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51. Induction of FOXP3-expressing regulatory CD4pos T cells by human mature autologous dendritic cells

Author

Verhasselt, Valérie, Vosters, Olivier, Beuneu, Claire, Nicaise, Charles, Stordeur, Patrick, Goldman, Michel, Verhasselt, Valérie, Vosters, Olivier, Beuneu, Claire, Nicaise, Charles, Stordeur, Patrick, and Goldman, Michel

Abstract

Current literature suggests that T cells recognizing antigen on mature dendritic cells (DC) differentiate into effector T cells whereas tolerance is induced when antigen is presented by immature DC. We investigated the consequences of the interactions between immature or lipopolysaccharide-matured DC and CD4pos T lymphocytes in absence of foreign antigen. While immature DC did not induce significant CD4pos T cell activation, we observed that a significant fraction of CD4pos T cells cultured with mature autologous DC displayed phenotypic features of activation and produced IL-2, IFN- + ,IL-10 and TGF- g .Furthermore, CD4pos T lymphocytes primed by mature, but not immature, autologous DC acquired regulatory properties. Indeed, when added to an allogeneic mixed leukocyte reaction, they suppressed the response of alloreactive T lymphocytes to the priming DC while responses to third-party stimulators were spared. The generation of CD4pos T cells with regulatory function by autologous stimulation did not require the presence of natural CD4posCD25pos regulatory T cells. In addition, the acquisition of regulatory function by CD4posCD25neg T cells stimulated by autologous mature DC was accompanied by the induction of FOXP3 expression. Our data suggest that during inflammatory conditions, presentation of self antigens by mature DC to autologous T lymphocytes could contribute to the generation of regulatory mechanisms., FLWIN, info:eu-repo/semantics/published

Published
2004

52. Cell-to-cell contact-independent regulatory T cells in human tuberculosis

Author

12th International Congress of Immunology and 4th Annual Meeting of the Federation of Clinical Immunology Societies (FOCIS). (18-23/07/2004: Montreal, Canada), Place, Sammy, Hougardy, Jean-Michel, Temmerman, Stéphane, Leloux, Gaëlle, Hildebrand, Marc, Verhasselt, Valérie, Debrie, Anne-Sophie, Locht, Camille, Mascart, Françoise, 12th International Congress of Immunology and 4th Annual Meeting of the Federation of Clinical Immunology Societies (FOCIS). (18-23/07/2004: Montreal, Canada), Place, Sammy, Hougardy, Jean-Michel, Temmerman, Stéphane, Leloux, Gaëlle, Hildebrand, Marc, Verhasselt, Valérie, Debrie, Anne-Sophie, Locht, Camille, and Mascart, Françoise

Abstract

info:eu-repo/semantics/nonPublished

Published
2004

54. Dendritic cells exposed to nacystelyn are refractory to maturation and promote the emergence of alloreactive regulatory T cells

Author

Neuvième réunion Nantes/Actualités/Transplantation de l'Institut de transplantation et de recherche en transplantation de Nantes (20-21 juin 2002: Nantes, France), Vosters, Olivier, Neve, Jean, Willems, Nicole, Goldman, Michel, Verhasselt, Valérie, Neuvième réunion Nantes/Actualités/Transplantation de l'Institut de transplantation et de recherche en transplantation de Nantes (20-21 juin 2002: Nantes, France), Vosters, Olivier, Neve, Jean, Willems, Nicole, Goldman, Michel, and Verhasselt, Valérie

Abstract

info:eu-repo/semantics/nonPublished

Published
2002

61. Inhibition of human dendritic cell functions by methylprednisolone.

Author

Vanderheyde, N, Verhasselt, Valérie, Goldman, Michel, Willems, Fabienne, Vanderheyde, N, Verhasselt, Valérie, Goldman, Michel, and Willems, Fabienne

