Three types of HLA-G+ extravillous trophoblasts that have distinct immune regulatory properties

Papúchová, Henrieta; Kshirsagar, Sarika; Xu, Lily; Gomes, Hannah Ananda Bougleux; Li, Qin; Iyer, Vidya; Norwitz, Errol R.; Strominger, Jack L.; Tilburgs, Tamara

doi:10.1073/pnas.2000484117

Cited by 44 publications

(32 citation statements)

References 49 publications

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“…HLA-G is also involved in the generation of a tumor tolerogenic microenvironment through regulatory cells: its expression is correlated with accumulation of MDSC, 61 increased CD4 + CD25 + FoxP3 + population 62 and secretion of IL-10 and TGF-β that are responsible for the TME maintenance. 17 Furthermore, HLA-G is expressed by tolerogenic immune cells such as CD4 + FoxP3 - HLA-G + Treg, 63 suppressive NK cells, 30 DC-10 cells, 64 infiltrating monocytes 65 and tumor-associated macrophages (TAM), 66 67 all involved in the TME. We did not formally demonstrate in the present manuscript that anti-HLA-G CAR-T cells were capable of killing real ex vivo tolerogenic HLA-G-expressing cells such as DC-10 cells.…”

Section: Discussionmentioning

confidence: 99%

First immunotherapeutic CAR-T cells against the immune checkpoint protein HLA-G

Anna

Bôle‐Richard

LeMaoult

et al. 2021

J Immunother Cancer

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BackgroundCAR-T cells immunotherapy is a breakthrough in the treatment of hematological malignancies such as acute lymphoblastic leukemia (ALL) and B-cell malignancies. However, CAR-T therapies face major hurdles such as the lack of tumor-specific antigen (TSA), and immunosuppressive tumor microenvironment sometimes caused by the tumorous expression of immune checkpoints (ICPs) such as HLA-G. Indeed, HLA-G is remarkable because it is both a potent ICP and a TSA. HLA-G tumor expression causes immune escape by impairing innate and adaptive immune responses and by inducing a suppressive microenvironment. Yet, to date, no immunotherapy targets it.MethodsWe have developed two anti-HLA-G third-generation CARs based on new anti-HLA-G monoclonal antibodies.ResultsAnti-HLA-G CAR-T cells were specific for immunosuppressive HLA-G isoforms. HLA-G-activated CAR-T cells polarized toward T helper 1, and became cytotoxic against HLA-G+ tumor cells. In vivo, anti-HLA-G CAR-T cells were able to control and eliminate HLA-G+ tumor cells. The interaction of tumor-HLA-G with interleukin (IL)T2-expressing T cells is known to result in effector T cell functional inhibition, but anti-HLA-G CAR-T cells were insensitive to this inhibition and still exerted their function even when expressing ILT2. Lastly, we show that anti-HLA-G CAR-T cells differentiated into long-term memory effector cells, and seemed not to lose function even after repeated stimulation by HLA-G-expressing tumor cells.ConclusionWe report for the first time that HLA-G, which is both a TSA and an ICP, constitutes a valid target for CAR-T cell therapy to specifically target and eliminate both tumor cells and HLA-G+ suppressive cells.

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Section: Discussionmentioning

confidence: 99%

First immunotherapeutic CAR-T cells against the immune checkpoint protein HLA-G

Anna

Bôle‐Richard

LeMaoult

et al. 2021

J Immunother Cancer

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“…This proportion has been shown to rise up to 70% at the end of pregnancy (77). At the same time, HLA-G expression has been observed to be higher in term pregnancy EVT cells than in firsttrimester EVTs (91). Decidual T cells have been reported to express the HLA-G receptor ILT2.…”

Section: Hla-g Participates In the Formation Of Maternal-fetal Immunementioning

confidence: 98%

Roles of HLA-G in the Maternal-Fetal Immune Microenvironment

2020

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During pregnancy, the maternal uterus and fetus form a special microenvironment at the maternal-fetal interface to support fetal development. Extravillous trophoblasts (EVTs), differentiated from the fetus, invade into the decidua and interact with maternal cells. Human leukocyte antigen (HLA)-G is a non-classical MHC-I molecule that is expressed abundantly and specifically on EVTs in physiological conditions. Soluble HLA-G (sHLA-G) is also found in maternal blood, amniotic fluid, and cord blood. The abnormal expression and polymorphisms of HLA-G are related to adverse pregnancy outcomes such as preeclampsia (PE) and recurrent spontaneous abortion (RSA). Here we summarize current findings about three main roles of HLA-G during pregnancy, namely its promotion of spiral artery remodeling, immune tolerance, and fetal growth, all resulting from its interaction with immune cells. These findings are not only of great significance for the treatment of pregnancy-related diseases but also provide clues to tumor immunology research since HLA-G functions as a checkpoint in tumors.

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“…In aged mouse and humans, the resolution of endometriosis is delayed [34]. Chronic inflammation in endometrial tissue decreases the telomerase activity of several cells, impeding their optimal physiological response in mouse [34] and humans [21,[35][36][37][38][39]. trNK cells could also be affected by the low telomerase response [34].…”

Section: Nk Cells and Endometrial Diseasementioning

confidence: 99%

“…trNK cells could also be affected by the low telomerase response [34]. On the other hand, senescent cells may activate the cytotoxic response of cNK cells [34][35][36][37][38][39] against autologous cells and, in consequence, generate more cell death maintaining the local chronic inflammatory response.…”

Section: Nk Cells and Endometrial Diseasementioning

confidence: 99%

“…In humans, NK cells, macrophages, and T cells are responsible for maintaining the local inflammatory response [35][36][37][38][39][40]. The role of TH17 and IFN γ has been widely discussed; however, the control of inflammation in the tissue is not achieved in many patients despite surgery or other therapeutic options raising the question of a wider variety of endometrial diseases [21,[36][37][38][39]. One of the often-overlooked events is autoantibodies, which can play an essential role in maintaining the inflammatory response [40][41][42].…”

Section: Nk Cells and Endometrial Diseasementioning

confidence: 99%

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A Brief Analysis of Tissue-Resident NK Cells in Pregnancy and Endometrial Diseases: The Importance of Pharmacologic Modulation

Garmendia

Sanctis

2021

Immuno

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NK cells are lymphocytes involved in the innate and adaptative immune response. These cells are located in peripheral blood and tissues with ample functions, from immune vigilant to tolerogenic reactions. In the endometrium, NK cell populations vary depending on age, hormones, and inflammation. When pregnancy occurs, tissue-resident NK cells and conventional NK cells are recruited to protect the fetus, a tolerogenic response. On the contrary, in the inflamed endometrium, various inflammatory cells down-regulate NK tolerance and impair embryo implantation. Therefore, NK cells’ pharmacological modulation is difficult to achieve. Several strategies have been used, from progesterone, lipid emulsions to steroids; the success has not been as expected. However, new therapeutic approaches have been proposed to decrease the endometrial inflammatory burden and increase pregnancy success based on understanding NK cell physiology.

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Three types of HLA-G+ extravillous trophoblasts that have distinct immune regulatory properties

Cited by 44 publications

References 49 publications

First immunotherapeutic CAR-T cells against the immune checkpoint protein HLA-G

First immunotherapeutic CAR-T cells against the immune checkpoint protein HLA-G

Roles of HLA-G in the Maternal-Fetal Immune Microenvironment

A Brief Analysis of Tissue-Resident NK Cells in Pregnancy and Endometrial Diseases: The Importance of Pharmacologic Modulation

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