in treating Shiga‐toxin‐producing Escherichia coli (STEC) hemolytic uremic syndrome (HUS) patients with neurological involvement remains unclear. We describe two distinctly different STEC‐HUS patients with neurologic involvement successfully managed with eculizumab, and perform a literature review of all published cases. Both patients had complete resolution of neurological symptoms after initiation of eculizumab. Eighty patients with STEC‐HUS treated with eculizumab were identified in the literature, 68.7% had complete resolution of neurological symptoms. Based on our experience and literature review, three prevailing themes were noted: 1) Early eculizumab administration optimized neurological outcomes, 2) Symptom resolution may not be immediate, neurological symptoms may initially worsen before improvement, and 3) Plasma exchange yielded no benefit. Early administration of eculizumab may reverse neurotoxicity in patients with STEC‐HUS.

Published

2024

58. Identification of potential C1-binding sites in the immunoglobulin CL domains.

Author

Yanaka, Saeko, Kodama, Atsuji, Nishiguchi, Shigetaka, Fujita, Rina, Shen, Jiana, Boonsri, Pornthip, Sung, Duckyong, Isono, Yukiko, Yagi, Hirokazu, Miyanoiri, Yohei, Uchihashi, Takayuki, and Kato, Koichi

Subjects

*IMMUNOGLOBULIN G, *ATOMIC force microscopy, *NUCLEAR magnetic resonance, *ISOELECTRIC point, *IMMUNOTECHNOLOGY, *CONNECTIN, *ECULIZUMAB

Abstract

Immunoglobulin G (IgG) molecules that bind antigens on the membrane of target cells spontaneously form hexameric rings, thus recruiting C1 to initiate the complement pathway. However, our previous report indicated that a mouse IgG mutant lacking the Cγ1 domain activates the pathway independently of antigen presence through its monomeric interaction with C1q via the CL domain, as well as Fc. In this study, we investigated the potential interaction between C1q and human CL isoforms. Quantitative single-molecule observations using high-speed atomic force microscopy revealed that human Cκ exhibited comparable C1q binding capabilities with its mouse counterpart, surpassing the Cλ types, which have a higher isoelectric point than the Cκ domains. Nuclear magnetic resonance and mutation experiments indicated that the human and mouse Cκ domains share a common primary binding site for C1q, centred on Glu194, a residue conserved in the Cκ domains but absent in the Cλ domains. Additionally, the Cγ1 domain, with its high isoelectric point, can cause electrostatic repulsion to the C1q head and impede the C1q-interaction adjustability of the Cκ domain in Fab. The removal of the Cγ1 domain is considered to eliminate these factors and thus promote Cκ interaction with C1q with the potential risk of uncontrolled activation of the complement pathway in vivo in the absence of antigen. However, this research underscores the presence of potential subsites in Fab for C1q binding, offering promising targets for antibody engineering to refine therapeutic antibody design. [ABSTRACT FROM AUTHOR]

Published

2024

59. Eculizumab use throughout pregnancy in two patients with aquaporin‐4‐positive neuromyelitis optica spectrum disorder.

Author

Fujimoto, Takeshi and Maeda, Yasuhiro

Subjects

*PREGNANCY complications, *MENINGOCOCCAL infections, *STEROID drugs, *IMMUNOSUPPRESSIVE agents, *PREGNANT women, *NEUROMYELITIS optica

Abstract

Background: Patients with neuromyelitis optica spectrum disorder (NMOSD) are at an increased risk of pregnancy complications. Lack of NMOSD treatment during pregnancy is a risk factor for relapse. Here, we report two cases of pregnant women with anti‐aquaporin‐4 antibody‐positive (AQP4+) NMOSD treated with eculizumab during pregnancy. Case Presentation: Patient 1 was diagnosed with AQP4+ NMOSD 2 mo after giving birth to her first child. She was treated with tacrolimus and prednisolone, before switching to prednisolone monotherapy. Following concerns of teratogenicity associated with immunosuppressive therapy and oral steroid use, she began eculizumab treatment prior to a second pregnancy. When she became pregnant, eculizumab treatment was briefly paused while safety data were reviewed with her neurologist. A total of three doses were missed. Patient 2 was diagnosed with AQP4+ NMOSD and began prednisolone treatment. Following a relapse, tacrolimus was added to her treatment regimen. Prior to pregnancy, she began eculizumab treatment alongside prednisolone and tacrolimus and maintained this regimen throughout her pregnancy. No relapses or meningococcal infections occurred after eculizumab initiation in either patient, and both gave birth without complications to healthy babies. Patient 2 continues to receive eculizumab while breastfeeding. Conclusions: We present two cases of pregnant women with AQP4+ NMOSD treated with eculizumab. Both women gave birth to healthy babies, have had no relapses since initiating eculizumab, and continued their treatment after birth. These cases are further evidence of the successful use of eculizumab during pregnancy. [ABSTRACT FROM AUTHOR]

Published

2024

60. PIK3CA inhibition in models of proliferative glomerulonephritis and lupus nephritis.

Author

Yamaguchi, Junna, Isnard, Pierre, Robil, Noémie, de la Grange, Pierre, Hoguin, Clément, Schmitt, Alain, Hummel, Aurélie, Megret, Jérôme, Goudin, Nicolas, Luka, Marine, Ménager, Mickaël M., Masson, Cécile, Zarhrate, Mohammed, Bôle-Feysot, Christine, Janiszewska, Michalina, Polyak, Kornelia, Dairou, Julien, Baldassari, Sara, Baulac, Stéphanie, and Broissand, Christine

Subjects

*LUPUS nephritis, *KIDNEY failure, *T cells, *NEPHRITIS, *B cells, *KIDNEY physiology, *GAIN-of-function mutations, *ECULIZUMAB

Abstract

Proliferative glomerulonephritis is a severe condition that often leads to kidney failure. There is a significant lack of effective treatment for these disorders. Here, following the identification of a somatic PIK3CA gain-of-function mutation in podocytes of a patient, we demonstrate using multiple genetically engineered mouse models, single-cell RNA sequencing, and spatial transcriptomics the crucial role played by this pathway for proliferative glomerulonephritis development by promoting podocyte proliferation, dedifferentiation, and inflammation. Additionally, we show that alpelisib, a PI3Kα inhibitor, improves glomerular lesions and kidney function in different mouse models of proliferative glomerulonephritis and lupus nephritis by targeting podocytes. Surprisingly, we determined that pharmacological inhibition of PI3Kα affects B and T lymphocyte populations in lupus nephritis mouse models, with a decrease in the production of proinflammatory cytokines, autoantibodies, and glomerular complement deposition, which are all characteristic features of PI3Kδ inhibition, the primary PI3K isoform expressed in lymphocytes. Importantly, PI3Kα inhibition does not impact lymphocyte function under normal conditions. These findings were then confirmed in human lymphocytes isolated from patients with active lupus nephritis. In conclusion, we demonstrate the major role played by PI3Kα in proliferative glomerulonephritis and show that in this condition, alpelisib acts on both podocytes and the immune system. [ABSTRACT FROM AUTHOR]

Published

2024

61. Kidney Disease and Antinephrin Antibodies.

Author

Reiser, Jochen and Ingelfinger, Julie R.

