Organization of the autoantibody repertoire in healthy newborns and adults revealed by system level informatics of antigen microarray data

Madi, Asaf; Hecht, Inbal; Bransburg-Zabary, Sharron; Merbl, Yifat; Pick, Adi; Zucker-Toledano, Merav; Quintana, Francisco J.; Tauber, Alfred I.; Cohen, Irun R.; Ben‐Jacob, Eshel

doi:10.1073/pnas.0901528106

Cited by 86 publications

(112 citation statements)

References 37 publications

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“…2C and 2D show that individual newborn IgM and IgA repertoires, relative to the scatter of maternal repertoires, were much more tightly packed in repertoire space; thus, the IgM and IgA cord serum isotypes showed a much higher correlation between the repertoires of individual newborns than did the individual IgM and IgA isotypes of their mothers. In other words, the IgM and IgA Abs produced by developing babies in utero manifest relatively similar global repertoires (13,14). Fig.…”

Section: Correlations Among Igg Igm and Iga Isotype Repertoiresmentioning

confidence: 99%

“…We used some of the same Ags as in the previous studies of healthy autoimmune repertoires (13,14); these included proteins, synthetic peptides from the sequences of key proteins, nucleotides, phospholipids, and other self and nonself molecules. See Supplemental Table I for the full list.…”

Section: Agsmentioning

confidence: 99%

“…1 for additional details). For dimensional reduction we used the Principal Component Analysis (PCA) algorithm (18) on the normalized Pearson correlation matrices, as previously described (13). Note that subjects manifesting relatively high normalized correlations are closely located in the three-dimensional space.…”

Section: Data Preprocessing Background Filtering and Analysismentioning

confidence: 99%

“…The blood samples were allowed to clot at room temperature. After centrifugation, sera were collected and stored at 220˚C (13,14).…”

Section: Serum Samplesmentioning

confidence: 99%

“…The women were all healthy, and their newborns' gestational age ranged from week 27 to 41. The soluble fraction of the milk was separated from the fat by centrifugation, collected, and stored at 220˚C (13,14).…”

Section: Milk Samplesmentioning

confidence: 99%

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Tumor-Associated and Disease-Associated Autoantibody Repertoires in Healthy Colostrum and Maternal and Newborn Cord Sera

Madi

Bransburg-Zabary

Maayan-Metzger

et al. 2015

The Journal of Immunology

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In this work, we studied autoantibody repertoires and Ig isotypes in 71 mothers and their 104 healthy newborns (including twins and triplets delivered term or premature). Newborns receive maternal IgG Abs via the placenta before birth, but developing infants must produce their own IgM and IgA Abs. We used an Ag microarray analysis to detect binding to a selection of 295 self-Ags, compared with 27 standard foreign Ags. The magnitude of binding to specific self-Ags was found to be not less than that to the foreign Ags. As expected, each newborn shared with its mother a similar IgG repertoire—manifest as early as the 24th week of gestation. IgM and IgA autoantibody repertoires in cord sera were highly correlated among the newborns and differed from their mothers’ repertoires; the latter differed in sera and milk. The autoantibodies bound to self-Ags known to be associated with tumors and to autoimmune diseases. Thus, autoantibody repertoires in healthy humans—the immunological homunculus—arise congenitally, differ in maternal milk and sera, and mark the potential of the immune system to attack tumors, beneficially, or healthy tissues, harmfully; regulation of the tissue site, the dynamics, and the response phenotype of homuncular autoimmunity very likely affects health.

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Section: Correlations Among Igg Igm and Iga Isotype Repertoiresmentioning

confidence: 99%

Section: Agsmentioning

confidence: 99%

Section: Data Preprocessing Background Filtering and Analysismentioning

confidence: 99%

“…The blood samples were allowed to clot at room temperature. After centrifugation, sera were collected and stored at 220˚C (13,14).…”

Section: Serum Samplesmentioning

confidence: 99%

Section: Milk Samplesmentioning

confidence: 99%

See 3 more Smart Citations

Tumor-Associated and Disease-Associated Autoantibody Repertoires in Healthy Colostrum and Maternal and Newborn Cord Sera

Madi

Bransburg-Zabary

Maayan-Metzger

et al. 2015

The Journal of Immunology

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Human neonatal thymectomy induces altered B‐cell responses and autoreactivity

et al. 2017

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An association between T‐cell lymphopenia and autoimmunity has long been proposed, but it remains to be elucidated whether T‐cell lymphopenia affects B‐cell responses to autoantigens. Human neonatal thymectomy (Tx) results in a decrease in T‐cell numbers and we used this model to study the development of autoreactivity. Two cohorts of neonatally thymectomized individuals were examined, a cohort of young (1–5 years post‐Tx, n = 10–27) and older children (>10 years, n = 26), and compared to healthy age‐matched controls. T‐cell and B‐cell subsets were assessed and autoantibody profiling performed. Early post‐Tx, a decrease in T‐cell numbers (2.75 × 109/L vs. 0.71 × 109/L) and an increased proportion of memory T cells (19.72 vs. 57.43%) were observed. The presence of autoantibodies was correlated with an increased proportion of memory T cells in thymectomized children. No differences were seen in percentages of different B‐cell subsets between the groups. The autoantigen microarray showed a skewed autoantibody response after Tx. In the cohort of older individuals, autoantibodies were present in 62% of the thymectomized children, while they were found in only 33% of the healthy controls. Overall, our data suggest that neonatal Tx skews the autoantibody profile. Preferential expansion and preservation of Treg (regulatory T) cell stability and function, may contribute to preventing autoimmune disease development after Tx.

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Current Status and Prospective Regarding the Therapeutic Potential of Natural Autoantibodies in Cancer Therapy

Ebrahimnezhad

Jazayeri

Hassanian

et al. 2017

Journal Cellular Physiology

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The presence of natural auto-antibodies (NAbs) in normal range/activity in healthy individuals is essential for body to maintain hemostasis, which are directed to self and altered self-components, while abnormal activity of this system can be associated with several health related diseases. It has been shown that NAbs regulate immune system, and can be changed during the individual's life. In other word, the level and pattern of Nabs is among the main factors to define the state of the body, suggesting their prognostic values as markers of immune system impairment such as autoimmunity and cancer. Such NAbs have gained substantial attention because several of them, including their recombinant forms, have therapeutic potential (e.g., programmed cell death-1 [PD-1, Pdcd1], which some of its inhibitors have been approved by FDA for cancer therapy). Whereas a large number of IgM and IgG NAbs have a key role in tissue homeostasis, while others modulate cellular and enzyme properties. The aim of current review is to give an overview about some of these NAbs and how these low-titer/affinity interact with Ag in homeostasis, with particular emphasis on related diseases such as systemic inflammatory response syndrome and cancer, and their application as potential therapeutic target for cancer therapy.

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Organization of the autoantibody repertoire in healthy newborns and adults revealed by system level informatics of antigen microarray data

Cited by 86 publications

References 37 publications

Tumor-Associated and Disease-Associated Autoantibody Repertoires in Healthy Colostrum and Maternal and Newborn Cord Sera

Tumor-Associated and Disease-Associated Autoantibody Repertoires in Healthy Colostrum and Maternal and Newborn Cord Sera

Human neonatal thymectomy induces altered B‐cell responses and autoreactivity

Current Status and Prospective Regarding the Therapeutic Potential of Natural Autoantibodies in Cancer Therapy

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