Interaction between dendritic cells and natural killer cells during pregnancy in mice.

Sandra M Blois; Gabriela Barrientos; Mariana G Garcia; Arif S Orsal; Mareike Tometten; Rosalia I Cordo-Russo; Burghard F Klapp; Angela Santoni; Nelson Fernández; Peter Terness; Petra Arck

Interaction between dendritic cells and natural killer cells during pregnancy in mice.

Standard

Interaction between dendritic cells and natural killer cells during pregnancy in mice. / Blois, Sandra M; Barrientos, Gabriela; Garcia, Mariana G; Orsal, Arif S; Tometten, Mareike; Cordo-Russo, Rosalia I; Klapp, Burghard F; Santoni, Angela; Fernández, Nelson; Terness, Peter; Arck, Petra.

In: J MOL MED, Vol. 86, No. 7, 7, 2008, p. 837-852.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Blois, SM, Barrientos, G, Garcia, MG, Orsal, AS, Tometten, M, Cordo-Russo, RI, Klapp, BF, Santoni, A, Fernández, N, Terness, P & Arck, P 2008, 'Interaction between dendritic cells and natural killer cells during pregnancy in mice.', J MOL MED, vol. 86, no. 7, 7, pp. 837-852. <http://www.ncbi.nlm.nih.gov/pubmed/18506412?dopt=Citation>

APA

Blois, S. M., Barrientos, G., Garcia, M. G., Orsal, A. S., Tometten, M., Cordo-Russo, R. I., Klapp, B. F., Santoni, A., Fernández, N., Terness, P., & Arck, P. (2008). Interaction between dendritic cells and natural killer cells during pregnancy in mice. J MOL MED, 86(7), 837-852. [7]. http://www.ncbi.nlm.nih.gov/pubmed/18506412?dopt=Citation

Vancouver

Blois SM, Barrientos G, Garcia MG, Orsal AS, Tometten M, Cordo-Russo RI et al. Interaction between dendritic cells and natural killer cells during pregnancy in mice. J MOL MED. 2008;86(7):837-852. 7.

Bibtex

@article{76a7472d03794194bff2796c542fef96,

title = "Interaction between dendritic cells and natural killer cells during pregnancy in mice.",

abstract = "A complex regulation of innate and adaptive immune responses at the maternal fetal interface promotes tolerance of trophoblast cells carrying paternally derived antigens. Such regulatory functions involve uterine dendritic cells (uDC) and natural killer (uNK) cells. The existence of a NK and DC {"}cross talk{"} has been revealed in various experimental settings; its biological significance ranging from cooperative stimulation to cell lysis. Little is known about the presence or role of NK and DC cross talk at the maternal fetal interface. The present study shows that mouse NK and DC interactions are subject to modulation by trophoblast cells in vitro. This interaction promotes a tolerogenic microenvironment characterized by downregulation of the expression of activation markers on uNK cells and uDC and dominance of Th2 cytokines. NK and DC interactions would also influence uterine cell proliferation and this process would be strongly modulated by trophoblast-derived signals. Indeed; while low proliferation rates were observed upon regular coculture allowing direct contact between uterine cells and trophoblasts, incubation in a transwell culture system markedly increased uterine cell proliferation suggesting that soluble factors are key mediators in the molecular {"}dialog{"} between the mother and the conceptus during the establishment of mouse pregnancy. Our data further reveal that the regulatory functions of trophoblast cells associated with tolerance induction are impaired in high abortion murine matings. Interestingly, we observed that secretion of interleukin-12p70 by uDC is dramatically abrogated in the presence of uNK cells. Taken together, our results provide the first evidence that a delicate balance of interactions involving NK cells, DC, and trophoblasts at the mouse maternal fetal interface supports a successful pregnancy outcome.",

author = "Blois, {Sandra M} and Gabriela Barrientos and Garcia, {Mariana G} and Orsal, {Arif S} and Mareike Tometten and Cordo-Russo, {Rosalia I} and Klapp, {Burghard F} and Angela Santoni and Nelson Fern{\'a}ndez and Peter Terness and Petra Arck",

year = "2008",

language = "Deutsch",

volume = "86",

pages = "837--852",

journal = "J MOL MED",

issn = "0946-2716",

publisher = "Springer",

number = "7",

}

RIS

TY - JOUR

T1 - Interaction between dendritic cells and natural killer cells during pregnancy in mice.

