<scp>IL1β‐NFκβ‐Myocardin</scp> signaling axis governs trophoblast‐directed plasticity of vascular smooth muscle cells

Das, Priyanka; Bose, Rumela; Paul, Madhurima; Nandy, Debdyuti; Basak, Trishita; Ain, Rupasri

doi:10.1096/fj.202302403r

The FASEB Journal

2024

DOI: 10.1096/fj.202302403r

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IL1β‐NFκβ‐Myocardin signaling axis governs trophoblast‐directed plasticity of vascular smooth muscle cells

Priyanka Das,

Rumela Bose,

Madhurima Paul

et al.

Abstract: Vascular smooth muscle cell (VSMC) plasticity is fundamental in uterine spiral artery remodeling during placentation in Eutherian mammals. Our previous work showed that the invasion of trophoblast cells into uterine myometrium coincides with a phenotypic change of VSMCs. Here, we elucidate the mechanism by which trophoblast cells confer VSMC plasticity. Analysis of genetic markers on E13.5, E16.5, and E19.5 in the rat metrial gland, the entry point of uterine arteries, revealed that trophoblast invasion is ass… Show more

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Apoptotic Receptors and CD107a Expression by NK Cells in an Interaction Model with Trophoblast Cells

Mikhailova,

Sokolov,

Grebenkina

et al. 2024

CIMB

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Natural killer cells (NK cells) exert cytotoxicity towards target cells in several ways, including the expression of apoptosis-mediating ligands (TRAIL, FasL). In addition, NK cells themselves may be susceptible to apoptosis due to the expression of TRAIL receptors. These receptors include TRAIL-R1 (DR4), TRAIL-R2 (DR5), capable of inducing apoptosis, and TRAIL-R3 (DcR1), TRAIL-R4 (DcR2), the so-called “decoy receptors”, which lack an intracellular domain initiating activation of caspases. Of particular interest is the interaction of uterine NK cells with cells of fetal origin, trophoblasts, which are potential targets for natural killer cells to carry out cytotoxicity. The aim of this work was to evaluate the expression of proapoptotic receptors and their ligands as well as CD107a expression by NK cells in a model of interaction with trophoblast cells. To evaluate NK cells, we used cells of the NK-92 line; cells of the JEG-3 line were used as target cells. The cytokines IL-1β, IL-15, IL-18, TNFα, IL-10, TGFβ and conditioned media (CM) of the first and third trimester chorionic villi explants were used as inducers. We established that cytokines changed the expression of apoptosic receptors by NK cells: in the presence of TNFα, the amount and intensity of Fas expression increased, while in the presence of TGFβ, the amount and intensity of expression of the DR5 receptor decreased. Soluble chorionic villi factors alter the expression of TRAIL and FasL by NK-92 cells, which can reflect the suppression of the TRAIL-dependent mechanism of apoptosis in the first trimester and stimulating the Fas-dependent mechanism in the third trimester. In the presence of trophoblast cells, the expression of TRAIL and DcR1 by NK cells was reduced compared to intact cells, indicating an inhibitory effect of trophoblast cells on NK cell cytotoxicity. In the presence of chorionic villi CM and trophoblast cells, a reduced number of NK-92 cells expressing DR4 and DR5 was found. Therefore, soluble factors secreted by chorionic villi cells regulate the resistance of NK cells to death by binding TRAIL, likely maintaining their activity at a certain level in case of contact with trophoblast cells.

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Apoptotic Receptors and CD107a Expression by NK Cells in an Interaction Model with Trophoblast Cells

Mikhailova,

Sokolov,

Grebenkina

et al. 2024

CIMB

View full text Add to dashboard Cite

show abstract

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IL1β‐NFκβ‐Myocardin signaling axis governs trophoblast‐directed plasticity of vascular smooth muscle cells

Cited by 1 publication

References 28 publications

Apoptotic Receptors and CD107a Expression by NK Cells in an Interaction Model with Trophoblast Cells

Apoptotic Receptors and CD107a Expression by NK Cells in an Interaction Model with Trophoblast Cells

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