Your search keyword '"Dimitrov, Jordan D."' showing total 32 results

1. TCTP regulates genotoxic stress and tumorigenicity via intercellular vesicular signaling.

Author

Amson, Robert, Senff-Ribeiro, Andrea, Karafin, Teele, Lespagnol, Alexandra, Honoré, Joane, Baylot, Virginie, Banroques, Josette, Tanner, N Kyle, Chamond, Nathalie, Dimitrov, Jordan D, Hoebeke, Johan, Droin, Nathalie M, Job, Bastien, Piard, Jonathan, Bommer, Ulrich-Axel, Choi, Kwang-Wook, Abdelfatah, Sara, Efferth, Thomas, Telerman, Stephanie B, and Geyer, Felipe Correa

Abstract

Oncogenic intercellular signaling is regulated by extracellular vesicles (EVs), but the underlying mechanisms remain mostly unclear. Since TCTP (translationally controlled tumor protein) is an EV component, we investigated whether it has a role in genotoxic stress signaling and malignant transformation. By generating a Tctp-inducible knockout mouse model (Tctp–/f–), we report that Tctp is required for genotoxic stress-induced apoptosis signaling via small EVs (sEVs). Human breast cancer cells knocked-down for TCTP show impaired spontaneous EV secretion, thereby reducing sEV-dependent malignant growth. Since Trp53–/– mice are prone to tumor formation, we derived tumor cells from Trp53–/–;Tctp–/f– double mutant mice and describe a drastic decrease in tumori-genicity with concomitant decrease in sEV secretion and content. Remarkably, Trp53–/–;Tctp–/f– mice show highly prolonged survival. Treatment of Trp53–/– mice with sertraline, which inhibits TCTP function, increases their survival. Mechanistically, TCTP binds DDX3, recruiting RNAs, including miRNAs, to sEVs. Our findings establish TCTP as an essential protagonist in the regulation of sEV-signaling in the context of apoptosis and tumorigenicity. Synopsis: Signaling via small extracellular vesicles (sEVs) is crucial for the regulation of cell fate. This study shows that TCTP is an essential component of sEVs, regulating their secretion, protein and RNA content, affecting thereby both apoptosis and cancer. Tctp–/f– sEVs have impaired cell death signaling capacity upon genotoxic stress. Deletion of Tctp reprograms/reverts Trp53–/–-driven tumorigenesis. Tumor-derived sEVs promote malignant transformation in a TCTP-dependent manner. TCTP binds DDX3 to regulate the transport of microRNAs into sEVs. Signaling via small extracellular vesicles (sEVs) is crucial for the regulation of cell fate. This study shows that TCTP is an essential component of sEVs, regulating their secretion, protein and RNA content, affecting thereby both apoptosis and cancer. [ABSTRACT FROM AUTHOR]

Published

2024

2. Polyreactivity of antibodies from different B-cell subpopulations is determined by distinct sequence patterns of variable region.

Author

Lecerf, Maxime, Lacombe, Robin V., and Dimitrov, Jordan D.

Subjects

IMMUNOGLOBULIN light chains, IMMUNOGLOBULIN heavy chains, IMMUNOGLOBULINS, AMINO acid residues, TALL-1 (Protein), SEQUENCE analysis

Abstract

An antibody molecule that can bind to multiple distinct antigens is defined as polyreactive. In the present study, we performed statistical analyses to assess sequence correlates of polyreactivity of >600 antibodies cloned from different Bcell types of healthy humans. The data revealed several sequence patterns of variable regions of heavy and light immunoglobulin chains that determine polyreactivity. The most prominent identified patterns were increased number of basic amino acid residues, reduced frequency of acidic residues, increased number of aromatic and hydrophobic residues, and longer length of CDR L1. Importantly, our study revealed that antibodies isolated from different B-cell populations used distinct sequence patterns (or combinations of them) for polyreactive antigen binding. Furthermore, we combined the data from sequence analyses with molecular modeling of selected polyreactive antibodies and demonstrated that human antibodies can use multiple pathways for achieving antigen-binding promiscuity. These data reconcile some contradictions in the literature regarding the determinants of antibody polyreactivity. Moreover, our study demonstrates that the mechanism of polyreactivity of antibodies evolves during immune response and might be tailored to specific functional properties of different B-cell compartments. Finally, these data can be of use for efforts in the development and engineering of therapeutic antibodies. [ABSTRACT FROM AUTHOR]

Published

2023

3. HIV-1 treatment timing shapes the human intestinal memory B-cell repertoire to commensal bacteria.

Author

Planchais, Cyril, Molinos-Albert, Luis M., Rosenbaum, Pierre, Hieu, Thierry, Kanyavuz, Alexia, Clermont, Dominique, Prazuck, Thierry, Lefrou, Laurent, Dimitrov, Jordan D., Hüe, Sophie, Hocqueloux, Laurent, and Mouquet, Hugo