Subjects

*FOCAL segmental glomerulosclerosis, *KIDNEY diseases, *IMMUNOGLOBULINS, *CYTOSKELETAL proteins, *ECULIZUMAB, *ANTI-glomerular basement membrane disease, *PEPTIDES, *RITUXIMAB

Abstract

The article explores the role of antinephrin antibodies in the pathogenesis of minimal change disease and focal segmental glomerulosclerosis (FSGS). Topics discussed include the function of nephrin in kidney filtration, the impact of autoantibodies on nephrin's role, and potential implications for targeting these antibodies in treatment strategies.

Published

2024

62. Stable responses to danicopan as add-on to ravulizumab in two patients with paroxysmal nocturnal hemoglobinuria.

Author

Füreder, Wolfgang and Valent, Peter

Subjects

*PAROXYSMAL hemoglobinuria, *ECULIZUMAB, *IRON supplements, *BUDD-Chiari syndrome, *MENORRHAGIA

Abstract

This article discusses the use of danicopan as an additional treatment for two patients with paroxysmal nocturnal hemoglobinuria (PNH), a stem cell disease that causes hemolysis. The patients had persistent anemia and fatigue despite standard treatment, so danicopan was added to their regimen. Both patients showed improvements in hemoglobin levels and fatigue scores with danicopan, but one patient experienced a slight decrease in hemoglobin and an increase in fatigue after a respiratory infection and meningococcal vaccine booster. The document also mentions the need for further research on the long-term effects of danicopan therapy and declares the competing interests of the authors. [Extracted from the article]

Published

2024

63. Ekulizumab a ravulizumab - inhibitory C5 složky komplementu v léčbě generalizované formy myasthenia gravis.

Author

Týblová, Michaela

Abstract

Copyright of Remedia is the property of Medical Tribune CZ, s.r.o. and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

64. Pharmacotherapy for CD55 deficiency with CHAPLE disease: how close are we to a cure?

Author

Can, Salim, Yorgun Altunbas, Melek, and Ozen, Ahmet

Subjects

IMMUNODEFICIENCY, CD55 antigen, GENETIC disorders, DRUG therapy, ECULIZUMAB

Published

2024

65. Improvements in hematologic markers and decreases in fatigue with pegcetacoplan for patients with paroxysmal nocturnal hemoglobinuria and mild or moderate anemia (hemoglobin ≥10 g/dL) who had received eculizumab or were naive to complement inhibitors

Author

Panse, Jens, Daguindau, Nicolas, Okuyama, Sonia, Peffault de Latour, Régis, Schafhausen, Philippe, Straetmans, Nicole, Al-Adhami, Mohammed, Persson, Emmelie, and Wong, Raymond Siu Ming

Subjects

*PAROXYSMAL hemoglobinuria, *COMPLEMENT inhibition, *FATIGUE (Physiology), *HEMOGLOBINS, *ECULIZUMAB, *FETAL hemoglobin, *ATRIAL flutter

Abstract

Background: Although complement component 5 inhibitors (C5is) eculizumab and ravulizumab improve paroxysmal nocturnal hemoglobinuria (PNH) outcomes, patients may experience persistent anemia. This post hoc analysis investigated whether the complement component 3-targeted therapy pegcetacoplan also improved hematologic outcomes and reduced fatigue in patients with PNH and mild/moderate anemia. Methods: Patients with PNH and hemoglobin ≥10.0 g/dL at baseline of PADDOCK (N = 6), PRINCE (N = 8), and PEGASUS (N = 11) were included. Before receiving pegcetacoplan, PADDOCK and PRINCE patients were C5i-naive; PEGASUS patients had hemoglobin <10.5 g/dL despite stably dosed eculizumab. Hemoglobin concentrations, percentages of patients with concentrations ≥12 g/dL, and sex-specific normalization were assessed at baseline and after 16 weeks of pegcetacoplan, as were absolute reticulocyte counts (ARCs) and normalization and fatigue scores and normalization. Results: From baseline to week 16, mean (SD) hemoglobin concentrations increased in C5i-naive patients (PADDOCK: 10.5 [0.4] to 12.7 [1.1] g/dL; PRINCE: 11.3 [1.0] to 14.0 [1.3] g/dL) and those with suboptimal eculizumab responses (PEGASUS: 10.2 [0.2] to 12.8 [2.6] g/dL). Percentage of patients with hemoglobin ≥12 g/dL increased (PADDOCK: 0 to 60.0% [3 of 5 patients]; PRINCE: 25.0% [2 of 8] to 87.5% [7 of 8]; PEGASUS: 0 to 72.7% [8 of 11]). Sex-specific hemoglobin normalization at week 16 occurred in 40.0% (2 of 5) (PADDOCK), 62.5% (5 of 8) (PRINCE), and 63.6% (7 of 11) (PEGASUS). In all studies, mean ARCs decreased from above normal to normal and ARC normalization increased. Mean Functional Assessment of Chronic Illness Therapy–Fatigue scores improved from below to above or near normal. Two patients had serious adverse events (PEGASUS: post-surgery sepsis, breakthrough hemolysis); breakthrough hemolysis resolved without study discontinuation. Conclusion: Patients with PNH and mild/moderate anemia who were C5i-naive or who had suboptimal hemoglobin concentrations despite eculizumab treatment had improved hematologic outcomes and reduced fatigue after initiating or switching to pegcetacoplan. Trial registration: Trial registration numbers: PADDOCK (NCT02588833), PRINCE (NCT04085601; EudraCT, 2018-004220-11), PEGASUS (NCT03500549). [ABSTRACT FROM AUTHOR]

Published

2024

66. 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

67. The safety and efficacy profile of eculizumab in myasthenic crisis: a prospective small case series.

Author

Song, Jie, Huan, Xiao, Chen, Yuanyi, Luo, Yeting, Zhong, Huahua, Wang, Yuan, Yang, Lei, Xi, Caihua, Yang, Yu, Xi, Jianying, Zheng, Jianming, Wu, Zongtai, Zhao, Chongbo, and Luo, Sushan

Subjects

ECULIZUMAB, DRUG efficacy, MEDICATION safety, MYASTHENIA gravis, CHOLINERGIC receptors