Abstract

BACKGROUND: The aim of this study was to better define how glucocorticoids influence primary human T cell responses. Dendritic cells (DC*) are the most effective antigen presenting cells able to activate naive T cells. Previous studies have shown that dexamethasone impaired the function of murine DC. Here, we analyzed how methylprednisolone (MP) might affect the function and maturation of human DC. METHODS: Human DC were generated from peripheral blood mononuclear cells cultured in granulocyte macrophage-colony stimulating factor and interleukin (IL)4. DC maturation was induced either by lipopolysaccharide (LPS) or by fibroblast transfected with the CD40-ligand gene (3T6-CD40L). DC phenotype was characterized by flow cytometric analysis, their cytokine production by ELISA. The ability of DC to activate naive T cells was evaluated in mixed leukocyte reactivity. RESULTS: Although MP did not affect viability of DC, it enhanced their antigen uptake and down-regulated their basal expression of CD86. The expression of CD80 and CD54 by DC was slightly decreased and HLA-DR expression was not modified. MP prevented LPS-induced DC maturation as assessed by the inhibition of CD86, CD80 and CD54 up-regulation, CD83 induction and production of TNF-alpha, IL-6, and IL-12. In contrast, when DC were stimulated by 3T6-CD40L, MP prevented only the synthesis of IL-12. Moreover, MP-treated DC were deficient in their ability to elicit proliferative responses of CD4+CD45RA+ allogeneic T cells as well as their synthesis of interferon (IFN)-gamma, IL-5, and IL-13. CONCLUSION. Glucocorticoids exert potent suppressive effects on human DC and thereby inhibit the induction of primary T cell responses., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published
1999

62. N-acetyl-L-cysteine inhibits primary human T cell responses at the dendritic cell level: association with NF-kappaB inhibition.

Author

Verhasselt, Valérie, Vanden Berghe, Wim, Vanderheyde, N, Willems, Fabienne, Haegeman, Guy, Goldman, Michel, Verhasselt, Valérie, Vanden Berghe, Wim, Vanderheyde, N, Willems, Fabienne, Haegeman, Guy, and Goldman, Michel

Abstract

N-acetyl-L-cysteine (NAC) is an antioxidant molecule endowed with immunomodulatory properties. To investigate the effect of NAC on the induction phase of T cell responses, we analyzed its action on human dendritic cells (DC) derived from adherent PBMC cultured with IL-4 and granulocyte-macrophage CSF. We first found that NAC inhibited the constitutive as well as the LPS-induced activity of the transcription factor NF-kappaB. In parallel, NAC was shown to down-regulate the production of cytokines by DC as well as their surface expression of HLA-DR, CD86 (B7-2), and CD40 molecules both at the basal state and upon LPS activation. NAC also inhibited DC responses induced by CD40 engagement. The inhibitory effects of NAC were not due to nonspecific toxicity as neither the viability of DC nor their mannose receptor-mediated endocytosis were modified by NAC. Finally, we found that the addition of NAC to MLR between naive T cells and allogeneic DC resulted in a profound inhibition of alloreactive responses, which could be attributed to a defect of DC as APC-independent T cell responses were not inhibited by NAC. Altogether, our results suggest that NAC might impair the generation of primary immune responses in humans through its inhibitory action on DC., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published
1999

63. Trypanosoma cruzi infects human dendritic cells and prevents their maturation: inhibition of cytokines, HLA-DR, and costimulatory molecules.