Subjects

B cells, IMMUNOLOGIC memory, HIV, MEMORY, INTESTINAL abnormalities, B cell receptors, HUMORAL immunity

Abstract

HIV-1 infection causes severe alterations of gut mucosa, microbiota and immune system, which can be curbed by early antiretroviral therapy. Here, we investigate how treatment timing affects intestinal memory B-cell and plasmablast repertoires of HIV-1-infected humans. We show that only class-switched memory B cells markedly differ between subjects treated during the acute and chronic phases of infection. Intestinal memory B-cell monoclonal antibodies show more prevalent polyreactive and commensal bacteria-reactive clones in late- compared to early-treated individuals. Mirroring this, serum IgA polyreactivity and commensal-reactivity are strongly increased in late-treated individuals and correlate with intestinal permeability and systemic inflammatory markers. Polyreactive blood IgA memory B cells, many of which egressed from the gut, are also substantially enriched in late-treated individuals. Our data establish gut and systemic B-cell polyreactivity to commensal bacteria as hallmarks of chronic HIV-1 infection and suggest that initiating treatment early may limit intestinal B-cell abnormalities compromising HIV-1 humoral response. HIV-1 infection is known to impact the gut mucosa, effecting the microbiota and immune system, but early antiretroviral therapy is linked to partial reversal of this phenomena. Here the authors explore the impact of early commencement of antiretroviral therapy and show this can limit the abnormal responses of intestinal B cells associated with HIV-1 infection. [ABSTRACT FROM AUTHOR]

Published

2023

4. Basic Mechanisms of Hemolysis-Associated Thrombo-Inflammation and Immune Dysregulation.

Author

Dimitrov, Jordan D., Roumenina, Lubka T., Perrella, Gina, and Rayes, Julie

Published

2023

5. Editorial: Mechanisms and strategies of unconventional antibody diversification for greater immune adaptability.

Author

Dimitrov, Jordan D., Mwangi, Waithaka, and Xiaotian Zhong

Subjects

IMMUNOGLOBULINS, POST-translational modification

Published

2023

6. Hyperoxidized Species of Heme Have a Potent Capacity to Induce Autoreactivity of Human IgG Antibodies.

Author

Wiatr, Marie, Hadzhieva, Maya, Lecerf, Maxime, Noé, Rémi, Justesen, Sune, Lacroix-Desmazes, Sébastien, Dragon-Durey, Marie-Agnès, and Dimitrov, Jordan D.

Subjects

FC receptors, HEME, IMMUNOGLOBULINS, IMMUNOGLOBULIN G, IRON oxidation, OXIDIZING agents, IRON in the body

Abstract

The interaction of some human antibodies with heme results in posttranslational acquisition of binding to various self- and pathogen-derived antigens. The previous studies on this phenomenon were performed with oxidized heme (Fe3+). In the present study, we elucidated the effect of other pathologically relevant species of heme, i.e., species that were formed after contact of heme with oxidizing agents such as hydrogen peroxide, situations in which heme's iron could acquire higher oxidation states. Our data reveal that hyperoxidized species of heme have a superior capacity to heme (Fe3+) in triggering the autoreactivity of human IgG. Mechanistic studies demonstrated that oxidation status of iron was of critical importance for the heme's effect on antibodies. We also demonstrated that hyperoxidized heme species interacted at higher affinities with IgG and that this binding occurred through a different mechanism as compared to heme (Fe3+). Regardless of their profound functional impact on the antigen-binding properties of antibodies, hyperoxidized species of heme did not affect Fc-mediated functions of IgG, such as binding to the neonatal Fc receptor. The obtained data contribute to a better understanding of the pathophysiological mechanism of hemolytic diseases and of the origin of elevated antibody autoreactivity in patients with some hemolytic disorders. [ABSTRACT FROM AUTHOR]

Published

2023

7. Oxidized hemoglobin triggers polyreactivity and autoreactivity of human IgG via transfer of heme.

Author

Planchais, Cyril, Noe, Remi, Gilbert, Marie, Lecerf, Maxime, Kaveri, Srini V., Lacroix-Desmazes, Sébastien, Roumenina, Lubka T., and Dimitrov, Jordan D.

Subjects

HEMOGLOBINS, HEME, MYOGLOBIN, IMMUNOGLOBULIN G, GLOBIN, MONOCLONAL antibodies, IMMUNOGLOBULINS, SITE-specific mutagenesis