Abstract

Eculizumab has improved recovery from ventilatory support in myasthenic crisis (MC) cases. However, the safety and efficacy profiles from prospective studies are still lacking. This study aimed to explore eculizumab's safety and efficacy in a prospective case series of patients with refractory MC. We followed a series of anti-acetylcholine receptor (AChR) antibody-positive myasthenia gravis (MG) patients who received eculizumab as an add-on therapy for 12 weeks during MC to facilitate the weaning process and reduced disease activity. Serum anti-AChR antibodies and peripheral immune molecules associated with the complement pathway were evaluated before and after eculizumab administration. Compared to the baseline Myasthenia Gravis Foundation of America (MGFA)-quantitative MG test (QMG) scores (22.25 ± 4.92) and MG-activities of daily living (MG-ADL; 18.25 ± 2.5) scores at crisis, improvements were observed from 4 weeks (14.5 ± 10.47 and 7.5 ± 7.59, respectively) through 12 weeks (7.5 ± 5.74 and 2.25 ± 3.86, respectively) post-treatment. Muscle strength consistently improved across ocular, bulbar, respiratory, and limb/gross domain groups. One patient died of cardiac failure at 16 weeks. Three cases remained in remission at 24 weeks, with a mean QMG score of 2.67 ± 2.89 and ADL score of 0.33 ± 0.58. No significant side effects were reported. Serum CH50 and soluble C5b-9 levels significantly declined, while there were no significant changes in serum anti-AChR antibody levels, C1q, C5a levels, or peripheral lymphocyte proportions. Eculizumab was well tolerated and showed efficacy in this case series. Large prospective cohort studies with extended follow-up periods are needed to further explore the safety and efficacy profile in real-world practice. [ABSTRACT FROM AUTHOR]

Published

2024

68. Transplant-associated thrombotic microangiopathy in pediatrics: incidence, risk factors, therapeutic options, and outcome based on data from a single center.

Author

Kafa, Kinan and Hoell, Jessica I.

Subjects

HEMATOPOIETIC stem cell transplantation, PAROXYSMAL hemoglobinuria

Abstract

Background: Transplant-associated thrombotic microangiopathy (TA-TMA) is a critical complication of hematopoietic stem cell transplantation. Awareness about TA-TMA has increased in recent years, resulting in the implementation of TA-TMA screening in most centers. Methods: Retrospective analysis of children who underwent autologous or allogeneic hematopoietic stem cell transplantation at our center between January 2018 and December 2022 was conducted to evaluate the incidence, clinical features, and outcomes of TA-TMA following the administration of different therapeutic options. Results: A total of 45 patients comprised the study cohort, of whom 10 developed TA-TMA with a cumulative incidence of 22% by 100 days after transplantation. Patients with and without TA-TMA in our cohort displayed an overall survival of 80% and 88%, respectively (p = 0.48), and a non-relapse mortality of 0% and 5.7%, respectively (p = 0.12), at 1 year after transplantation. Risk factors for TA-TMA development included allogeneic transplantation and total body irradiation-based conditioning regime. Among the 10 patients with TA-TMA, 7 did not meet the high-risk criteria described by Jodele and colleagues. Of these seven patients, two responded to calcineurin-inhibitor withdrawal without further therapy and five developed multiorgan dysfunction syndrome and were treated with anti-inflammatory steroids (prednisone), and all responded to therapy. The three patients with high-risk TA-TMA were treated with complement blockade or prednisone, and all responded to therapy. Conclusion: TA-TMA is a multifactorial complication with high morbidity rates. Patients with high-risk TA-TMA may benefit from complement blockade using eculizumab. No consensus has been reached regarding therapy for patients who do not meet high-risk criteria. Our analysis showed that these patients may respond to anti-inflammatory treatment with prednisone. [ABSTRACT FROM AUTHOR]

Published

2024

69. TNF-α-positive patients with recurrent pregnancy loss: The etiology and management.

Author

Cai, Zhuhua, Guo, Xueke, Zheng, Ge, Xiang, Junmiao, Liu, Lingyun, Lin, Dongmei, and Deng, Xiaohui

Subjects

*RECURRENT miscarriage, *ECULIZUMAB, *COMPLEMENT (Immunology), *PREGNANCY outcomes, *TUMOR necrosis factors, *ANTINUCLEAR factors, *IMMUNOGLOBULIN M

Abstract

Elevated levels of tumor necrosis factor-alpha (TNF-α) have been associated with adverse pregnancy outcomes, specifically recurrent pregnancy loss (RPL). These elevated levels may be associated with the presence of autoantibodies. Although TNF-α inhibitors have shown promise in improving pregnancy rates, further research is needed to comprehend their impact and mechanisms in RPL patients. This study aims to investigate the association between elevated TNF-α levels and autoantibodies in RPL patients, as well as evaluate the effect of TNF-α inhibition on pregnancy outcomes. A total of 249 RPL patients were included in this study. Serum levels of TNF-α, autoantibodies, and complement were measured and monitored. Among these patients, 138 tested positive for TNF-α, while 111 tested negative. The medical records of these patients were retrospectively evaluated. Additionally, 102 patients with elevated TNF-α levels were treated with TNF-α inhibitors, and their pregnancy outcomes were assessed.TNF-α-positive RPL patients had higher levels of complement C1q, anti-cardiolipin (ACL)-IgA, ACL-IgM ,ACL-IgG, thyroglobulin antibody, and Anti-phosphatidylserine/prothrombin IgM antibody, as well as a higher positive rate of antinuclear antibodies compared to TNF-α-negative patients (23.19% vs. 12.6%, P< 0.05). Conversely, complement C3 were lower in TNF-α-positive patients (t test, P< 0.05). The use of TNF-α inhibitors led to a reduction in the early abortion rate (13.7% vs. 44.4%, P< 0.001) and an improvement in term delivery rate (52.0% vs. 27.8%, P= 0.012). Furthermore, patients who used TNF-α inhibitors before 5 weeks of pregnancy had a lower early abortion rate (7.7% vs. 24.3%, P= 0.033) and a higher term delivery rate (69.2% vs. 48.6%, P= 0.033).TNF-α plays a role in the occurrence and development of RPL, and its expression is closely associated with autoantibodies and complements. TNF-α inhibitors increase the term delivery rate in TNF-α-positive RPL patients, and their use before 5 weeks of pregnancy may more beneficial. [ABSTRACT FROM AUTHOR]

Published

2024

70. Systems-level computational modeling in ischemic stroke: from cells to patients.

Author

Geli Li, Yanyong Zhao, Wen Ma, Yuan Gao, and Chen Zhao

Subjects

ISCHEMIC stroke, CEREBRAL circulation, ECULIZUMAB, SYSTEMS biology, COMPUTATIONAL biology, BRAIN damage