Author

Van Overtvelt, L., Vanderheyde, N, Verhasselt, Valérie, Ismaili, J, De Vos, Louis, Goldman, Michel, Willems, Fabienne, Vray, B, Van Overtvelt, L., Vanderheyde, N, Verhasselt, Valérie, Ismaili, J, De Vos, Louis, Goldman, Michel, Willems, Fabienne, and Vray, B

Abstract

Trypanosoma cruzi, a parasitic protozoan, is the etiological agent of Chagas' disease. Despite the many immune system disorders recognized in this infection and the crucial role played by dendritic cells (DC) in acquired immune responses, it was not known whether these cells could be infected by T. cruzi trypomastigotes and the consequences of such an infection on their immune functions. We now provide evidence that human monocyte-derived DC can be infected by T. cruzi and can support its intracellular multiplication. Interestingly, this infection has functional consequences on immature DC and on their maturation induced by lipopolysaccharide (LPS). First, after T. cruzi infection, the basal synthesis of interleukin-12 (IL-12) and tumor necrosis factor alpha (TNF-alpha) was impaired. Furthermore, the process of maturation of DC induced by LPS was drastically affected by T. cruzi infection. Indeed, secretion of cytokines such as IL-12, TNF-alpha, and IL-6, which are released normally at high levels by LPS-activated DC, as well as the up-regulation of HLA-DR and CD40 molecules, was significantly reduced after this infection. The same effects could be induced by T. cruzi-conditioned medium, indicating that at least these inhibitory effects were mediated by soluble factors released by T. cruzi. Taken together, these results provide new insights into a novel efficient mechanism, directly involving the alteration of DC function, which might be used by T. cruzi to escape the host immune responses in Chagas' disease and thus might favor persistent infection., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published
1999

65. Oxidative stress up-regulates IL-8 and TNF-alpha synthesis by human dendritic cells

Author

Verhasselt, Valérie, Goldman, Michel, Willems, Fabienne, Verhasselt, Valérie, Goldman, Michel, and Willems, Fabienne

Abstract

In addition to their damaging effects, reactive oxygen intermediates exert a regulatory role on gene expression and cell apoptosis. In this study, we evaluated the effects of oxidative stress on human dendritic cells (DC), a cell type which is critical for the initiation of the immune response. For this purpose, we tested the effects of H2O2 on DC derived from adherent peripheral blood mononuclear cells cultured in the presence of granulocyte-macrophage colony-stimulating factor and IL-4. Despite a moderate increase of DC apoptosis in the presence of H2O2, we observed that H2O2 stimulated the production of IL-8 and TFN-alpha by DC in a dose-dependent manner. The induction of cytokine synthesis was found to depend on the oxidative properties of H2O2 as it was inhibited by the addition of catalase, and to require de novo protein synthesis as it was not observed in the presence of cycloheximide. These data suggest that DC could contribute to innate immunity through an enhanced production of inflammatory cytokines in response to oxidative stress., Journal Article, Research Support, Non-U.S. Gov't, FLWIN, info:eu-repo/semantics/published

Published
1998

66. ChemR23, a putative chemoattractant receptor, is expressed in monocyte-derived dendritic cells and macrophages and is a coreceptor for SIV and some primary HIV-1 strains.

Author

Samson, M, Edinger, A L, Stordeur, P, Rucker, J, Verhasselt, Valérie, Sharron, M, Govaerts, Cédric, Mollereau, Catherine, Vassart, Gilbert, Doms, Robert W., Parmentier, Marc, Samson, M, Edinger, A L, Stordeur, P, Rucker, J, Verhasselt, Valérie, Sharron, M, Govaerts, Cédric, Mollereau, Catherine, Vassart, Gilbert, Doms, Robert W., and Parmentier, Marc