Abstract

Intravascular hemolysis occurs in diverse pathological conditions. Extracellular hemoglobin and heme have strong pro-oxidative and pro-inflammatory potentials that can contribute to the pathology of hemolytic diseases. However, many of the effects of extracellular hemoglobin and heme in hemolytic diseases are still not well understood. Here we demonstrate that oxidized hemoglobin (methemoglobin) can modify the antigen-binding characteristics of human immunoglobulins. Thus, incubation of polyclonal or some monoclonal human IgG in the presence of methemoglobin results in an appearance of binding reactivities towards distinct unrelated self-proteins, including the protein constituent of hemoglobin i.e., globin. We demonstrate that a transfer of heme from methemoglobin to IgG is indispensable for this acquisition of antibody polyreactivity. Our data also show that only oxidized form of hemoglobin have the capacity to induce polyreactivity of antibodies. Site-directed mutagenesis of a heme-sensitive human monoclonal IgG1 reveals details about the mechanism of methemoglobin-induced antigen-binding polyreactivity. Further here we assess the kinetics and thermodynamics of interaction of a heme-induced polyreactive human antibody with hemoglobin and myoglobin. Taken together presented data contribute to a better understanding of the functions of extracellular hemoglobin in the context of hemolytic diseases. Oxidized hemoglobin induces polyreactivity and autoreactivity of human IgG through direct transfer and binding of heme to the variable region of IgG, which contributes to a better understanding of the physiopathology of hemolytic diseases. [ABSTRACT FROM AUTHOR]

Published

2023

8. Evolutionary trajectory of receptor binding specificity and promiscuity of the spike protein of SARS‐CoV‐2.

Author

Planchais, Cyril, Reyes‐Ruiz, Alejandra, Lacombe, Robin, Zarantonello, Alessandra, Lecerf, Maxime, Revel, Margot, Roumenina, Lubka T., Atanasov, Boris P., Mouquet, Hugo, and Dimitrov, Jordan D.

Abstract

SARS‐CoV‐2 infects cells by attachment to its receptor—the angiotensin converting enzyme 2 (ACE2). Regardless of the wealth of structural data, little is known about the physicochemical mechanism of interactions of the viral spike (S) protein with ACE2 and how this mechanism has evolved during the pandemic. Here, we applied experimental and computational approaches to characterize the molecular interaction of S proteins from SARS‐CoV‐2 variants of concern (VOC). Data on kinetics, activation‐, and equilibrium thermodynamics of binding of the receptor binding domain (RBD) from VOC with ACE2 as well as data from computational protein electrostatics revealed a profound remodeling of the physicochemical characteristics of the interaction during the evolution. Thus, as compared to RBDs from Wuhan strain and other VOC, Omicron RBD presented as a unique protein in terms of conformational dynamics and types of non‐covalent forces driving the complex formation with ACE2. Viral evolution resulted in a restriction of the RBD structural dynamics, and a shift to a major role of polar forces for ACE2 binding. Further, we investigated how the reshaping of the physicochemical characteristics of interaction affects the binding specificity of S proteins. Data from various binding assays revealed that SARS‐CoV‐2 Wuhan and Omicron RBDs manifest capacity for promiscuous recognition of unrelated human proteins, but they harbor distinct reactivity patterns. These findings might contribute for mechanistic understanding of the viral tropism and capacity to evade immune responses during evolution. [ABSTRACT FROM AUTHOR]

Published

2022

9. Assessment of the breadth of binding promiscuity of heme towards human proteins.

Author

Roumenina, Lubka T. and Dimitrov, Jordan D.

Subjects

HEME, DNA-binding proteins, CARRIER proteins, PROTEIN microarrays, PROTEINS

Abstract

Heme regulates important biological processes by transient interactions with many human proteins. The goal of the present study was to assess extends of protein binding promiscuity of heme. To this end we evaluated interaction of heme with >9000 human proteins. Heme manifested high binding promiscuity by binding to most of the proteins in the array. Nevertheless, some proteins have outstanding heme binding capacity. Bioinformatics analyses revealed that apart from typical haemoproteins, these proteins are frequently involved in metal binding or have the potential to recognize DNA. This study can contribute for understanding the regulatory functions of labile heme. [ABSTRACT FROM AUTHOR]

Published

2022

10. Heme Interferes With Complement Factor I-Dependent Regulation by Enhancing Alternative Pathway Activation.

Author

Gerogianni, Alexandra, Dimitrov, Jordan D., Zarantonello, Alessandra, Poillerat, Victoria, Chonat, Satheesh, Sandholm, Kerstin, McAdam, Karin E., Ekdahl, Kristina N., Mollnes, Tom E., Mohlin, Camilla, Roumenina, Lubka T., and Nilsson, Per H.

Subjects

HEME, PAROXYSMAL hemoglobinuria, COMPLEMENT factor H, BLOOD proteins, SICKLE cell anemia, COMPLEMENT receptors