Abstract

Ischemic stroke, a significant threat to human life and health, refers to a class of conditions where brain tissue damage is induced following decreased cerebral blood flow. The incidence of ischemic stroke has been steadily increasing globally, and its disease mechanisms are highly complex and involve a multitude of biological mechanisms at various scales from genes all the way to the human body system that can affect the stroke onset, progression, treatment, and prognosis. To complement conventional experimental research methods, computational systems biology modeling can integrate and describe the pathogenic mechanisms of ischemic stroke across multiple biological scales and help identify emergent modulatory principles that drive disease progression and recovery. In addition, by running virtual experiments and trials in computers, these models can efficiently predict and evaluate outcomes of different treatment methods and thereby assist clinical decision-making. In this review, we summarize the current research and application of systems-level computational modeling in the field of ischemic stroke from the multiscale mechanism-based, physics-based and omics-based perspectives and discuss how modeling-driven research frameworks can deliver insights for future stroke research and drug development. [ABSTRACT FROM AUTHOR]

Published

2024

71. Current insights into the Pathophysiology of kidney diseases.

Author

Westphal, Anika

Subjects

*KIDNEY diseases, *FUROSEMIDE, *REPERFUSION injury, *DIABETES insipidus, *ECULIZUMAB, *PATHOLOGICAL physiology, *DIABETIC nephropathies, *POLYCYSTIC kidney disease

Abstract

This article provides current insights into the pathophysiology of kidney diseases. It highlights the importance of early diagnosis for successful treatment and discusses markers for renal injury and fibrosis. The article also explores potential preventive measures and therapeutic options for acute kidney injury (AKI) and chronic kidney disease (CKD). Additionally, it examines the role of factors such as aquaporin-2, uremic toxins, mesangial tissues, mTOR signaling, and the renin-angiotensin-aldosterone system in kidney diseases. The findings presented in this article contribute to the understanding of kidney diseases and may aid in the development of new therapeutic approaches. [Extracted from the article]

Published

2024

72. Eculizumab in Adolescent Patients With Refractory Generalized Myasthenia Gravis: A Phase 3, Open-Label, Multicenter Study.

Author

Brandsema, John F., Ginsberg, Matthew, Hoshino, Hideki, Mimaki, Masakazu, Nagata, Satoru, Rao, Vamshi K., Ruzhansky, Katherine, Suresh, Niraja, Tiongson, Emmanuelle, Yamanouchi, Hideo, Frick, Glen, Hicks, Eden, Liao, Serena, and Howard, James F.

Subjects

*MYASTHENIA gravis, *COMPLEMENT (Immunology), *ECULIZUMAB, *COMPLEMENT inhibition, *TEENAGERS, *MUSCLE weakness

Abstract

This study evaluated the efficacy and safety of eculizumab, a terminal complement C5 inhibitor, in juvenile generalized myasthenia gravis (gMG). Adolescents aged 12 to 17 years with refractory anti-acetylcholine receptor (AChR) antibody-positive gMG received eculizumab (weekly induction [one to two doses of 600 mg or four doses of 900 mg] followed by maintenance doses [300 to 1200 mg] every two weeks for up to 26 weeks) in a phase 3, open-label multicenter study (NCT03759366). Change from baseline to week 26 in Quantitative Myasthenia Gravis (QMG) total score (primary end point) and secondary end points including Myasthenia Gravis-Activities of Daily Living (MG-ADL) total score, Myasthenia Gravis Composite score, Myasthenia Gravis Foundation of America postintervention status, EuroQol 5-Dimensions (Youth) and Neurological Quality-of-Life Pediatric Fatigue questionnaire scores, as well as pharmacokinetics, pharmacodynamics, and safety, were recorded. Eleven adolescents (mean ± S.D. age 14.8 ± 1.8 years) were enrolled; 10 completed the primary evaluation period. Least-squares mean changes from baseline at week 26 were −5.8 (standard error [SE] 1.2; P = 0.0004) for QMG total score and −2.3 (SE 0.6; P = 0.0017) for MG-ADL total score. Overall, the primary and all secondary efficacy end point analyses met statistical significance from the first assessment and were sustained throughout. Complete terminal complement inhibition was sustained through 26 weeks in all patients. Treatment-emergent adverse events were all mild/moderate and predominantly unrelated to eculizumab. Eculizumab was effective in reducing disease burden and was well tolerated in adolescents with refractory AChR antibody-positive gMG. [ABSTRACT FROM AUTHOR]

Published

2024

73. Deteriorating neurological symptoms of Degos disease despite the treatment with eculizumab and beraprost: A case report with detailed radiological findings.

Author

Nakamura, Yamato, Sawamura, Masanori, Miyazaki, Tatsuhiko, Muramatsu, Aya, Suzuki, Makoto, Yagi, Hiroaki, Hori, Akinobu, Katsuyama, Yusuke, Yoshida, Hidefumi, Kim, Kang, Yamada, Hiroshi, Takahashi, Ryosuke, and Harada, Kiyoshi

Subjects

*MAGNETIC resonance angiography, *THERAPEUTICS, *SYMPTOMS, *ECULIZUMAB, *MALIGNANT atrophic papulosis

Abstract

Degos disease is a rare vasculopathy with a poor prognosis. Here, we report a case of a 17‐year‐old Japanese male with Degos disease who exhibited progressive deterioration of neurological symptoms despite treatment with eculizumab and beraprost. We also report detailed radiological findings including brain magnetic resonance imaging and perfusion computed tomography, and hereby suggest the importance of the perfusion study in detecting early changes associated with Degos disease. [ABSTRACT FROM AUTHOR]

Published

2024

74. Emerging role of C5aR2: novel insights into the regulation of uterine immune cells during pregnancy.

Author

Froehlich, Fenna, Landerholm, Konstanze, Neeb, Johanna, Meß, Ann-Kathrin, Seiler, Daniel Leonard, Tilburgs, Tamara, and Karsten, Christian Marcel

Subjects

PREGNANCY complications, FETAL growth retardation, ECULIZUMAB, KILLER cells, PREGNANCY, COMPLEMENT (Immunology), PLACENTAL growth factor