Abstract

Leukocyte chemoattractants act through a rapidly growing subfamily of G protein-coupled receptors. We report the cloning of a novel human gene encoding an orphan receptor (ChemR23) related to the C3a, C5a and formyl Met-Leu-Phe receptors, and more distantly to the subfamilies of chemokine receptors. ChemR23 transcripts were found to be abundant in monocyte-derived dendritic cells and macrophages, treated or not with LPS. Low expression could also be detected by reverse transcription-PCR in CD4+ T lymphocytes. The gene encoding ChemR23 was assigned by radiation hybrid mapping to the q21.2-21.3 region of human chromosome 12, outside the gene clusters identified so far for chemoattractant receptors. Given the increasing number of chemoattractant receptors used by HIV-1, HIV-2 and SIV as coreceptors, ChemR23 was tested in fusion assays for potential coreceptor activity by a range of viral strains. None of the tested HIV-2 strains made use of ChemR23 as a coreceptor, but several SIV strains (SIVmac316, SIVmac239, SIVmacl7E-Fr and SIVsm62A), as well as a primary HIV-1 strain (92UG024-2) used it efficiently. ChemR23 therefore appears as a coreceptor for immunodeficiency viruses that does not belong to the chemokine receptor family. It is also a putative chemoattractant receptor relatively specific for antigen-presenting cells, and it could play an important role in the recruitment or trafficking of these cell populations. Future work will be required to identify the ligand(s) of this new G protein-coupled receptor and to define its precise role in the physiology of dendritic cells and macrophages., Journal Article, Research Support, Non-U.S. Gov't, Research Support, U.S. Gov't, P.H.S., FLWIN, info:eu-repo/semantics/published

Published
1998

67. Interleukin-10 prevents the generation of dendritic cells from human peripheral blood mononuclear cells cultured with interleukin-4 and granulocyte/macrophage-colony-stimulating factor

Author

Buelens, Christel, Verhasselt, Valérie, De Groote, Donat, Thielemans, Kris M., Goldman, Michel, Willems, Fabienne, Buelens, Christel, Verhasselt, Valérie, De Groote, Donat, Thielemans, Kris M., Goldman, Michel, and Willems, Fabienne

Abstract

We evaluated the effects of interleukin (IL)-10 on the differentiation of dendritic cells (DC) obtained by culturing plastic-adherent peripheral blood mononuclear cells for 7 days in presence of granulocyte/macrophage-colony-stimulating factor (GM-CSF) + IL-4. The addition of IL-10 at the initiation of culture resulted in the generation of macrophage-like cells with expressing high levels of CD14 and decreased levels of CD1a and CD1c. Furthermore, cells generated in presence of IL-10 secreted lower levels of IL-12, but higher levels of IL-8 compared with DC generated in absence of IL-10, both spontaneously and after CD40 engagement. Finally, cells generated in presence of IL-10 were less efficient than DC in stimulating the production of IL-2, interferon-gamma, and IL-4 by allogeneic T cells. We conclude that IL-10 prevents the generation of DC induced by GM-CSF + IL-4 and favors the development of macrophages with a lower T cell stimulatory potential, but secreting higher levels of IL-8 than DC., Journal Article, Research Support, Non-U.S. Gov't, FLWIN, info:eu-repo/semantics/published

Published
1997

68. Bacterial lipopolysaccharide stimulates the production of cytokines and the expression of costimulatory molecules by human peripheral blood dendritic cells: evidence for a soluble CD14-dependent pathway

Author

Verhasselt, Valérie, Buelens, Christel, Willems, Fabienne, De Groote, Donat, Haeffner-Cavaillon, Nicole, Goldman, Michel, Verhasselt, Valérie, Buelens, Christel, Willems, Fabienne, De Groote, Donat, Haeffner-Cavaillon, Nicole, and Goldman, Michel

Abstract

To investigate the responses of dendritic cells (DC) during Gram-negative infections, we analyzed the effects of graded doses of LPS on the cytokine profile, phenotype, and allostimulatory potential of human DC generated by culturing plastic-adherent PBMC in presence of IL-4 and granulocyte-macrophage-CSF. First, we found that LPS stimulates the production of high levels of TNF-alpha, IL-6, IL-8, IL-12 by DC and up-regulates their expression of HLA-DR, B7-1, B7-2, and CD40. The effects of LPS were dose dependent, with a significant stimulatory effect already observed at a concentration of 0.1 ng/ml and a plateau being reached at 10 ng/ml. These phenotypic changes correlated with increased allostimulatory properties of LPS-activated DC because DC treated with LPS were significantly more efficient than untreated DC in eliciting IL-2 and IFN-gamma synthesis by alloreactive T cells and stimulating their proliferation. Experiments using neutralizing anti-IL-12 mAb indicated that LPS-induced IL-12 is responsible for the increased production of IFN-gamma but not for the increased proliferation during MLR. Finally, we observed that the DC responses to low levels of LPS (1 ng/ml) were dramatically inhibited by a blocking anti-CD14 mAb, although DC do not express CD14 molecules on their membrane. Experiments using serum depleted of soluble CD14 (sCD14) and sCD14 either purified from human serum or in recombinant form further established that DC respond to LPS via a soluble CD14-dependent pathway., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published
1997