Abstract

Hemolysis, as a result of disease or exposure to biomaterials, is characterized by excess amounts of cell-free heme intravascularly and consumption of the protective heme-scavenger proteins in plasma. The liberation of heme has been linked to the activation of inflammatory systems, including the complement system, through alternative pathway activation. Here, we investigated the impact of heme on the regulatory function of the complement system. Heme dose-dependently inhibited factor I-mediated degradation of soluble and surface-bound C3b, when incubated in plasma or buffer with complement regulatory proteins. Inhibition occurred with factor H and soluble complement receptor 1 as co-factors, and the mechanism was linked to the direct heme-interaction with factor I. The heme-scavenger protein hemopexin was the main contaminant in purified factor I preparations. This led us to identify that hemopexin formed a complex with factor I in normal human plasma. These complexes were significantly reduced during acute vasoocclusive pain crisis in patients with sickle cell disease, but the complexes were normalized at their baseline outpatient clinic visit. Hemopexin exposed a protective function of factor I activity in vitro, but only when it was present before the addition of heme. In conclusion, we present a mechanistic explanation of how heme promotes uncontrolled complement alternative pathway amplification by interfering with the regulatory capacity of factor I. Reduced levels of hemopexin and hemopexin-factor I complexes during an acute hemolytic crisis is a risk factor for heme-mediated factor I inhibition. [ABSTRACT FROM AUTHOR]

Published

2022

11. The receptor for advanced glycation end products is a sensor for cell‐free heme.

Author

May, Olivia, Yatime, Laure, Merle, Nicolas S., Delguste, Florian, Howsam, Mike, Daugan, Marie V., Paul‐Constant, Charles, Billamboz, Muriel, Ghinet, Alina, Lancel, Steve, Dimitrov, Jordan D., Boulanger, Eric, Roumenina, Lubka T., and Frimat, Marie

Subjects

ADVANCED glycation end-products, RECEPTOR for advanced glycation end products (RAGE), HEME, TOLL-like receptors

Abstract

Heme's interaction with Toll‐like receptor 4 (TLR4) does not fully explain the proinflammatory properties of this hemoglobin‐derived molecule during intravascular hemolysis. The receptor for advanced glycation end products (RAGE) shares many features with TLR4 such as common ligands and proinflammatory, prothrombotic, and pro‐oxidative signaling pathways, prompting us to study its involvement as a heme sensor. Stable RAGE‐heme complexes with micromolar affinity were detected as heme‐mediated RAGE oligomerization. The heme‐binding site was located in the V domain of RAGE. This interaction was Fe3+‐dependent and competitive with carboxymethyllysine, another RAGE ligand. We confirmed a strong basal gene expression of RAGE in mouse lungs. After intraperitoneal heme injection, pulmonary TNF‐α, IL1β, and tissue factor gene expression levels increased in WT mice but were significantly lower in their RAGE−/− littermates. This may be related to the lower activation of ERK1/2 and Akt observed in the lungs of heme‐treated, RAGE−/− mice. Overall, heme binds to RAGE with micromolar affinity and could promote proinflammatory and prothrombotic signaling in vivo, suggesting that this interaction could be implicated in heme‐overload conditions. [ABSTRACT FROM AUTHOR]

Published

2021

12. Interaction of clinical-stage antibodies with heme predicts their physiochemical and binding qualities.

Author

Lecerf, Maxime, Kanyavuz, Alexia, Rossini, Sofia, and Dimitrov, Jordan D.

Subjects

IMMUNOGLOBULIN fab fragments, MOLECULAR weights, COFACTORS (Biochemistry), PROTEIN expression, HEME

Abstract

Immunoglobulin repertoires contain a fraction of antibodies that recognize low molecular weight compounds, including some enzymes' cofactors, such as heme. Here, by using a set of 113 samples with variable region sequences matching clinical-stage antibodies, we demonstrated that a considerable number of these antibodies interact with heme. Antibodies that interact with heme possess specific sequence traits of their antigen-binding regions. Moreover they manifest particular physicochemical and functional qualities i.e. increased hydrophobicity, higher propensity of self-binding, higher intrinsic polyreactivity and reduced expression yields. Thus, interaction with heme is a strong predictor of different molecular and functional qualities of antibodies. Notably, these qualities are of high importance for therapeutic antibodies, as their presence was associated with failure of drug candidates to reach clinic. Our study reveled an important facet of information about relationship sequence-function in antibodies. It also offers a convenient tool for detection of liabilities of therapeutic antibodies. Lecerf et al. examine over 100 samples with variable region sequences matching clinical-stage immunoglobulin antibodies, to demonstrate that many interact with heme. They find that those that do interact with heme possess specific sequence traits that manifest qualities such as increased hydrophobicity, self-binding and intrinsic polyreactivity, thus suggesting that heme interaction is a predictor for therapeutically important qualities. [ABSTRACT FROM AUTHOR]

Published

2021

13. Relevance of the Materno-Fetal Interface for the Induction of Antigen-Specific Immune Tolerance.

Author

Mimoun, Angelina, Delignat, Sandrine, Peyron, Ivan, Daventure, Victoria, Lecerf, Maxime, Dimitrov, Jordan D., Kaveri, Srinivas V., Bayry, Jagadeesh, and Lacroix-Desmazes, Sébastien

Subjects

IMMUNOLOGICAL tolerance, SECOND trimester of pregnancy, FC receptors, TYPE 1 diabetes, ANIMAL models in research