Abstract

Pregnancy is a fascinating immunological phenomenon because it allows allogeneic fetal and placental tissues to survive inside the mother. As a component of innate immunity with high inflammatory potential, the complement system must be tightly regulated during pregnancy. Dysregulation of the complement system plays a role in pregnancy complications including pre-eclampsia and intrauterine growth restriction. Complement components are also used as biomarkers for pregnancy complications. However, the mechanisms of detrimental role of complement in pregnancy is poorly understood. C5a is the most potent anaphylatoxin and generates multiple immune reactions via two transmembrane receptors, C5aR1 and C5aR2. C5aR1 is pro-inflammatory, but the role of C5aR2 remains largely elusive. Interestingly, murine NK cells have been shown to express C5aR2 without the usual co-expression of C5aR1. Furthermore, C5aR2 appears to regulate IFN-γ production by NK cells in vitro. As IFN-γ produced by uterine NK cells is one of the major factors for the successful development of a vital pregnancy, we investigated the role anaphylatoxin C5a and its receptors in the establishment of pregnancy and the regulation of uterine NK cells by examinations of murine C5ar2-/- pregnancies and human placental samples. C5ar2-/- mice have significantly reduced numbers of implantation sites and a maternal C5aR2 deficiency results in increased IL-12, IL-18 and IFN-γ mRNA expression as well as reduced uNK cell infiltration at the maternal-fetal interface. Human decidual leukocytes have similar C5a receptor expression patterns showing clinical relevance. In conclusion, this study identifies C5aR2 as a key contributor to dNK infiltration and pregnancy success. [ABSTRACT FROM AUTHOR]

Published

2024

75. Clinical efficacy and safety of switching from eculizumab to ravulizumab in adult patients with aHUS– real-world data.

Author

Schönfelder, Kristina, Kühne, Lucas, Schulte-Kemna, Lena, Kaufeld, Jessica, Rohn, Hana, Kribben, Andreas, Schröppel, Bernd, Brinkkötter, Paul T., and Gäckler, Anja

Subjects

HEMOLYTIC-uremic syndrome, ECULIZUMAB, ADULTS, KIDNEY transplantation, KIDNEY physiology

Abstract

Background: The complement factor 5 (C5)-inhibitor eculizumab has been established as standard-of-care for the treatment of atypical hemolytic uremic syndrome (aHUS). In 2021, the long-acting C5-inhibitor ravulizumab was approved, extending intervals of intravenous treatment from two to eight weeks resulting in improvement of quality of life for patients and lowering direct and indirect therapy associated costs. Methods: This multicenter, retrospective data analysis of 32 adult patients with aHUS (including 10 kidney transplant recipients) treated with eculizumab for at least three months and switched to ravulizumab aims to evaluate the safety and efficacy of switching medication in the real-world setting. Hematologic parameters, kidney function, concurrent therapy and aHUS associated events were evaluated three months before and until up to 12 months after switching to ravulizumab. Results: Mean age (range) at ravulizumab initiation was 41 years (19–78 years) and 59% of the patients were female. Genetic analysis was available for all patients with 72% showing a pathogenic variant. Median time (range) on eculizumab before switching was 20 months (3–120 months). No new events of TMA or worsening of renal function were reported during up to 12 months of follow-up during ravulizumab treatment. Conclusions: This is the largest, non-industry derived, multi-center retrospective analysis of adult patients with aHUS switching C5-inhibitor treatment from eculizumab to ravulizumab in the real-world setting. Switching to ravulizumab was safe and efficient resulting in sustained hematological stability and preservation of renal function. [ABSTRACT FROM AUTHOR]

Published

2024

76. 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

77. Urinary complement biomarkers in immune-mediated kidney diseases.

Author

Kesarwani, Vartika, Bukhari, Muhammad Hamza, Kahlenberg, J. Michelle, and Shudan Wang

Subjects

KIDNEY diseases, ECULIZUMAB, BIOMARKERS, THROMBOTIC microangiopathies, IGA glomerulonephritis, COMPLEMENT (Immunology)

Abstract

The complement system, an important part of the innate system, is known to play a central role in many immune mediated kidney diseases. All parts of the complement system including the classical, alternative, and mannose-binding lectin pathways have been implicated in complement-mediated kidney injury. Although complement components are thought to be mainly synthesized in the liver and activated in the circulation, emerging data suggest that complement is synthesized and activated inside the kidney leading to direct injury. Urinary complement biomarkers are likely a better reflection of inflammation within the kidneys as compared to traditional serum complement biomarkers which may be influenced by systemic inflammation. In addition, urinary complement biomarkers have the advantage of being non-invasive and easily accessible. With the rise of therapies targeting the complement pathways, there is a critical need to better understand the role of complement in kidney diseases and to develop reliable and non-invasive biomarkers to assess disease activity, predict treatment response and guide therapeutic interventions. In this review, we summarized the current knowledge on urinary complement biomarkers of kidney diseases due to immune complex deposition (lupus nephritis, primary membranous nephropathy, IgA nephropathy) and due to activation of the alternative pathway (C3 glomerulopathy, thrombotic microangiography, ANCA-associated vasculitis). We also address the limitations of current research and propose future directions for the discovery of urinary complement biomarkers. [ABSTRACT FROM AUTHOR]

Published

2024

78. The histone demethylase JMJD1C regulates CPS1 expression and promotes the proliferation of paroxysmal nocturnal haemoglobinuria clones through cell metabolic reprogramming.

Author

Chen, Yingying, Liu, Hui, Wang, Chaomeng, Chen, Weixin, Li, Liyan, Wu, Junshu, Wang, Guanrou, Ling, Guang Sheng, and Fu, Rong

Subjects

*METABOLIC reprogramming, *DEMETHYLASE, *CELL metabolism, *ERYTHROCYTE membranes, *MOLECULAR cloning, *ECULIZUMAB

Abstract

Summary: Paroxysmal nocturnal haemoglobinuria (PNH) is a disorder resulting from erythrocyte membrane deficiencies caused by PIG‐A gene mutations. While current treatments alleviate symptoms, they fail to address the underlying cause of the disease—the pathogenic PNH clones. In this study, we found that the expression of carbamoyl phosphate synthetase 1 (CPS1) was downregulated in PNH clones, and the level of CPS1 was negatively correlated with the proportion of PNH clones. Using PIG‐A knockout K562 (K562 KO) cells, we demonstrated that CPS1 knockdown increased cell proliferation and altered cell metabolism, suggesting that CPS1 participates in PNH clonal proliferation through metabolic reprogramming. Furthermore, we observed an increase in the expression levels of the histone demethylase JMJD1C in PNH clones, and JMJD1C expression was negatively correlated with CPS1 expression. Knocking down JMJD1C in K562 KO cells upregulated CPS1 and H3K36me3 expression, decreased cell proliferation and increased cell apoptosis. Chromatin immunoprecipitation analysis further demonstrated that H3K36me3 regulated CPS1 expression. Finally, we demonstrated that histone demethylase inhibitor JIB‐04 can suppressed K562 KO cell proliferation and reduced the proportion of PNH clones in PNH mice. In conclusion, aberrant regulation of the JMJD1C‐H3K36me3‐CPS1 axis contributes to PNH clonal proliferation. Targeting JMJD1C with a specific inhibitor unveils a potential strategy for treating PNH patients. [ABSTRACT FROM AUTHOR]

Published

2024

79. 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

80. Safety and Efficacy of Very Early Conversion to Belatacept in Pediatric Kidney Transplantation with Transplant-Associated Thrombotic Microangiopathy: Case Study and Review of Literature.

