Quantitative multiplex profiling of the complement system to diagnose complement‐mediated diseases

Willems, Esther; Lorés‐Motta, Laura; Zanichelli, Andrea; Suffritti, Chiara; Flier, Michiel van der; Molen, Renate G. van der; Langereis, Jeroen D.; Drongelen, J. van; Heuvel, Lambert P. van den; Volokhina, Elena; Kar, N.C. van de; Keizer-Garritsen, Jenneke J.; Levin, Michael; Herberg, Jethro; Martinón-Torres, Federico; Wessels, Hans J.C.T.; Breuk, Anita de; Fauser, Sascha; Hoyng, Carel B.; Hollander, Anneke I. den; Groot, Ronald de; Gool, Alain J. van; Gloerich, Jolein; Jonge, Marien I. de

doi:10.1002/cti2.1225

Cited by 9 publications

(10 citation statements)

References 43 publications

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“…For patient A, significant lower levels of C1 inhibitor, C3, C5 and vitronectin were detected. 10 In addition, and especially relevant for complement deficiencies that can be compensated by sufficient CP activation, nasopharyngeal colonisation or subclinical infections induce immunisation that would protect against reinfection.…”

Section: Discussionmentioning

confidence: 99%

“…Analysis of 34 complement proteins in serum by mass spectrometry revealed undetectable fD and significant lower C1 inhibitor, C3, C5 and vitronectin serum level. 10 Genetic analysis of complement genes revealed a maternal heterozygous NM_001928.3(CFD):c.125C>A p.(Ser42*) gene mutation. Additional analysis of 386 primary immunodeficiency genes using clinical exome sequencing was further normal.…”

Section: Patient Detailsmentioning

confidence: 99%

“…Analysis of 34 complement proteins in serum by mass spectrometry revealed undetectable fD. 10 Genetic analysis of complement genes demonstrated the familial heterozygous fD mutation. Following diagnosis, she was started on co-trimoxazole prophylaxis and received additional pneumococcal, meningococcal ACYW and 4CMenB vaccines.…”

Section: Patient Detailsmentioning

confidence: 99%

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Complement factor D haplodeficiency is associated with a reduced complement activation speed and diminished bacterial killing

et al. 2021

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Objectives Complete deficiency of alternative pathway (AP) complement factors, explained by homozygous mutations, is a well‐known risk factor for invasive bacterial infections; however, this is less obvious for heterozygous mutations. We describe two siblings with a heterozygous NM_001928.3(CFD):c.125C>A p.(Ser42*) mutation in the complement factor D (fD) gene having a history of recurrent bacterial infections. We determined the effect of heterozygous fD deficiency on AP complement activity. Methods We determined the effect of fD levels on complement activation as measured by AP activity, complement C3 binding to the bacterial surface of Neisseria meningitidis (Nm), Streptococcus pneumoniae (Sp) and non‐typeable Haemophilus influenzae (NTHi), and complement‐mediated killing of Nm and NTHi. In addition, we measured the effect of vaccination of complement C3 binding to the bacterial surface and killing of Nm. Results Reconstitution of fD‐deficient serum with fD increased AP activity in a dose‐ and time‐dependent way. Reconstitution of patient serum with fD to normal levels increased complement C3 binding to Sp, Nm and NTHi, as well as complement‐mediated killing of Nm and NTHi. Vaccination increased complement C3 binding and resulted in complete killing of Nm without fD reconstitution. Conclusion We conclude that low fD serum levels (< 0.5 μg mL −1 ) lead to a reduced speed of complement activation, which results in diminished bacterial killing, consistent with recurrent bacterial infections observed in our index patients. Specific antibodies induced by vaccination are able to overcome the diminished bacterial killing capacity in patients with low fD levels.