Abstract

In humans, maternal IgGs are transferred to the fetus from the second trimester of pregnancy onwards. The transplacental delivery of maternal IgG is mediated by its binding to the neonatal Fc receptor (FcRn) after endocytosis by the syncytiotrophoblast. IgGs present in the maternal milk are also transferred to the newborn through the digestive epithelium upon binding to the FcRn. Importantly, the binding of IgGs to the FcRn is also responsible for the recycling of circulating IgGs that confers them with a long half-life. Maternally delivered IgG provides passive immunity to the newborn, for instance by conferring protective anti-flu or anti-pertussis toxin IgGs. It may, however, lead to the development of autoimmune manifestations when pathological autoantibodies from the mother cross the placenta and reach the circulation of the fetus. In recent years, strategies that exploit the transplacental delivery of antigen/IgG complexes or of Fc-fused proteins have been validated in mouse models of human diseases to impose antigen-specific tolerance, particularly in the case of Fc-fused factor VIII (FVIII) domains in hemophilia A mice or pre-pro-insulin (PPI) in the case of preclinical models of type 1 diabetes (T1D). The present review summarizes the mechanisms underlying the FcRn-mediated transcytosis of IgGs, the physiopathological relevance of this phenomenon, and the repercussion for drug delivery and shaping of the immune system during its ontogeny. [ABSTRACT FROM AUTHOR]

Published

2020

14. Natural Antibodies: from First-Line Defense Against Pathogens to Perpetual Immune Homeostasis.

Author

Maddur, Mohan S., Lacroix-Desmazes, Sébastien, Dimitrov, Jordan D., Kazatchkine, Michel D., Bayry, Jagadeesh, and Kaveri, Srini V.

Abstract

Natural antibodies (nAbs) are most commonly defined as immunoglobulins present in the absence of pathological conditions or deliberate immunizations. Occurrence of nAbs in germ- and antigen-free mice suggest that their production is driven, at least in part, by self-antigens. Accordingly, nAbs are constituted of natural autoantibodies (nAAbs), and can belong to the IgM, IgG, or IgA subclasses. These nAbs provide immediate protection against infection while the adaptive arm of the immune system mounts a specific and long-term response. Beyond immediate protection from infection, nAbs have been shown to play various functional roles in the immune system, which include clearance of apoptotic debris, suppression of autoimmune and inflammatory responses, regulation of B cell responses, selection of the B cell repertoires, and regulation of B cell development. These various functions of nAbs are afforded by their reactivity, which is broad, cross-reactive, and shown to recognize evolutionarily fixed epitopes shared between foreign and self-antigens. Furthermore, nAbs have unique characteristics that also contribute to their functional roles and set them apart from antigen-specific antibodies. In further support for the role of nAbs in the protection against infections and in the maintenance of immune homeostasis, the therapeutic preparation of polyclonal immunoglobulins, intravenous immunoglobulin (IVIG), rich in nAbs is commonly used in the replacement therapy of primary and secondary immunodeficiencies and in the immunotherapy of a large number of autoimmune and inflammatory diseases. Here, we review several topics on nAbs features and functions, and therapeutic applications in human diseases. [ABSTRACT FROM AUTHOR]

Published

2020

15. P-selectin drives complement attack on endothelium during intravascular hemolysis in TLR-4/heme-dependent manner.

Author

Merle, Nicolas S., Paule, Romain, Leon, Juliette, Daugan, Marie, Robe-Rybkine, Tania, Poillerat, Victoria, Torset, Carine, Frémeaux-Bacchi, Véronique, Dimitrov, Jordan D., and Roumenina, Lubka T.

Subjects

HEMOLYTIC anemia, SELECTIN genetics, HEMOLYSIS & hemolysins, TOLL-like receptors, HEME, CARDIOVASCULAR diseases

Abstract

Hemolytic diseases are frequently linked to multiorgan failure subsequent to vascular damage. Deciphering the mechanisms leading to organ injury upon hemolytic event could bring out therapeutic approaches. Complement system activation occurs in hemolytic disorders, such as sickle cell disease, but the pathological relevance and the acquisition of a complement-activating phenotype during hemolysis remain unclear. Here we found that intravascular hemolysis, induced by injection of phenylhydrazine, resulted in increased alanine aminotransferase plasma levels and NGAL expression. This liver damage was at least in part complement-dependent, since it was attenuated in complement C3-/- mice and by injection of C5-blocking antibody. We evidenced C3 activation fragments' deposits on liver endothelium in mice with intravascular hemolysis or injected with heme as well as on cultured human endothelial cells (EC) exposed to heme. This process was mediated by TLR4 signaling, as revealed by pharmacological blockade and TLR4 deficiency in mice. Mechanistically, TLR4-dependent surface expression of P-selectin triggered an unconventional mechanism of complement activation by noncovalent anchoring of C3 activation fragments, including the typical fluid-phase C3(H2O), measured by surface plasmon resonance and flow cytometry. P-selectin blockade by an antibody prevented complement deposits and attenuated the liver stress response, measured by NGAL expression, in the hemolytic mice. In conclusion, these results revealed the critical impact of the triad TLR4/P-selectin/complement in the liver damage and its relevance for hemolytic diseases. We anticipate that blockade of TLR4, P-selectin, or the complement system could prevent liver injury in hemolytic diseases like sickle cell disease. [ABSTRACT FROM AUTHOR]