Author

Acharya, Ratna, Clapp, William, and Upadhyay, Kiran

Subjects

*LITERATURE reviews, *BELATACEPT, *KIDNEY transplantation, *IMMUNOSUPPRESSIVE agents, *THROMBOTIC thrombocytopenic purpura, *ECULIZUMAB

Abstract

The inhibition of co-stimulation during T-cell activation has been shown to provide effective immunosuppression in kidney transplantation (KT). Hence, the conversion from calcineurin inhibitor (CNI) to belatacept is emerging as a potential alternate maintenance immunosuppressive therapy in those with transplant-associated thrombotic microangiopathy (TA-TMA) or in the prevention of TA-TMA. We present a 17-year-old male who presented with biopsy-proven CNI-associated TA-TMA immediately post-KT. The administration of eculizumab led to the reversal of TMA. Tacrolimus was converted to belatacept with excellent efficacy and safety during a short-term follow-up of one year. Further larger controlled studies are required to demonstrate the efficacy of this approach in children who present with early-onset TMA post-KT. [ABSTRACT FROM AUTHOR]

Published

2024

81. Exploring treatment strategies for paroxysmal nocturnal hemoglobinuria: an overview of registered clinical trials.

Author

Peixoto, Vanda P., Prudêncio, Cristina, and Vieira, Mónica

Subjects

*PAROXYSMAL hemoglobinuria, *CLINICAL trials, *COMPLEMENT inhibition, *ERYTHROCYTES, *THERAPEUTICS, *COMPLEMENT activation

Abstract

Paroxysmal nocturnal hemoglobinuria (PNH) is a rare, acquired disease in which blood cells lack anchored proteins that regulate the complement system. The erythrocytes are then destroyed because of uncontrolled complement activity, leading to intravascular hemolysis (IVH) and a high risk of thrombosis outcome. A huge alteration in the treatment of the disease was the development of terminal complement inhibitors, with the achievement of IVH blockade, reduction or abolishment of red blood cell (RBC) transfusions, and thromboembolic events prevention. However, patients treated with these inhibitors can still present extravascular hemolysis (EVH) caused by C3 activation and residual IVH or clinically relevant levels of breakthrough hemolysis (BTH). Proximal complement inhibitors turned out to be the key to the solution of this problem by targeting components of the proximal complement pathway, avoiding intra and extravascular hemolysis. FDA approved eculizumab, ravulizumab (terminal inhibitors), pegcetacoplan, iptacopan, and danicopan (proximal inhibitors) as a treatment for PNH so far. Various clinical trials are underway to find the most effective method to treat patients with PNH. This review aimed to summarize 71 registered clinical trials in the ClinicalTrials.gov database with the various treatment drugs, possible mechanisms, and novel findings related to PNH treatment. [ABSTRACT FROM AUTHOR]

Published

2024

82. Eculizumab Treatment of Massive Hemolysis Occurring in a Rare Co-Existence of Paroxysmal Nocturnal Hemoglobinuria and Myasthenia Gravis.

Author

Bicskó, Ráhel Réka, Illés, Árpád, Hevessy, Zsuzsanna, Ivády, Gergely, Kerekes, György, Méhes, Gábor, Csépány, Tünde, and Gergely, Lajos

Subjects

*MYASTHENIA gravis, *PAROXYSMAL hemoglobinuria, *HEMOLYSIS & hemolysins, *RESPIRATORY acidosis, *ECULIZUMAB, *RESPIRATORY diseases

Abstract

The co-occurrence of myasthenia gravis (MG) and paroxysmal nocturnal hemoglobinuria (PNH) is rare; only one case has been published so far. We report a 63-year-old Caucasian female patient who was diagnosed with MG at the age of 43. Thymoma was also detected, and so it was surgically resected, which resulted in reasonable disease control for nearly 20 years. Slight hemolysis began to emerge, and then myasthenia symptoms progressed, so immunosuppressive therapy was started. Due to progressive disease and respiratory failure, the patient underwent plasmapheresis, and ventilatory support was stopped. Marked hemolysis was present, and diagnostic tests confirmed PNH with type III PNH cells. Her myasthenia symptoms aggravated, mechanical ventilation had to be started again, and due to the respiratory acidosis, massive hemolysis occurred. After two plasmapheresis sessions, the patient received eculizumab at 600 mg, resulting in prompt hemolysis control. After the second dose of the treatment, the patient was extubated. Still, due to their inability to cough, she developed another respiratory failure and pneumonia–sepsis, resulting in the patient's death. This case highlights the rare association between these two serious diseases and similar immune-mediated pathophysiology mechanisms involving the complement system. [ABSTRACT FROM AUTHOR]

Published

2024

83. Zilucoplan: A Newly Approved Macrocyclic Peptide for Treatment of Anti-Acetylcholine Receptor Positive Myasthenia Gravis.

Author

Costa, Lia and Fernandes, Carla

Subjects

*MYASTHENIA gravis, *PEPTIDES, *ECULIZUMAB, *COMPLEMENT inhibition, *MYONEURAL junction, *THERAPEUTICS

Abstract

Zilucoplan is a synthetic macrocyclic peptide approved by the Food and Drug Administration (FDA), in October 2023, for the treatment of generalized myasthenia gravis. It is considered as an orphan drug that causes the inhibition of terminal complement cascade activation with a dual mechanism of action preventing the formation of the membrane attack complex (MAC) and the destruction of the neuromuscular junction. This drug has been demonstrated to be able to treat the generalized myasthenia gravis without significant adverse effects, with good efficacy, safety, and tolerability profile. Zilucoplan is not only innovative and promising in the therapeutics of generalized myasthenia gravis, but it could also be beneficial for the treatment of other diseases as well as a model for synthesis of analogues to improve pharmacological profile. [ABSTRACT FROM AUTHOR]

Published

2024

84. Network Meta-analysis of Ravulizumab and Alternative Interventions for the Treatment of Neuromyelitis Optica Spectrum Disorder.