69. Human dendritic cell responses to lipopolysaccharide and CD40 ligation are differentially regulated by interleukin-10

Author

Buelens, Christel, Verhasselt, Valérie, De Groote, Donat, Thielemans, Kris, Goldman, Michel, Willems, Fabienne, Buelens, Christel, Verhasselt, Valérie, De Groote, Donat, Thielemans, Kris, Goldman, Michel, and Willems, Fabienne

Abstract

We evaluated the effects of interleukin (IL)-10 on the maturation of human dendritic cells (DC) induced either by lipopolysaccharide (LPS) or CD40 engagement. For this purpose, DC generated by culturing plastic-adherent peripheral blood mononuclear cells for 7 days with granulocyte/macrophage-colony-stimulating factor and IL-4 were incubated for 3 days with either LPS (10 ng/ml) or 3T6 fibroblasts transfected with the gene encoding CD40 ligand, in absence or presence of IL-10. First we found that the membrane expression of CD83, a marker of mature DC, was inhibited by IL-10 when induced by LPS but not by CD40 engagement. Likewise, IL-10 inhibited LPS-induced but not CD40-dependent CD86 (B7.2) up-regulation on DC. Furthermore, IL-10 inhibited the production of IL-8 and tumor necrosis factor-alpha by DC when activated by LPS but not by CD40. In contrast, IL-10 inhibited IL-12 production in both activation systems. We conclude that IL-10 differentially influences LPS-dependent and CD40-dependent pathways of DC maturation., In Vitro, Journal Article, Research Support, Non-U.S. Gov't, FLWIN, info:eu-repo/semantics/published

Published
1997

70. Interaction of amiloride with rat parotid muscarinic and alpha-adrenergic receptors.

Author

Dehaye, Jean-Paul, Verhasselt, Valérie, Dehaye, Jean-Paul, and Verhasselt, Valérie

Abstract

1. In rat parotid acini, amiloride inhibited the secretion of amylase and the efflux of calcium and rubidium in response to carbamylcholine and to norepinephrine. 2. Amiloride competitively inhibited the binding of [3H]N-methylscopolamine and [3H] is thus a competitive antagonist of muscarinic and norepinephrine alpha-adrenergic receptors. 3. Amiloride did not affect the response to substance P with respect to secretion or ion movements. 4. Thus the Na+/H+ antiporter is not involved in the short-term regulation of amylase secretion and calcium and potassium movements in rat parotid gland function., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published
1995

71. Cryptococcosis in AIDS

Author

36th International colloquium: Invasive Mycoses in AIDS patients (December 9-8, 1994: Antwerp, Belgium), Verhasselt, Valérie, De Wit, Stéphane, Clumeck, Nathan, 36th International colloquium: Invasive Mycoses in AIDS patients (December 9-8, 1994: Antwerp, Belgium), Verhasselt, Valérie, De Wit, Stéphane, and Clumeck, Nathan

Abstract

info:eu-repo/semantics/nonPublished

Published
1994

76. ChemR23, a putative chemoattractant receptor, is expressed in monocyte-derived dendritic cells and macrophages and is a coreceptor for SIV and some primary HIV-1 strains

Author

Samson, Michel, primary, Edinger, Aimee L., additional, Stordeur, Patrick, additional, Rucker, Joseph, additional, Verhasselt, Valérie, additional, Sharron, Matthew, additional, Govaerts, Cedric, additional, Mollereau, Catherine, additional, Vassart, Gilbert, additional, Doms, Robert W., additional, and Parmentier, Marc, additional

Published
1998
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80. Trypanosoma cruzi down‐regulates lipopolysaccharide‐induced MHC class I on human dendritic cells and impairs antigen presentation to specific CD8+ T lymphocytes.