Published

2019

16. Conformational Plasticity in Broadly Neutralizing HIV-1 Antibodies Triggers Polyreactivity.

Author

Prigent, Julie, Jarossay, Annaëlle, Planchais, Cyril, Eden, Caroline, Dufloo, Jérémy, Kök, Ayrin, Lorin, Valérie, Vratskikh, Oxana, Couderc, Thérèse, Bruel, Timothée, Schwartz, Olivier, Seaman, Michael S., Ohlenschläger, Oliver, Dimitrov, Jordan D., and Mouquet, Hugo

Abstract

Summary Human high-affinity antibodies to pathogens often recognize unrelated ligands. The molecular origin and the role of this polyreactivity are largely unknown. Here, we report that HIV-1 broadly neutralizing antibodies (bNAbs) are frequently polyreactive, cross-reacting with non-HIV-1 molecules, including self-antigens. Mutating bNAb genes to increase HIV-1 binding and neutralization also results in de novo polyreactivity. Unliganded paratopes of polyreactive bNAbs with improved HIV-1 neutralization exhibit a conformational flexibility, which contributes to enhanced affinity of bNAbs to various HIV-1 envelope glycoproteins and non-HIV antigens. Binding adaptation of polyreactive bNAbs to the divergent ligands mainly involves hydrophophic interactions. Plasticity of bNAbs’ paratopes may, therefore, facilitate accommodating divergent viral variants, but it simultaneously triggers promiscuous binding to non-HIV-1 antigens. Thus, a certain level of polyreactivity can be a mark of adaptable antibodies displaying optimal pathogens’ recognition. [ABSTRACT FROM AUTHOR]

Published

2018

17. Antibody Polyspecificity.

Author

Dimitrov, Jordan D., Pashov, Anastas D., and Vassilev, Tchavdar L.

Published

2012

18. Serum or breast milk immunoglobulins mask the self-reactivity of human natural IgG antibodies.

Author

Djoumerska‐Alexieva, Iglika, Manoylov, Iliyan, Dimitrov, Jordan D., and Tchorbanov, Andrey

Subjects

B cells, IMMUNOGLOBULIN G, ANTIGENS, IMMUNE system, BREAST milk, THERAPEUTICS

Abstract

B cells producing IgG antibodies specific to a variety of self- or foreign antigens are a normal constituent of the immune system of all healthy individuals. These naturally occurring IgG antibodies are found in the serum, external secretions, and pooled human immunoglobulin preparations. They bind with low affinity to antigens, which can also be targets for pathologic autoantibodies. An enhancement of naturally occurring IgG autoantibody activity was observed after treatment of human IgG molecules with protein-destabilizing agents. We have investigated the interactions of human immunoglobulins that were obtained from serum or from breast milk of healthy individuals or IVIg with human liver antigens. Proteins from an individual serum or milk were isolated by two methods, one of which included exposure to low pH and the other did not. Purified serum, mucosal IgM, IgA, and the fraction containing immunoglobulin G F(ab')2 fragments each inhibited the binding of a single donor or pooled IgG to human liver antigens. Our study presents findings regarding the role of the breast milk or serum antibodies in blocking the self-reactivity of IgG antibodies. It supports the suggestion that not IVIg only, but also the pooled human IgM and IgA might possess a potent beneficial immunomodulatory activity in autoimmune patients. [ABSTRACT FROM AUTHOR]

Published

2014

19. Functional Changes of Therapeutic Antibodies upon Exposure to Pro-Oxidative Agents.

Author

Lecerf, Maxime, Lacombe, Robin, Kanyavuz, Alexia, and Dimitrov, Jordan D.

Subjects

IMMUNOGLOBULIN light chains, IMMUNOGLOBULIN heavy chains, IMMUNOGLOBULINS, MONOCLONAL antibodies, IRON ions, ANTIGENS

Abstract

Therapeutic monoclonal antibodies have exerted a transformative impact on clinical practice in last two decades. However, development of a therapeutic antibody remains a complex process. Various physiochemical and functional liabilities can compromise the production or the therapeutic efficacy of antibodies. One of these liabilities is the susceptibility to oxidation. In the present study, we portrayed an oxidation-dependent vulnerability of immunoglobulins that can be of concern for therapeutic antibodies. By using a library of 119 monoclonal IgG1 molecules, containing variable domain matching clinical-stage antibodies, we demonstrated that a substantial number of these molecules acquired antigen-binding polyreactivity upon exposure to ferrous ions. Statistical analyses revealed that the potential for induction of polyreactivity by the redox-active metal ions correlated with a higher number of somatic mutations in V genes encoding variable domains of heavy and light immunoglobulin chains. Moreover, the sensitive antibodies used with biased frequencies particular V gene families encoding variable domains of their light chains. Besides the exposure to ferrous ions the induction of polyreactivity of therapeutic antibodies occurred after contact with an unrelated pro-oxidative substance—hypochlorite ions. Our data also revealed that induction of polyreactivity by pro-oxidative agents did not impact the binding of antibodies to their cognate antigens. The results from this study may contribute for better selection of antibody therapeutics with suitable developability profiles. [ABSTRACT FROM AUTHOR]