Author

Clardy, Stacey L., Pittock, Sean J., Aktas, Orhan, Nakahara, Jin, Isobe, Noriko, Centonze, Diego, Fam, Sami, Kielhorn, Adrian, Yu, Jeffrey C., Jansen, Jeroen, and Zhang, Ina

Subjects

*NEUROMYELITIS optica, *CENTRAL nervous system, *BAYESIAN analysis

Abstract

Introduction: Anti-aquaporin-4 antibody-positive (AQP4-Ab+) neuromyelitis optica spectrum disorder (NMOSD) is a complement-mediated autoimmune disease in which unpredictable and relapsing attacks on the central nervous system cause irreversible and accumulating damage. Comparative efficacy of new NMOSD therapies, such as ravulizumab, with established therapies is critical in making informed treatment decisions. Methods: Efficacy of ravulizumab relative to established AQP4-Ab+ NMOSD treatments, such as eculizumab, inebilizumab, and satralizumab, was evaluated in a Bayesian network meta-analysis (NMA). Data were extracted from trials identified by a systematic literature review. The final evidence base consisted of 17 publications representing five unique and global studies (PREVENT, N-MOmentum, SAkuraSky, SAkuraStar, and CHAMPION-NMOSD). The primary endpoint was time-to-first relapse; other outcomes included annualized relapse rates (ARRs). Results: For patients receiving monotherapy (monoclonal antibody only), ravulizumab was associated with a lower risk of relapse than inebilizumab (hazard ratio [HR] 0.09, 95% credible interval [CrI] 0.02, 0.57) or satralizumab (HR 0.08, 95% CrI 0.01, 0.55) and was comparable to eculizumab (HR 0.86, 95% Crl 0.16, 4.52). Ravulizumab + immunosuppressive therapy (IST) was associated with a lower risk of relapse than satralizumab + IST (HR 0.15, 95% CrI 0.03, 0.78); the comparison with eculizumab + IST suggested no difference. No patients treated with inebilizumab received background IST and were thus excluded from analysis. The ARR with ravulizumab monotherapy was 98% lower compared with inebilizumab (rate ratio [RR] 0.02, 95% Crl 0.00, 0.38) and satralizumab (RR 0.02, 95% Crl 0.00, 0.42) monotherapies. The ARR with ravulizumab ± IST showed the strongest treatment-effect estimates compared with other interventions. Conclusion: In the absence of head-to-head randomized controlled trials, NMA results suggest ravulizumab, a C5 inhibitor, is likely to be more effective in preventing NMOSD relapse in patients with AQP4-Ab+ NMOSD when compared with other treatments having different methods of action. Plain Language Summary: Anti-aquaporin-4 antibody-positive neuromyelitis optica spectrum disorder, also called AQP4-Ab+ NMOSD, is a rare autoimmune disease that causes repeated episodes of symptoms such as blindness, arm/leg weakness, painful spasms, vomiting, and hiccups, among other symptoms. Each episode can cause nervous system damage to worsen, making it more difficult to recover back to regular abilities. Repeated episodes are likely to cause permanent damage, such as blindness and paralysis. Medical treatments that reduce episodes also reduce the damage and the chances symptoms will become permanent. One treatment, ravulizumab, is being studied to treat adults with AQP4-Ab+ NMOSD. This analysis looked at information from published clinical studies to compare ravulizumab with three other treatments (eculizumab, inebilizumab, and satralizumab) to determine how well each treatment reduced NMOSD episodes. There are no studies that have tested all four treatments in one study. Here, the treatments were compared by a method used to estimate the likelihood of a treatment being better than the others. While all four treatments successfully reduced episodes in their own studies, this analysis predicts that ravulizumab would likely be best in preventing episodes compared with inebilizumab or satralizumab when used alone or in combination with other immunosuppressive treatments. These findings, in consideration along with other relevant factors such as cost, safety, dosing delivery method, and frequency of treatment, may help doctors and patients decide what is the best treatment option for each individual patient to prevent attacks in adults with AQP4-Ab+ NMOSD. [ABSTRACT FROM AUTHOR]

Published

2024

85. Monoclonal antibodies that target fibroblast growth factor receptor 2 isoform b and Claudin‐18 isoform 2 splicing variants in gastric cancer and other solid tumours.

Author

Katoh, Masuko, Nakayama, Izuma, Wainberg, Zev A, Shitara, Kohei, and Katoh, Masaru

Subjects

*FIBROBLAST growth factor 2, *FIBROBLAST growth factor receptors, *ECULIZUMAB, *STOMACH cancer, *MONOCLONAL antibodies, *PANCREATIC intraepithelial neoplasia, *ANTIBODY-dependent cell cytotoxicity

Abstract

This article explores the role of splicing variants in cellular processes and their potential as targets for cancer treatments. Specifically, it focuses on two splicing variants, FGFR2b and CLDN18.2, which are overexpressed in gastric and other solid tumors. The article discusses two biologic drugs, bemarituzumab and zolbetuximab, that target these splicing variants in gastric and gastroesophageal junction adenocarcinoma patients. Bemarituzumab has shown promising results in phase I and II studies, while zolbetuximab has achieved positive outcomes in phase III studies. Ongoing clinical trials are further investigating the use of these drugs and their potential in other types of cancer. [Extracted from the article]

Published

2024

86. Formation of Multinucleated Giant Cells after Experimental Intracerebral Hemorrhage: Characteristics and Role of Complement C3.

Author

Fu, Xiongjie, Wang, Ming, Wan, Yingfeng, Hua, Ya, Keep, Richard F., and Xi, Guohua

Subjects

MULTINUCLEATED giant cells, COMPLEMENT (Immunology), CEREBRAL hemorrhage, ECULIZUMAB, COMPLEMENT activation, ERYTHROCYTES

Abstract

Hematoma clearance is critical for mitigating intracerebral hemorrhage (ICH)-induced brain injury. Multinucleated giant cells (MGCs), a type of phagocyte, and the complement system may play a pivotal role in hematoma resolution, but whether the complement system regulates MGC formation after ICH remains unclear. The current study investigated the following: (1) the characteristics of MGC formation after ICH, (2) whether it was impacted by complement C3 deficiency in mice and (3) whether it also influenced hematoma degradation (hemosiderin formation). Young and aged male mice, young female mice and C3-deficient and -sufficient mice received a 30 μL injection of autologous whole blood into the right basal ganglia. Brain histology and immunohistochemistry were used to examine MGC formation on days 3 and 7. Hemosiderin deposition was examined by autofluorescence on day 28. Following ICH, MGCs were predominantly located in the peri-hematoma region exhibiting multiple nuclei and containing red blood cells or their metabolites. Aging was associated with a decrease in MGC formation after ICH, while sex showed no discernible effect. C3 deficiency reduced MGC formation and reduced hemosiderin formation. Peri-hematomal MGCs may play an important role in hematoma resolution. Understanding how aging and complement C3 impact MGCs may provide important insights into how to regulate hematoma resolution. [ABSTRACT FROM AUTHOR]

