Elevated Plasma Complement Factors in CRB1-Associated Inherited Retinal Dystrophies

Lude Moekotte; Joke H. de Boer; Sanne Hiddingh; Aafke de Ligt; Xuan Thanh An Nguyen; Carel B. Hoyng; Chris F. Inglehearn; Martin McKibbin; Tina M. Lamey; Jennifer A. Thompson; Fred K. Chen; Terri L. McLaren; Alaa AlTalbishi; Daan M. Panneman; Erica G.M. Boonen; Sandro Banfi; Béatrice Bocquet; Isabelle Meunier; Elfride De Baere; Robert Koenekoop; Monika Ołdak; Carlo Rivolta; Lisa Roberts; Raj Ramesar; Rasa Strupaitė-Šileikiene; Susanne Kohl; G. Jane Farrar; Marion van Vugt; Jessica van Setten; Susanne Roosing; L. Ingeborgh van den Born; Camiel J.F. Boon; Maria M. van Genderen; Jonas J.W. Kuiper

doi:10.1167/iovs.66.2.55

Elevated Plasma Complement Factors in CRB1-Associated Inherited Retinal Dystrophies

Lude Moekotte^*, Joke H. de Boer, Sanne Hiddingh, Aafke de Ligt, Xuan Thanh An Nguyen, Carel B. Hoyng, Chris F. Inglehearn, Martin McKibbin, Tina M. Lamey, Jennifer A. Thompson, Fred K. Chen, Terri L. McLaren, Alaa AlTalbishi, Daan M. Panneman, Erica G.M. Boonen, Sandro Banfi, Béatrice Bocquet, Isabelle Meunier, Elfride De Baere, Robert KoenekoopMonika Ołdak, Carlo Rivolta, Lisa Roberts, Raj Ramesar, Rasa Strupaitė-Šileikiene, Susanne Kohl, G. Jane Farrar, Marion van Vugt, Jessica van Setten, Susanne Roosing, L. Ingeborgh van den Born, Camiel J.F. Boon, Maria M. van Genderen, Jonas J.W. Kuiper

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

PURPOSE. To determine the profile of inflammation-related proteins and complement system factors in the plasma of CRB1-associated inherited retinal dystrophies (CRB1-IRDs). METHODS. We used the Olink Explore 384 Inflammation II panel for targeted proteomics in 30 cases and 29 controls (cohort I) to identify immune pathways involved in CRB1-IRDs. Genotyping was performed in cohort I and a second cohort of 123 patients from 14 countries and 1292 controls (cohort II). RESULTS. A significant shift in complement cascade factors was observed in plasma proteomes of CRB1-IRD patients (enrichment for complement cascade, Padj = 3.03 × 10^–15). We detected higher plasma levels of complement factor I and complement factor H [CFH] (q = 0.008 and q = 0.046, respectively, adjusted for age and sex), inhibitors of complement component 3 (C3), which correlated significantly (Pearson’s coefficient >0.6) with elevated levels of C3 (q = 0.064). The CRB1 missense variants frequently found in patients showed a strong linkage disequilibrium with the common CFH variant rs7535263 (D^̷ = 0.97 for p.(Cys948Tyr); D^̷ = 1.0 for p.(Arg764Cys)), known to be linked with altered plasma CFH-related protein levels. Correction for the CFH genotype revealed significantly elevated plasma levels of CFH-related 2 (CFHR2) in CRB1-IRD patients (q = 0.041). CONCLUSIONS. CRB1-IRDs are characterized by changes in plasma levels of complement factors and proteins of the innate immune system, and linkage between CRB1 and CFH genes implicates functional variants of the CFH-CFHR locus with specific pathogenic variants of CRB1.

Original language	English
Article number	55
Journal	Investigative ophthalmology & visual science
Volume	66
Issue number	2
DOIs	https://doi.org/10.1167/iovs.66.2.55 https://doi.org/10.1167/iovs.66.2.55
Publication status	Published - Feb 2025

Keywords

CFH
complement
CRB1
inflammation
inherited retinal dystrophy
proteomics

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Elevated Plasma Complement Factors in CRB1-Associated Inherited Retinal DystrophiesFinal published version, 3.82 MBLicence: CC BY-NC-ND

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Moekotte, L., de Boer, J. H., Hiddingh, S., de Ligt, A., Nguyen, X. T. A., Hoyng, C. B., Inglehearn, C. F., McKibbin, M., Lamey, T. M., Thompson, J. A., Chen, F. K., McLaren, T. L., AlTalbishi, A., Panneman, D. M., Boonen, E. G. M., Banfi, S., Bocquet, B., Meunier, I., De Baere, E., ... Kuiper, J. J. W. (2025). Elevated Plasma Complement Factors in CRB1-Associated Inherited Retinal Dystrophies. Investigative ophthalmology & visual science, 66(2), Article 55. https://doi.org/10.1167/iovs.66.2.55, https://doi.org/10.1167/iovs.66.2.55