Author

Overtvelt, Laurence Van, Andrieu, Muriel, Verhasselt, Valérie, Connan, Francine, Choppin, Jeannine, Vercruysse, Vincent, Goldman, Michel, Hosmalin, Anne, and Vray, Bernard

Abstract

Trypanosoma cruzi, the etiological agent of Chagas’ disease, may persist for many years in its mammalian host. This suggests escape from the immune response and particularly a suboptimal CD8+ T cell response, since these cells are involved in infection control. In this report, we show that T. cruzi inhibits the lipopolysaccharide (LPS)‐induced up‐regulation of MHC class I molecules at the surface of human dendritic cells (DC). To further investigate the functional consequences of this inhibition, a trypomastigote surface antigen‐derived peptide (TSA‐1514–522 peptide) was selected for its stable binding to HLA‐A*0201 molecules and used to generate a primary T. cruzi‐specific human CD8+ T cell line in vitro. We observed that DC infected with T. cruzi or treated with T. cruzi‐conditioned medium (TCM) had a weaker capacity to present this peptide to the specific CD8+ T cell line as shown in an IFN‐γ ELISPOT assay. Interestingly, T. cruzi or TCM also reduced the antigen presentation capacity of DC to CD8+ T cell lines specific for the influenza virus M58–66 or HIV RT476–484 epitopes. This dysfunction appears to be linked essentially to reduced MHC class I molecule expression since the stimulation of the RT476–484 peptide‐specific CD8+ T cell line was shown to depend mainly on the MHC class I–TCR interaction and not on the co‐stimulatory signals which, however, were also inhibited by T. cruzi. This impairment of DC function may represent a novel mechanism reducing in vivo the host’s ability to combat efficiently T. cruzi infection. [ABSTRACT FROM PUBLISHER]

Published
2002
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81. Expression of c-FLIPLand resistance to CD95-mediated apoptosis of monocyte-derived dendritic cells: inhibition by bisindolylmaleimide

Author

Willems, Fabienne, Amraoui, Zoulikha, Vanderheyde, Nathalie, Verhasselt, Valérie, Aksoy, Ezra, Scaffidi, Carsten, Peter, Marcus E., Krammer, Peter H., and Goldman, Michel

Abstract

To gain insight into the mechanisms controlling apoptosis of dendritic cells (DC), human monocyte-derived DC were analyzed for their expression of CD95 (Fas/Apo-1) and their response to CD95 ligation. Although DC expressed the CD95 molecule on their membrane, they did not undergo apoptosis on CD95 ligation unless sensitized by cycloheximide. In parallel, DC synthesized c-FLIPL, an inhibitor of the CD95-mediated death-signaling cascade. We also demonstrated that bisindolylmaleimide down-regulates c-FLIPLexpression in DC and, in parallel, allows CD95-mediated apoptosis in these cells. In contrast, Bcl-2, Bcl-xl, and Bax levels were not affected by bisindolylmaleimide. We conclude that DC resist CD95- mediated apoptosis in association with c-FLIPLexpression and that the immunosuppressive potential of bisindolylmaleimide previously observed at the T-cell level also involves facilitation of CD95-mediated DC apoptosis.