Published

2024

87. Ravulizumab in adults and children with atypical hemolytic uremic syndrome: a plain language summary of three studies

Author

Michal Nowicki and Nikoleta Printza

Subjects

ahus, atypical hemolytic uremic syndrome, blood clots, complement system, dialysis, eculizumab, ravulizumab, Public aspects of medicine, RA1-1270

Abstract

This summary gives an overview of three published articles that report the results of research studies of ravulizumab, an approved treatment for people with atypical hemolytic uremic syndrome (often shortened to aHUS). This is a rare and serious condition where blood clots form in small blood vessels. Blood vessels are structures that transport blood around the body. Blood clots are the body's way of stopping someone from bleeding too much. However, if they form when they are not needed, they can cause harm. In atypical hemolytic uremic syndrome, the blood clots can cause injury to organs like the kidney. In the three studies, the researchers wanted to know if ravulizumab could decrease the formation of these clots and improve kidney function. • Children who had never received ravulizumab or a similar treatment took part in the first study. • Adults who had never received ravulizumab or a similar treatment took part in the second study. • In the third study, children whose disease was already controlled by a medication called eculizumab switched to ravulizumab. Ravulizumab is dosed less frequently than eculizumab. The researchers looked at kidney function and the levels of different blood components to see how well the treatment was working. They also monitored the adverse effects that participants experienced.

Published

2024

88. Successful eculizumab treatment as an adjunctive therapy to desensitization in ABO-incompatible living donor kidney transplantation and its molecular phenotypes

Author

Ga Young Heo, Minsun Jung, Honglin Piao, Hyun Jeong Kim, Hyung Woo Kim, Juhan Lee, Kyu Ha Huh, Beom Seok Kim, and Jaeseok Yang

Subjects

ABO-incompatible kidney transplantation, antibody-mediated rejection, complement, desensitization, eculizumab, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionABO-incompatible (ABOi) kidney transplantation (KT) has become an important option to overcome organ shortage. Plasmapheresis/rituximab-based desensitization therapy has successfully reduced anti-ABO antibody levels and suppressed antibody-mediated rejection (AMR) in ABOi KT. However, high titers of anti-ABO antibodies in some patients are refractory to standard desensitization, leading to loss of KT opportunities or AMR.MethodsEculizumab treatment was used an adjunctive therapy to rescue high-titer ABOi KT patients refractory to plasmapheresis/rituximab-based desensitization. Molecular phenotypes of allograft biopsies and cellular phenotypes of peripheral blood mononuclear cells of eculizumab group were compared with those of control groups using the Banff Human Organ Transplant gene panel and flow-cytometric analysis, respectively.ResultsThe initial titers of anti-ABO antibodies in the two patients were 1:512 and >1:1024; the final pre-transplant titers after desensitization were 1:128 and 1:64. Both patients received eculizumab from KT day to two or four weeks post-KT and maintained stable renal function up to one-year post-transplantation without overt infection, despite early episodes of probable AMR or borderline T cell-mediated rejection. Molecular phenotype analysis revealed that gene expression patterns in the ABOi KT with eculizumab group overlapped with those in the ABOi KT with AMR group more than in the ABOi KT without AMR group, except for complement pathway-related gene expression. Anti-ABO antibody titers decreased to low levels 1–3 months post-transplant in the eculizumab group in parallel with decreasing anti-B-specific B cells.ConclusionsShort-term eculizumab therapy is promising for rescuing ABOi KT recipients with high anti-ABO antibody titers refractory to plasmapheresis-based desensitization therapy.

Published

2024

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

Author

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

Subjects

antiphospholipid syndrome, complement system, eculizumab, kidney failure, timing, catastrophic antiphospholipid antibody syndrome (CAPS), Immunologic diseases. Allergy, RC581-607

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 eculizumab was 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.

Published

2024

90. Eculizumab for pregnancy-related atypical hemolytic uremic syndrome.

Author

Korotchaeva, Yulia, Kozlovskaya, Natalia, Shifman, Efim, Kudlay, Dmitry, and Moiseev, Sergey

Subjects

*THIRD generation cephalosporins, *CHRONIC kidney failure, *HEMOLYTIC-uremic syndrome, *ADULT respiratory distress syndrome, *COMPLEMENT inhibition, *THROMBOTIC thrombocytopenic purpura, *KIDNEY diseases

Published

2024

91. A Phase 3 Open-Label Study of Eculizumab in Pediatric Participants With Refractory Generalized Myasthenia Gravis (gMG)

Published

2023

92. Comparative PK, Safety, Tolerability, Immunogenicity, and PD Profile Study of TUR03 and Soliris in Healthy Participants

Published

2023

93. Study of Danicopan in Participants With Paroxysmal Nocturnal Hemoglobinuria With Inadequate Response to Eculizumab (PNH)

Author

Achillion, a wholly owned subsidiary of Alexion

Published

2023

94. The Use of Eculizumab in HELLP Syndrome

Author

Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD)

Published

2023

95. Complement Regulation to Undo Systemic Harm in Preeclampsia (CRUSH)

Author

Alexion Pharmaceuticals, Inc. and S Ananth Karumanchi, Professor of Medicine, Cedars-Sinai Medical Center

Published

2023

96. Eculizumab to Treat Thrombotic Microangiopathy/Atypical Hemolytic Uremic Syndrome -Associated Multiple Organ Dysfunction Syndrome in Hematopoietic Stem Cell Transplant Recipients

Published

2023

97. Prospective Observational Study of Long-term Pathogenic Treatment of Elizaria® (NAP)

Published

2023

98. Steroids and Immunomodulating Agents

Author

Alcoba, Shantal, Perez, Daitiara, Mahanna Gabrielli, Elizabeth, editor, O'Phelan, Kristine H., editor, Kumar, Monisha A., editor, Levine, Joshua, editor, Le Roux, Peter, editor, Gabrielli, Andrea, editor, and Layon, A. Joseph, editor

Published

2024

99. Management of paroxysmal nocturnal hemoglobinuria with low-level hemolysis in pregnancy– a report of two cases

Author

Riedl, Julia, Pfeilstöcker, Michael, Farr, Alex, Häusler, Günther, Ay, Cihan, and Füreder, Wolfgang

Published

2024

100. Eculizumab in refractory myasthenia gravis: a real-world single-center experience

Author

Ricciardi, Dario, Erra, Carmen, Tuccillo, Francesco, De Martino, Bernardo Maria, Fasolino, Alessandra, and Habetswallner, Francesco

Published

2024