@article{f51f1fc91c6c4064b603f04e67f0fc4c,

title = "Elevated Plasma Complement Factors in CRB1-Associated Inherited Retinal Dystrophies",

abstract = "PURPOSE. To determine the profile of inflammation-related proteins and complement system factors in the plasma of CRB1-associated inherited retinal dystrophies (CRB1-IRDs). METHODS. We used the Olink Explore 384 Inflammation II panel for targeted proteomics in 30 cases and 29 controls (cohort I) to identify immune pathways involved in CRB1-IRDs. Genotyping was performed in cohort I and a second cohort of 123 patients from 14 countries and 1292 controls (cohort II). RESULTS. A significant shift in complement cascade factors was observed in plasma proteomes of CRB1-IRD patients (enrichment for complement cascade, Padj = 3.03 × 10–15). We detected higher plasma levels of complement factor I and complement factor H [CFH] (q = 0.008 and q = 0.046, respectively, adjusted for age and sex), inhibitors of complement component 3 (C3), which correlated significantly (Pearson{\textquoteright}s coefficient >0.6) with elevated levels of C3 (q = 0.064). The CRB1 missense variants frequently found in patients showed a strong linkage disequilibrium with the common CFH variant rs7535263 (D̷ = 0.97 for p.(Cys948Tyr); D̷ = 1.0 for p.(Arg764Cys)), known to be linked with altered plasma CFH-related protein levels. Correction for the CFH genotype revealed significantly elevated plasma levels of CFH-related 2 (CFHR2) in CRB1-IRD patients (q = 0.041). CONCLUSIONS. CRB1-IRDs are characterized by changes in plasma levels of complement factors and proteins of the innate immune system, and linkage between CRB1 and CFH genes implicates functional variants of the CFH-CFHR locus with specific pathogenic variants of CRB1.",

keywords = "CFH, complement, CRB1, inflammation, inherited retinal dystrophy, proteomics",

author = "Lude Moekotte and {de Boer}, {Joke H.} and Sanne Hiddingh and {de Ligt}, Aafke and Nguyen, {Xuan Thanh An} and Hoyng, {Carel B.} and Inglehearn, {Chris F.} and Martin McKibbin and Lamey, {Tina M.} and Thompson, {Jennifer A.} and Chen, {Fred K.} and McLaren, {Terri L.} and Alaa AlTalbishi and Panneman, {Daan M.} and Boonen, {Erica G.M.} and Sandro Banfi and B{\'e}atrice Bocquet and Isabelle Meunier and {De Baere}, Elfride and Robert Koenekoop and Monika O{\l}dak and Carlo Rivolta and Lisa Roberts and Raj Ramesar and Rasa Strupaitė-{\v S}ileikiene and Susanne Kohl and Farrar, {G. Jane} and {van Vugt}, Marion and {van Setten}, Jessica and Susanne Roosing and {van den Born}, {L. Ingeborgh} and Boon, {Camiel J.F.} and {van Genderen}, {Maria M.} and Kuiper, {Jonas J.W.}",

year = "2025",

month = feb,

doi = "10.1167/iovs.66.2.55",

language = "English",

volume = "66",

journal = "Investigative ophthalmology & visual science",

issn = "0146-0404",

publisher = "Association for Research in Vision and Ophthalmology Inc.",

number = "2",

}

Moekotte, L, de Boer, JH, Hiddingh, S, de Ligt, A, Nguyen, XTA, Hoyng, CB, Inglehearn, CF, McKibbin, M, Lamey, TM, Thompson, JA, Chen, FK, McLaren, TL, AlTalbishi, A, Panneman, DM, Boonen, EGM, Banfi, S, Bocquet, B, Meunier, I, De Baere, E, Koenekoop, R, Ołdak, M, Rivolta, C, Roberts, L, Ramesar, R, Strupaitė-Šileikiene, R, Kohl, S, Farrar, GJ, van Vugt, M , van Setten, J, Roosing, S, van den Born, LI, Boon, CJF, van Genderen, MM & Kuiper, JJW 2025, 'Elevated Plasma Complement Factors in CRB1-Associated Inherited Retinal Dystrophies', Investigative ophthalmology & visual science, vol. 66, no. 2, 55. https://doi.org/10.1167/iovs.66.2.55, https://doi.org/10.1167/iovs.66.2.55

TY - JOUR

T1 - Elevated Plasma Complement Factors in CRB1-Associated Inherited Retinal Dystrophies

AU - Moekotte, Lude

AU - de Boer, Joke H.

AU - Hiddingh, Sanne

AU - de Ligt, Aafke

AU - Nguyen, Xuan Thanh An

AU - Hoyng, Carel B.

AU - Inglehearn, Chris F.

AU - McKibbin, Martin

AU - Lamey, Tina M.