AU - Blois, Sandra M

AU - Barrientos, Gabriela

AU - Garcia, Mariana G

AU - Orsal, Arif S

AU - Tometten, Mareike

AU - Cordo-Russo, Rosalia I

AU - Klapp, Burghard F

AU - Santoni, Angela

AU - Fernández, Nelson

AU - Terness, Peter

AU - Arck, Petra

PY - 2008

Y1 - 2008

N2 - A complex regulation of innate and adaptive immune responses at the maternal fetal interface promotes tolerance of trophoblast cells carrying paternally derived antigens. Such regulatory functions involve uterine dendritic cells (uDC) and natural killer (uNK) cells. The existence of a NK and DC "cross talk" has been revealed in various experimental settings; its biological significance ranging from cooperative stimulation to cell lysis. Little is known about the presence or role of NK and DC cross talk at the maternal fetal interface. The present study shows that mouse NK and DC interactions are subject to modulation by trophoblast cells in vitro. This interaction promotes a tolerogenic microenvironment characterized by downregulation of the expression of activation markers on uNK cells and uDC and dominance of Th2 cytokines. NK and DC interactions would also influence uterine cell proliferation and this process would be strongly modulated by trophoblast-derived signals. Indeed; while low proliferation rates were observed upon regular coculture allowing direct contact between uterine cells and trophoblasts, incubation in a transwell culture system markedly increased uterine cell proliferation suggesting that soluble factors are key mediators in the molecular "dialog" between the mother and the conceptus during the establishment of mouse pregnancy. Our data further reveal that the regulatory functions of trophoblast cells associated with tolerance induction are impaired in high abortion murine matings. Interestingly, we observed that secretion of interleukin-12p70 by uDC is dramatically abrogated in the presence of uNK cells. Taken together, our results provide the first evidence that a delicate balance of interactions involving NK cells, DC, and trophoblasts at the mouse maternal fetal interface supports a successful pregnancy outcome.

AB - A complex regulation of innate and adaptive immune responses at the maternal fetal interface promotes tolerance of trophoblast cells carrying paternally derived antigens. Such regulatory functions involve uterine dendritic cells (uDC) and natural killer (uNK) cells. The existence of a NK and DC "cross talk" has been revealed in various experimental settings; its biological significance ranging from cooperative stimulation to cell lysis. Little is known about the presence or role of NK and DC cross talk at the maternal fetal interface. The present study shows that mouse NK and DC interactions are subject to modulation by trophoblast cells in vitro. This interaction promotes a tolerogenic microenvironment characterized by downregulation of the expression of activation markers on uNK cells and uDC and dominance of Th2 cytokines. NK and DC interactions would also influence uterine cell proliferation and this process would be strongly modulated by trophoblast-derived signals. Indeed; while low proliferation rates were observed upon regular coculture allowing direct contact between uterine cells and trophoblasts, incubation in a transwell culture system markedly increased uterine cell proliferation suggesting that soluble factors are key mediators in the molecular "dialog" between the mother and the conceptus during the establishment of mouse pregnancy. Our data further reveal that the regulatory functions of trophoblast cells associated with tolerance induction are impaired in high abortion murine matings. Interestingly, we observed that secretion of interleukin-12p70 by uDC is dramatically abrogated in the presence of uNK cells. Taken together, our results provide the first evidence that a delicate balance of interactions involving NK cells, DC, and trophoblasts at the mouse maternal fetal interface supports a successful pregnancy outcome.

M3 - SCORING: Zeitschriftenaufsatz

VL - 86

SP - 837

EP - 852

JO - J MOL MED

JF - J MOL MED

SN - 0946-2716

IS - 7

M1 - 7

ER -