Jana Dupor
University of Milan
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Publication
Featured researches published by Jana Dupor.
Proceedings of the National Academy of Sciences of the United States of America | 2007
Yeny Martinez de la Torre; Chiara Buracchi; Elena Monica Borroni; Jana Dupor; Raffaella Bonecchi; Manuela Nebuloni; Fabio Pasqualini; Andrea Doni; Eleonora Lauri; Chiara Agostinis; Roberta Bulla; Donald N. Cook; Bodduluri Haribabu; Pier Luigi Meroni; Daniel Rukavina; Luca Vago; Francesco Tedesco; Annunciata Vecchi; Sergio A. Lira; Massimo Locati; Alberto Mantovani
Fetal loss in animals and humans is frequently associated with inflammatory conditions. D6 is a promiscuous chemokine receptor with decoy function, expressed in lymphatic endothelium, that recognizes and targets to degradation most inflammatory CC chemokines. Here, we report that D6 is expressed in placenta on invading extravillous trophoblasts and on the apical side of syncytiotrophoblast cells, at the very interface between maternal blood and fetus. Exposure of D6−/− pregnant mice to LPS or antiphospholipid autoantibodies results in higher levels of inflammatory CC chemokines and increased leukocyte infiltrate in placenta, causing an increased rate of fetal loss, which is prevented by blocking inflammatory chemokines. Thus, the promiscuous decoy receptor for inflammatory CC chemokines D6 plays a nonredundant role in the protection against fetal loss caused by systemic inflammation and antiphospholipid antibodies.
European Journal of Immunology | 2005
Yeny Martinez de la Torre; Massimo Locati; Chiara Buracchi; Jana Dupor; Donald N. Cook; Raffaella Bonecchi; Manuela Nebuloni; Daniel Rukavina; Luca Vago; Annunciata Vecchi; Sergio A. Lira; Alberto Mantovani
Chemokines are chemotactic cytokines with a key role in the control of cell trafficking and positioning under homeostatic and inflammatory conditions. D6 is a promiscuous 7‐transmembrane‐domain receptor expressed on lymphatic vessels which recognizes most inflammatory, but not homeostatic, CC chemokines. In vitro experiments demonstrated that D6 is unable to signal after ligand engagement, and it is structurally adapted to sustain rapid and efficient ligand internalization and degradation. These unique functional properties lead to the hypothesis that D6 may be involved in the control of inflammation by acting as a decoy and scavenger receptor for inflammatory chemokines. Consistent with this hypothesis, here we report that D6–/– mice showed an anticipated and exacerbated inflammatory response in a model of skin inflammation. Moreover, the absence of D6 resulted in increase cellularity and inflammatory‐chemokine levels in draining lymph nodes. Thus, D6 is a decoy receptor structurally adapted and strategically located to tune tissue inflammation and control transfer of inflammatory chemokines to draining lymph nodes.
American Journal of Reproductive Immunology | 2005
Tatjana Bogović Crnčić; Gordana Laškarin; Koraljka Juretić; Natasa Strbo; Jana Dupor; Suzana Sršen; Ljiljana Randić; Philippe Le Bouteiller; Julie Tabiasco; Daniel Rukavina
The immunogenetic enigma of maternal acceptance of the fetal semiallograft has been termed an immunological paradox. The first trimester decidua is heavily infiltrated with CD56brightCD16− uterine natural killer (uNK) cells which must be prepared to respond to potential pathogen challenges and still be able to control immune responses that allow the development of the fetus. The significant presence of cytolytic mediators, perforin and Fas/Fas ligand (FasL), at the maternal–fetal interface raises a question of their role(s) in the immunological interrelations between maternal tissues and trophoblast cells. As uNK cells in vitro lyse target cell lines (K562, P815 and P815Fas) using these effector molecules, it seems that, although immunocompetent, their cytotoxicity is not directed against trophoblast during normal pregnancy. Therefore, it is generally believed that the hormonal and Th1/Th2 cytokine balance plays an important role in the tolerance and maintenance of pregnancy. This paper gives an overview of the recent findings on the complex immunological events that occur at the maternal–fetal interface.
Clinical and Experimental Rheumatology | 2007
Ym de la Torre; Chiara Buracchi; Em Borroni; Jana Dupor; Raffaella Bonecchi; Manuela Nebuloni; Fabio Pasqualini; Andrea Doni; Eleonora Lauri; Chiara Agostinis; Roberta Bulla; Dn Cook; Bodduluri Haribabu; P. L. Meroni; Daniel Rukavina; Luca Vago; Francesco Saverio Tedesco; Annunciata Vecchi; Sa Lira; Massimo Locati; A. . . Less Mantovani
Abstract book Molecular Mechanisms of Implantation, Second EMBIC Summer School | 2006
Gordana Laškarin; Natasa Strbo; Koraljka Juretic Frankovic; Jana Dupor; Danijela Veljković; Herman Haller; Tea Štimac; Paola Allavena; Aleberto Mantovani; Daniel Rukavina
ECRI | 2004
Tatjana Bogović Crnčić; Natasa Strbo; Gordana Laškarin; Kristijan Ćupurdija; Dorotea Dorčić; Koraljka Juretić; Jana Dupor; Vlatka Sotošek Tokmadžić; Ivica Vlastelić; Ljiljana Randić; Daniel Rukavina
Am. J. Reprod Immunol.51(6):465, O6, 2004. (CC) | 2016
Natasa Strbo; Kristijan Ćupurdija; Koraljka Juretić; Jana Dupor; Dorotea Dorčić; Tatjana Bogović Crnčić; Gordana Laškarin; Ljiljana Randić; Echard R Podack; Daniel Rukavina
Second EMBIC Summer School "Molecular Mechanisms of Implantation" : Abstract book | 2006
Koraljka Juretic Frankovic; Gordana Laškarin; Jana Dupor; Natasa Strbo; Tatjana Bogović Crnčić; Ivica Bedenicki; Suzana Sršen Medančić; Danijela Veljković; Ljiljana Randić; Julie Tabiasco; Philippe Le Bouteiller; Daniel Rukavina
Archive | 2006
Koraljka Juretic Frankovic; Gordana Laškarin; Natasa Strbo; Tatjana Bogović Crnčić; Jana Dupor; Dorotea Dorčić; Suzana Sršen Medančić; Danijela Veljković; Ljiljana Randić; Julie Tabiasco; Le Bouteiller; Philippe; Daniel Rukavina
European Congress of Reproductive Immunology (4 ; 2006) | 2006
Gordana Laškarin; Suzana Sršen Medančić; Jana Dupor; Danijela Veljković; Koraljka Juretic Frankovic; Ljiljana Randić; Tea Štimac; Alberto Mantovani; Paola Allavena; Daniel Rukavina