Citrullination of a phage-displayed human peptidome library reveals the fine specificities of rheumatoid arthritis-associated autoantibodies

Román‐Meléndez, Gabriel D.; Monaco, Daniel R.; Montagne, Janelle M.; Quizon, Rachel S.; Konig, Maximilian F.; Astatke, Mekbib; Darrah, Erika; Larman, H. Benjamin

doi:10.1016/j.ebiom.2021.103506

Cited by 11 publications

(7 citation statements)

References 51 publications

(47 reference statements)

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“…PhIP-seq is a powerful tool for antigen discovery due to its throughput and scalability. Continually declining costs in sequencing paired with scaled protocols such as the ones presented here result in a low per-sample cost and experimental time, and declining costs of custom oligonucleotide based-libraries allow for extensive adaptation ( Román-Meléndez et al, 2021 ; Vogl et al, 2021 ). Yet, as the technology is relatively new, increased discussion around best practices in experimental design, methodology, and data interpretation would be beneficial.…”

Section: Discussionmentioning

confidence: 99%

“…Similarly, the increased sensitivity of whole protein validation relative to PhIP-seq for BTNL8 autoantibodies highlights the need for rapid and sensitive secondary assays to confirm or even increase the importance of a given candidate antigen. These principles may be extended to other related PhIP-seq modalities ( Mina et al, 2019 ; Román-Meléndez et al, 2021 ; Vogl et al, 2021 ).…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Autoantibody discovery across monogenic, acquired, and COVID-19-associated autoimmunity with scalable PhIP-seq

Vazquez

Mann

Bodansky

et al. 2022

eLife

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Phage Immunoprecipitation-Sequencing (PhIP-Seq) allows for unbiased, proteome-wide autoantibody discovery across a variety of disease settings, with identification of disease-specific autoantigens providing new insight into previously poorly understood forms of immune dysregulation. Despite several successful implementations of PhIP-Seq for autoantigen discovery, including our previous work (Vazquez et al. 2020), current protocols are inherently difficult to scale to accommodate large cohorts of cases and importantly, healthy controls. Here, we develop and validate a high throughput extension of PhIP-seq in various etiologies of autoimmune and inflammatory diseases, including APS1, IPEX, RAG1/2 deficiency, Kawasaki Disease (KD), Multisystem Inflammatory Syndrome in Children (MIS-C), and finally, mild and severe forms of COVID19. We demonstrate that these scaled datasets enable machine-learning approaches that result in robust prediction of disease status, as well as the ability to detect both known and novel autoantigens, such as PDYN in APS1 patients, and intestinally expressed proteins BEST4 and BTNL8 in IPEX patients. Remarkably, BEST4 antibodies were also found in 2 patients with RAG1/2 deficiency, one of whom had very early onset IBD. Scaled PhIP-Seq examination of both MIS-C and KD demonstrated rare, overlapping antigens, including CGNL1, as well as several strongly enriched putative pneumonia-associated antigens in severe COVID19, including the endosomal protein EEA1. Together, scaled PhIP-Seq provides a valuable tool for broadly assessing both rare and common autoantigen overlap between autoimmune diseases of varying origins and etiologies.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Autoantibody discovery across monogenic, acquired, and COVID-19-associated autoimmunity with scalable PhIP-seq

Vazquez

Mann

Bodansky

et al. 2022

eLife

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“…Similarly, as phage displayed peptide tiles are products of bacteria, PhIP-Seq inherently lacks eukaryotic post-translational modifications (PTMs) of proteins and therefore can pose a challenge in cases where PTMs on pathogens are targeted by the humoral immune response. The PTM problem is partially addressed in a recent work where the investigators used a phage library modified by a PTM enzyme, calcium-dependent peptidylarginine deaminase (PAD), to citrullinate relevant peptide tiles [ 40 ]. While this proof-of-concept study was successful in improving the detection of citrullinated proteins in patients with rheumatoid arthritis, more work must be performed to cover the numerous other PTM processes in eukaryotic cells.…”

Section: Improving Phip-seqmentioning

confidence: 99%

Phage ImmunoPrecipitation Sequencing (PhIP-Seq): The Promise of High Throughput Serology

et al. 2022

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Phage ImmunoPrecipitation Sequencing (PhIP-Seq) is a high throughput serological technology that is revolutionizing the manner in which we track antibody profiles. In this review, we mainly focus on its application to viral infectious diseases. Through the pull-down of patient antibodies using peptide-tile-expressing T7 bacteriophages and detection using next-generation sequencing (NGS), PhIP-Seq allows the determination of antibody repertoires against peptide targets from hundreds of proteins and pathogens. It differs from conventional serological techniques in that PhIP-Seq does not require protein expression and purification. It also allows for the testing of many samples against the whole virome. PhIP-Seq has been successfully applied in many infectious disease investigations concerning seroprevalence, risk factors, time trends, etiology of disease, vaccinology, and emerging pathogens. Despite the inherent limitations of this technology, we foresee the future expansion of PhIP-Seq in both investigative studies and tracking of current, emerging, and novel viruses. Following the review of PhIP-Seq technology, its limitations, and applications, we recommend that PhIP-Seq be integrated into national surveillance programs and be used in conjunction with molecular techniques to support both One Health and pandemic preparedness efforts.

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“…This has previously also been demonstrated using the VirScan platform for screening of antibody responses to common viruses [4]. In Rom an-Mel endez et al [2], this concept is further advanced by developing a T7 proteomic platform for mapping autoantibody responses to PTM antigens targeted by ACPA in RA.…”

mentioning

confidence: 99%

“…In the current study by Rom an-Mel endez et al [2], the scope has been to use phage display technology to help define the breadth of anti-citrullinated peptide autoantibodies (ACPA) in rheumatoid arthritis (RA). Within the field of clinical immunology, a positive serological antibody test is often part of the clinical diagnostic criteria, and in many disease settings the precise target(s) of autoantibodies are well understood.…”

mentioning

confidence: 99%

New technologies laying a foundation for next generation clinical serology

Grönwall

Malmström

2021

eBioMedicine

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Citrullination of a phage-displayed human peptidome library reveals the fine specificities of rheumatoid arthritis-associated autoantibodies

Cited by 11 publications

References 51 publications

Autoantibody discovery across monogenic, acquired, and COVID-19-associated autoimmunity with scalable PhIP-seq

Autoantibody discovery across monogenic, acquired, and COVID-19-associated autoimmunity with scalable PhIP-seq

Phage ImmunoPrecipitation Sequencing (PhIP-Seq): The Promise of High Throughput Serology

New technologies laying a foundation for next generation clinical serology

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