Published

2022

20. Diversification posttraductionnelle de la spécificité des immunoglobulines.

Author

Planchais, Cyril, Gupta, Nimesh, Kaveri, Srinivas V., Lacroix-Desmazes, Sebastien, and Dimitrov, Jordan D.

Published

2013

21. Exposure of IgG to an acidic environment results in molecular modifications and in enhanced protective activity in sepsis.

Author

Djoumerska-Alexieva, Iglika K., Dimitrov, Jordan D., Voynova, Elisaveta N., Lacroix-Desmazes, Sebastien, Kaveri, Srinivas V., and Vassilev, Tchavdar L.

Subjects

SEPSIS, IMMUNOGLOBULIN G, ANTIGENS, ENDOTOXINS, IMMUNOTHERAPY

Abstract

IgG molecules are exposed on a regular basis to acidic conditions during immunoaffinity purification procedures, as well as during the production of some therapeutic immunoglobulin preparations. This exposure is known to induce in them an antigen-binding polyreactivity. The molecular mechanisms and the possible biological significance of this phenomenon remain, however, poorly understood. In addition to the previously reported ability of these modified IgG antibodies to interact with a large panel of self-antigens, enhanced binding to non-self-antigens (bacterial), an increased ability to engage in F(ab′)2/F(ab′)2 (idiotype/anti-idiotype) interactions and an increased functional antigen-binding affinity are reported here. The newly acquired ‘induced polyreactivity’ of low-pH buffer-exposed IgG is related to structural changes in the immunoglobulin molecules, and is at least partly attributable to the enhanced role of the hydrophobic effect in their interactions with antigen. Our results suggest that data from many previous studies on monoclonal and polyclonal IgG antibodies purified by low-pH buffer elution from protein A or protein G immunoaffinity columns should be reconsidered, as the procedure itself may have dramatically affected their antigen-binding behavior and biological activity. Low-pH buffer-treated pooled therapeutic immunoglobulins acquire novel beneficial properties, as passive immunotherapy with the pH 4.0 buffer-exposed, but not with the native therapeutic intravenous immunoglobulin preparation, improves the survival of mice with bacterial lipopolysaccharide-induced septic shock. [ABSTRACT FROM AUTHOR]

Published

2010

22. Factor VIII-hydrolyzing IgG in acquired and congenital hemophilia

Author

Wootla, Bharath, Mahendra, Ankit, Dimitrov, Jordan D., Friboulet, Alain, Borel-Derlon, Annie, Rao, Desirazu N., Uda, Taizo, Borg, Jeanne-Yvonne, Bayry, Jagadeesh, Kaveri, Srinivas V., and Lacroix-Desmazes, Sébastien

Subjects

BLOOD coagulation factor VIII, HYDROLYSIS, IMMUNOGLOBULIN G, HEMOPHILIA, AUTOANTIBODIES, HEMOPHILIACS

Abstract

Abstract: Anti-factor VIII (FVIII) inhibitory IgG may arise as alloantibodies to therapeutic FVIII in patients with congenital hemophilia A, or as autoantibodies to endogenous FVIII in individuals with acquired hemophilia. We have described FVIII-hydrolyzing IgG both in hemophilia A patients with anti-FVIII IgG and in acquired hemophilia patients. Here, we compared the properties of proteolytic auto- and allo-antibodies. Rates of FVIII hydrolysis differed significantly between the two groups of antibodies. Proline-phenylalanine-arginine-methylcoumarinamide was a surrogate substrate for FVIII-hydrolyzing autoantibodies. Our data suggest that populations of proteolytic anti-FVIII IgG in acquired hemophilia patients are different from that of inhibitor-positive hemophilia A patients. [Copyright &y& Elsevier]

Published

2009

23. Identification of target antigens of self-reactive IgG in intravenous immunoglobulin preparations.

Author

Bussone, Guillaume, Dib, Hanadi, Dimitrov, Jordan D., Camoin, Luc, Broussard, Cédric, Tamas, Nicolas, Guillevin, Loïc, Kaveri, Srini V., and Mouthon, Luc

Published

2009

24. Compact program resolves overlapping voltammetric peaks.

Author

Dimitrov, Jordan D.