Published
2000
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82. Trypanosoma cruziInfects Human Dendritic Cells and Prevents Their Maturation: Inhibition of Cytokines, HLA-DR, And Costimulatory Molecules

Author

Van Overtvelt, Laurence, Vanderheyde, Nathalie, Verhasselt, Valérie, Ismaili, Jamila, De Vos, Louis, Goldman, Michel, Willems, Fabienne, and Vray, Bernard

Abstract

ABSTRACTTrypanosoma cruzi, a parasitic protozoan, is the etiological agent of Chagas’ disease. Despite the many immune system disorders recognized in this infection and the crucial role played by dendritic cells (DC) in acquired immune responses, it was not known whether these cells could be infected by T. cruzitrypomastigotes and the consequences of such an infection on their immune functions. We now provide evidence that human monocyte-derived DC can be infected by T. cruziand can support its intracellular multiplication. Interestingly, this infection has functional consequences on immature DC and on their maturation induced by lipopolysaccharide (LPS). First, after T. cruziinfection, the basal synthesis of interleukin-12 (IL-12) and tumor necrosis factor alpha (TNF-α) was impaired. Furthermore, the process of maturation of DC induced by LPS was drastically affected by T. cruziinfection. Indeed, secretion of cytokines such as IL-12, TNF-α, and IL-6, which are released normally at high levels by LPS-activated DC, as well as the up-regulation of HLA-DR and CD40 molecules, was significantly reduced after this infection. The same effects could be induced by T. cruzi-conditioned medium, indicating that at least these inhibitory effects were mediated by soluble factors released by T. cruzi. Taken together, these results provide new insights into a novel efficient mechanism, directly involving the alteration of DC function, which might be used byT. cruzito escape the host immune responses in Chagas’ disease and thus might favor persistent infection.

Published
1999
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83. EAACI guideline: Preventing the development of food allergy in infants and young children (2020 update).

Author

Halken S, Muraro A, de Silva D, Khaleva E, Angier E, Arasi S, Arshad H, Bahnson HT, Beyer K, Boyle R, du Toit G, Ebisawa M, Eigenmann P, Grimshaw K, Hoest A, Jones C, Lack G, Nadeau K, O'Mahony L, Szajewska H, Venter C, Verhasselt V, Wong GWK, and Roberts G

Subjects
Allergens, Animals, Breast Feeding, Cattle, Child, Child, Preschool, Female, Humans, Infant, Infant Formula, Pregnancy, Food Hypersensitivity prevention & control, Milk Hypersensitivity
Abstract

Background: This guideline from the European Academy of Allergy and Clinical Immunology (EAACI) recommends approaches to prevent the development of immediate-onset / IgE-mediated food allergy in infants and young children. It is an update of a 2014 EAACI guideline., Methods: The guideline was developed using the AGREE II framework and the GRADE approach. An international Task Force with representatives from 11 countries and different disciplinary and clinical backgrounds systematically reviewed research and considered expert opinion. Recommendations were created by weighing up benefits and harms, considering the certainty of evidence and examining values, preferences and resource implications. The guideline was peer-reviewed by external experts, and feedback was incorporated from public consultation., Results: All of the recommendations about preventing food allergy relate to infants (up to 1 year) and young children (up to 5 years), regardless of risk of allergy. There was insufficient evidence about preventing food allergy in other age groups. The EAACI Task Force suggests avoiding the use of regular cow's milk formula as supplementary feed for breastfed infants in the first week of life. The EAACI Task Force suggests introducing well-cooked, but not raw egg or uncooked pasteurized, egg into the infant diet as part of complementary feeding. In populations where there is a high prevalence of peanut allergy, the EAACI Task Force suggests introducing peanuts in an age-appropriate form as part of complementary feeding. According to the studies, it appears that the most effective age to introduce egg and peanut is from four to 6 months of life. The EAACI Task Force suggests against the following for preventing food allergy: (i) avoiding dietary food allergens during pregnancy or breastfeeding; and (ii) using soy protein formula in the first 6 months of life as a means of preventing food allergy. There is no recommendation for or against the following: use of vitamin supplements, fish oil, prebiotics, probiotics or synbiotics in pregnancy, when breastfeeding or in infancy; altering the duration of exclusive breastfeeding; and hydrolysed infant formulas, regular cow's milk-based infant formula after a week of age or use of emollients., Conclusions: Key changes from the 2014 guideline include suggesting (i) the introduction of peanut and well-cooked egg as part of complementary feeding (moderate certainty of evidence) and (ii) avoiding supplementation with regular cow's milk formula in the first week of life (low certainty of evidence). There remains uncertainty in how to prevent food allergy, and further well-powered, multinational research using robust diagnostic criteria is needed., (© 2021 The Authors. Pediatric Allergy and Immunology published by European Academy of Allergy and Clinical Immunology and John Wiley & Sons Ltd.)