AU - Thompson, Jennifer A.

AU - Chen, Fred K.

AU - McLaren, Terri L.

AU - AlTalbishi, Alaa

AU - Panneman, Daan M.

AU - Boonen, Erica G.M.

AU - Banfi, Sandro

AU - Bocquet, Béatrice

AU - Meunier, Isabelle

AU - De Baere, Elfride

AU - Koenekoop, Robert

AU - Ołdak, Monika

AU - Rivolta, Carlo

AU - Roberts, Lisa

AU - Ramesar, Raj

AU - Strupaitė-Šileikiene, Rasa

AU - Kohl, Susanne

AU - Farrar, G. Jane

AU - van Vugt, Marion

AU - van Setten, Jessica

AU - Roosing, Susanne

AU - van den Born, L. Ingeborgh

AU - Boon, Camiel J.F.

AU - van Genderen, Maria M.

AU - Kuiper, Jonas J.W.

PY - 2025/2

Y1 - 2025/2

N2 - PURPOSE. To determine the profile of inflammation-related proteins and complement system factors in the plasma of CRB1-associated inherited retinal dystrophies (CRB1-IRDs). METHODS. We used the Olink Explore 384 Inflammation II panel for targeted proteomics in 30 cases and 29 controls (cohort I) to identify immune pathways involved in CRB1-IRDs. Genotyping was performed in cohort I and a second cohort of 123 patients from 14 countries and 1292 controls (cohort II). RESULTS. A significant shift in complement cascade factors was observed in plasma proteomes of CRB1-IRD patients (enrichment for complement cascade, Padj = 3.03 × 10–15). We detected higher plasma levels of complement factor I and complement factor H [CFH] (q = 0.008 and q = 0.046, respectively, adjusted for age and sex), inhibitors of complement component 3 (C3), which correlated significantly (Pearson’s coefficient >0.6) with elevated levels of C3 (q = 0.064). The CRB1 missense variants frequently found in patients showed a strong linkage disequilibrium with the common CFH variant rs7535263 (D̷ = 0.97 for p.(Cys948Tyr); D̷ = 1.0 for p.(Arg764Cys)), known to be linked with altered plasma CFH-related protein levels. Correction for the CFH genotype revealed significantly elevated plasma levels of CFH-related 2 (CFHR2) in CRB1-IRD patients (q = 0.041). CONCLUSIONS. CRB1-IRDs are characterized by changes in plasma levels of complement factors and proteins of the innate immune system, and linkage between CRB1 and CFH genes implicates functional variants of the CFH-CFHR locus with specific pathogenic variants of CRB1.

AB - PURPOSE. To determine the profile of inflammation-related proteins and complement system factors in the plasma of CRB1-associated inherited retinal dystrophies (CRB1-IRDs). METHODS. We used the Olink Explore 384 Inflammation II panel for targeted proteomics in 30 cases and 29 controls (cohort I) to identify immune pathways involved in CRB1-IRDs. Genotyping was performed in cohort I and a second cohort of 123 patients from 14 countries and 1292 controls (cohort II). RESULTS. A significant shift in complement cascade factors was observed in plasma proteomes of CRB1-IRD patients (enrichment for complement cascade, Padj = 3.03 × 10–15). We detected higher plasma levels of complement factor I and complement factor H [CFH] (q = 0.008 and q = 0.046, respectively, adjusted for age and sex), inhibitors of complement component 3 (C3), which correlated significantly (Pearson’s coefficient >0.6) with elevated levels of C3 (q = 0.064). The CRB1 missense variants frequently found in patients showed a strong linkage disequilibrium with the common CFH variant rs7535263 (D̷ = 0.97 for p.(Cys948Tyr); D̷ = 1.0 for p.(Arg764Cys)), known to be linked with altered plasma CFH-related protein levels. Correction for the CFH genotype revealed significantly elevated plasma levels of CFH-related 2 (CFHR2) in CRB1-IRD patients (q = 0.041). CONCLUSIONS. CRB1-IRDs are characterized by changes in plasma levels of complement factors and proteins of the innate immune system, and linkage between CRB1 and CFH genes implicates functional variants of the CFH-CFHR locus with specific pathogenic variants of CRB1.

KW - CFH

KW - complement

KW - CRB1

KW - inflammation

KW - inherited retinal dystrophy

KW - proteomics

UR - http://www.scopus.com/inward/record.url?scp=85218985127&partnerID=8YFLogxK

U2 - 10.1167/iovs.66.2.55

DO - 10.1167/iovs.66.2.55

M3 - Article

C2 - 39982393

AN - SCOPUS:85218985127

SN - 0146-0404

VL - 66

JO - Investigative ophthalmology & visual science

JF - Investigative ophthalmology & visual science

IS - 2

M1 - 55

ER -

Elevated Plasma Complement Factors in CRB1-Associated Inherited Retinal Dystrophies

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