Subjects

VOLTAMMETRY, ELECTROCHEMICAL analysis, MATHEMATICAL optimization, QUANTITATIVE chemical analysis, DATABASES, MATHEMATICAL analysis

Abstract

A simple self-contained program designed to separate overlapping peaks from electrochemical analyses is presented. Combining an original interactive way to define initial parameter estimates with nonlinear curve fitting based on the simplex method of optimization, it allows the user to resolve voltammograms consisting of 2 to 5 analytical peaks raised on a straight base line. The program provides highly intuitive interface, easy operation, and straightforward result documentation. A free package including the program, three data files and user instructions is available on request. [ABSTRACT FROM AUTHOR]

Published

2004

25. "Rational Vaccine Design" for HIV Should Take into Account the Adaptive Potential of Polyreactive Antibodies.

Author

Dimitrov, Jordan D., Kazatchkine, Michel D., Kaveri, Srinivas V., and Lacroix-Desmazes, Sebastien

Subjects

DRUG design, IMMUNOGLOBULINS, DRUG development, HEPATITIS C, IMMUNE response, ADAPTABILITY (Personality), CHEMICAL modification of proteins

Published

2011

26. Protein destabilizing agents induce polyreactivity and enhanced immunomodulatory activity in IVIg preparations.

Author

Djoumerska-Alexieva, Iglika K., Dimitrov, Jordan D., Nacheva, Julia, Kaveri, Srini V., and Vassilev, Tchavdar L.

Subjects

BLOOD protein separation, IMMUNOREGULATION, CYTOKINES, SERUM, SEPTIC shock

Abstract

Normal pooled human IVIg are produced using various blood protein fractionation technologies and as a result they may well differ in their biological properties. We have demonstrated that exposure of IVIg, for a period as short as 15 min, to protein-destabilizing agents like acidic pH, ROS or pro-oxidative ferrous ions dramatically increases the panel of recognized Ag including pro-inflammatory cytokines. We now show that exposure of IVIg to ferrous ions modifies some IgG molecules without denaturating them and enhances the protective activity of the preparation in experimental septic shock. [ABSTRACT FROM AUTHOR]

Published

2009

27. Thermodynamic Analysis of Hepatitis C Virus Vitality in Syringes.

Author

Kang, Jonghoon, Blalock, Garrett R., and Dimitrov, Jordan D.

Published

2011

28. Heme oxygenase-1 is dispensable for the anti-inflammatory activity of intravenous immunoglobulin.

Author

Galeotti, Caroline, Hegde, Pushpa, Das, Mrinmoy, Stephen-Victor, Emmanuel, Canale, Fernando, Muñoz, Marcos, Sharma, Varun K., Dimitrov, Jordan D., Kaveri, Srini V., and Bayry, Jagadeesh

Published

2016

29. Neutralization of Japanese Encephalitis Virus by heme-induced broadly reactive human monoclonal antibody.

Author

Gupta, Nimesh, de Wispelaere, Mélissanne, Lecerf, Maxime, Kalia, Manjula, Scheel, Tobias, Vrati, Sudhanshu, Berek, Claudia, Kaveri, Srinivas V., Desprès, Philippe, Lacroix-Desmazes, Sébastien, and Dimitrov, Jordan D.

Subjects

JAPANESE B encephalitis, ENCEPHALITIS viruses, MONOCLONAL antibody probes, IMMUNOGLOBULINS, HEME

Abstract

Geographical expansion and re-emerging new genotypes of the Japanese encephalitis virus (JEV) require the development of novel therapeutic approaches. Here, we studied a non-conventional approach for antibody therapy and show that, upon exposure to heme, a fraction of natural human immunoglobulins acquires high-affinity reactivity with the antigenic domain-III of JEV E glycoprotein. These JEV-reactive antibodies exhibited neutralizing activity against recently dominant JEV genotypes. This study opens new therapeutic options for Japanese encephalitis. [ABSTRACT FROM AUTHOR]

Published

2015

30. Molecular basis for bacterial peptidoglycan recognition by LysM domains.

Author

Mesnage, Stéphane, Dellarole, Mariano, Baxter, Nicola J., Rouget, Jean-Baptiste, Dimitrov, Jordan D., Wang, Ning, Fujimoto, Yukari, Hounslow, Andrea M., Lacroix-Desmazes, Sébastien, Fukase, Koichi, Foster, Simon J., and Williamson, Michael P.

Published

2014

31. Metrics: journal's impact factor skewed by a single paper.

Author

Dimitrov, Jordan D., Kaveri, Srini V., and Bayry, Jagadeesh

Subjects

LETTERS to the editor, SCIENTISTS

Abstract

A letter to the editor is presented in response to the article about the metrics used in the assessment of the impact of scientists on the publishing behaviour of journals by Jevin West in the previous issue.

Published

2010

32. Cofactor-mediated protein promiscuity.

Author

Dimitrov, Jordan D and Vassilev, Tchavdar L

Subjects

LETTERS to the editor, PROTEIN binding

Abstract

A letter to the editor is presented in response to an article about protein binding, by Nobeli and colleagues, published in the February 2009 issue.

Published

2009