Published
2021
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84. Breastfeeding, a Personalized Medicine with Influence on Short- and Long-Term Immune Health.

Author

Verhasselt V

Subjects
Adult, Female, Humans, Infant, Infant, Newborn, Milk, Human, Breast Feeding, Hypersensitivity prevention & control, Precision Medicine
Abstract

The neonatal immune system has its own reactivity, constraints, and challenges, which profoundly differ from the adult. Breast milk is most probably a key requirement both for optimal immune function in early life and for imprinting of the immune system for long-term immune health. Here, we will highlight how breast milk fills the needs and the gaps of the developing immune system and thereby represents the unbeatable way to prevent infectious disease. We will further focus on some factors in breast milk that we extensively studied and found to actively influence the immune trajectory and long-term immune health. More specifically, we will review how the presence of allergens in breast milk together with maternal milk cofactors such as TGF-β, vitamin A, and immunoglobulins influence mucosal immunity in early life with long-term effects on allergic disease susceptibility. We will see that, depending on the content and the nature of allergens in breast milk as well as the presence of immune modulators, very different outcomes are observed, ranging from protection to an increased allergy risk. We are starting to decipher the specific requirements for the neonatal immune system to function optimally. We are discovering how breast milk fulfills these requirements and guides immune trajectories from early life. Answering these questions will provide the infant with preventive and curative approaches that are tailored to this very specific period of life and will ensure long-term immune health., (© 2020 Nestlé Nutrition Institute, Switzerland/S. Karger AG, Basel.)

Published
2020
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85. Early-Life Nutrition and Gut Immune Development.

Author

van den Elsen LWJ, Rekima A, and Verhasselt V

Subjects
Animals, Antigens immunology, Diet, Food, Gastrointestinal Microbiome immunology, Gastrointestinal Microbiome physiology, Humans, Infant, Infant, Newborn, Intestinal Mucosa immunology, Milk, Human, Vitamin A physiology, Gastrointestinal Tract growth & development, Gastrointestinal Tract immunology, Infant Nutritional Physiological Phenomena physiology
Abstract

Gut immune function conditions the development of local and systemic diseases that result from defects in immune regulation, such as inflammatory bowel disease, allergy and obesity. As epidemiological studies support the developmental origin of health and disease, deciphering the critical factors modulating gut immune development should allow the advance of primary prevention strategies specifically adapted to the early-life immune system. Here, we will review gut mucosal immunity development and cover in more detail the recent understanding of the impact of early nutrition on this process. We will emphasize how nutrition can shape microbiota composition and metabolic function and thereby the production of metabolites with immune-modulatory properties. We will also focus on the role of dietary compounds recently demonstrated to be essential in immune development and function, such as dietary antigens, vitamin A, and aryl hydrocarbon receptor ligands. Finally, we will discuss that early-life physiologic food for mammals contains factors capable of compensating for neonatal immune deficiencies, but also factors that are decisive for immune maturation towards a maternal milk-independent and efficient immune system., (© 2019 Nestlé Nutrition Institute, Switzerland/S. Karger AG, Basel.)

Published
2019
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