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Section: Discussionmentioning

confidence: 99%

Section: Patient Detailsmentioning

confidence: 99%

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Complement factor D haplodeficiency is associated with a reduced complement activation speed and diminished bacterial killing

et al. 2021

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“…Another area of recent advancement is the potential to gain information by multiplexing complement testing. As complement is a cascade of multiple pathways and multiple components, the value of being able to test across the pathways is clear ( 84 ). An example of the potential value of this type of approach is presented in the work of Lennart Hammarström of the Karolinska Institute that has pioneered using dried blood spot samples in conjunction with multiplex immunoassays to detect primary complement deficiencies ( 85 ).…”

Section: Complement Testing Addressed In the Standardization Effortsmentioning

confidence: 99%

“…An example of the potential value of this type of approach is presented in the work of Lennart Hammarström of the Karolinska Institute that has pioneered using dried blood spot samples in conjunction with multiplex immunoassays to detect primary complement deficiencies ( 85 ). Taking another approach, the group led by Marien I. de Jonge has demonstrated success using mass spectrometry to profile the complement system ( 84 ). These early successes are likely only the start of future multiplex testing in the complement laboratory.…”

Section: Complement Testing Addressed In the Standardization Effortsmentioning

confidence: 99%

Expanding Horizons in Complement Analysis and Quality Control

Frazer‐Abel¹,

Kirschfink²,

Prohászka³

2021

Front. Immunol.

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Complement not only plays a key role in host microbial defense but also modulates the adaptive immune response through modification of T- and B-cell reactivity. Moreover, a normally functioning complement system participates in hematopoiesis, reproduction, lipid metabolism, and tissue regeneration. Because of its powerful inflammatory potential, multiple regulatory proteins are needed to prevent potential tissue damage. In clinical practice, dysregulation and overactivation of the complement system are major causes of a variety of inflammatory and autoimmune diseases ranging from nephropathies, age-related macular degeneration (AMD), and systemic lupus erythematosus (SLE) to graft rejection, sepsis, and multi-organ failure. The clinical importance is reflected by the recent development of multiple drugs targeting complement with a broad spectrum of indications. The recognition of the role of complement in diverse diseases and the advent of complement therapeutics has increased the number of laboratories and suppliers entering the field. This has highlighted the need for reliable complement testing. The relatively rapid expansion in complement testing has presented challenges for a previously niche field. This is exemplified by the issue of cross-reactivity of complement-directed antibodies and by the challenges of the poor stability of many of the complement analytes. The complex nature of complement testing and increasing clinical demand has been met in the last decade by efforts to improve the standardization among laboratories. Initiated by the IUIS/ICS Committee for the Standardization and Quality Assessment in Complement Measurements 14 rounds of external quality assessment since 2010 resulted in improvements in the consistency of testing across participating institutions, while extending the global reach of the efforts to more than 200 laboratories in 30 countries. Worldwide trends of assay availability, usage, and analytical performance are summarized based on the past years’ experiences. Progress in complement analysis has been facilitated by the quality assessment and standardization efforts that now allow complement testing to provide a comprehensive insight into deficiencies and the activation state of the system. This in turn enables clinicians to better define disease severity, evolution, and response to therapy.

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A look into retinal organoids: methods, analytical techniques, and applications

Afanasyeva

Corral-Serrano²,

Garanto

et al. 2021

Cell. Mol. Life Sci.

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Inherited retinal diseases (IRDs) cause progressive loss of light-sensitive photoreceptors in the eye and can lead to blindness. Gene-based therapies for IRDs have shown remarkable progress in the past decade, but the vast majority of forms remain untreatable. In the era of personalised medicine, induced pluripotent stem cells (iPSCs) emerge as a valuable system for cell replacement and to model IRD because they retain the specific patient genome and can differentiate into any adult cell type. Three-dimensional (3D) iPSCs-derived retina-like tissue called retinal organoid contains all major retina-specific cell types: amacrine, bipolar, horizontal, retinal ganglion cells, Müller glia, as well as rod and cone photoreceptors. Here, we describe the main applications of retinal organoids and provide a comprehensive overview of the state-of-art analysis methods that apply to this model system. Finally, we will discuss the outlook for improvements that would bring the cellular model a step closer to become an established system in research and treatment development of IRDs.

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Quantitative multiplex profiling of the complement system to diagnose complement‐mediated diseases

Cited by 9 publications

References 43 publications

Complement factor D haplodeficiency is associated with a reduced complement activation speed and diminished bacterial killing

Complement factor D haplodeficiency is associated with a reduced complement activation speed and diminished bacterial killing

Expanding Horizons in Complement Analysis and Quality Control

A look into retinal organoids: methods, analytical techniques, and applications

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