| Literature DB >> 35720179 |
Abstract
Gestational diabetes mellitus (GDM) is one of the common pregnancy complications, which increases the risk of short-term and long-term adverse consequences in both the mother and offspring. However, the pathophysiological mechanism of GDM is still poorly understood. Inflammation, insulin resistance and oxidative stress are considered critical factors in the occurrence and development of GDM. Although the lifestyle intervention and insulin are the primary treatment, adverse pregnancy outcomes still cannot be ignored. Exosomes have a specific function of carrying biological information, which can transmit information to target cells and play an essential role in intercellular communication. Their possible roles in normal pregnancy and GDM have been widely concerned. The possibility of exosomal cargos as biomarkers of GDM is proposed. This paper reviews the literature in recent years and discusses the role of exosomes in GDM and their possible mechanisms to provide some reference for the prediction, prevention, and treatment of GDM and improve the outcome of pregnancy.Entities:
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Year: 2022 PMID: 35720179 PMCID: PMC9200544 DOI: 10.1155/2022/2169259
Source DB: PubMed Journal: Oxid Med Cell Longev ISSN: 1942-0994 Impact factor: 7.310
The upregulated expression levels of RNAs in GDM and the possible mechanism involved in GDM.
| Sample | Upregulated | Related mechanism | Publication |
|---|---|---|---|
| Serum and urine | miR-429 | IRS-1: a target gene of miR-429 | [ |
| Serum | miR-1323 | Inhibit trophoblast cell viability via inhibiting TP53INP1 | [ |
| Serum | miR-16-5p, miR-29a-3p, and miR-134-5p | — | [ |
| Placenta | miR-222 | Suppress inflammatory response by promoting CXCR4 and inactivating NLRP3 inflammasomes | [ |
| Serum | miR-2467 | Adiponectin: a target gene of miR-2467 | [ |
| Placenta | miR-140-3p | Relate to defective placental IR signaling | [ |
| Blood | miRNA-223 | — | [ |
| Serum | miR-195-5p | Inhibit cell viability and proliferation and promote apoptosis by targeting EZH2 | [ |
| Blood | miR-330-3p | INS-1 cell dysfunction | [ |
| Peripheral blood | miR-770-5p | Influence pancreatic | [ |
| Placental macrophages | miR-657 | Regulate macrophage proliferation, migration and polarization | [ |
| Serum | miRNA-19a and miRNA-19b | — | [ |
| Placenta-derived mononuclear macrophages | miR-657 | Influence inflammatory response via IL-37/NF- | [ |
| Plasma | miR-137 | HG-induced VEC dysfunction | [ |
| Whole blood cells | miRNA-340 | PAIP1: a miRNA-340 target gene | [ |
| Placenta tissue | miR-503 | Regulate pancreatic | [ |
| Plasma | miR-16-5p, miR-17-5p, and miR-20a-5p | Correlate with IR | [ |
| Placenta | miR-98 | Link to the global DNA methylation by targeting Mecp2 | [ |
| HUVECs | circ_0074673 | Regulate the proliferation, migration and angiogenesis of HG-HUVECs via the miR-1200/MEOX2 axis | [ |
| Plasma | circ_0008285 | circ_0008285 may maintain the HTR-8/SVneo trophoblast cell function by the PI3K/Akt signaling pathway | [ |
| Placental tissues | Circ-PNPT1 | Promoted HG-induced trophoblast cell biological dysfunction through miR-889-3p/PAK1 axis | [ |
| Peripheral blood | ERMP1, TSPAN32, MRPL38, and RPL13P5 | RPL13P5 involved in insulin resistance via the PI3K-AKT and insulin signaling pathways | [ |
| Umbilical cord blood exosomes | Lnc-RXYLT1-3 : 2, lnc-TFDP2-7 : 2, lncCOX17-2 : 3, and lnc-ZBTB46-3 : 6 | Most of the exosomal lncRNAs harbored miRNA binding sites | [ |
| Plasma | MEG8 | — | [ |
| Placental tissues | MALAT1 | Associate with inflammation and the proliferation, invasion, and migration of placental trophoblastic cells via modulating the TGF- | [ |
| Blood and placental villous tissues | MEG3 | miR-345-3p: a target; inhibit HTR-8/SVneo cell viability, and prevent cell migration and invasion in addition to inducing cell apoptosis | [ |
| Serum | MALAT1 | — | [ |
| Plasma | SOX2OT | — | [ |
Abbreviations: IRS: insulin receptor substrate; CXCR4: C-X-C chemokine receptor type 4; IR: insulin resistance; EZH2: enhancer of zeste homolog 2; IL: interleukin; NF-κB: nuclear factor κB; HG: high glucose; VEC: vascular endothelial cell; mTOR: mammalian target of rapamycin; Mecp2: methyl CpG binding protein 2; HUVECs: human umbilical vein endothelial cells; PI3K: phosphatidylinositol 3-kinase; Akt: protein kinase B; PAK1: p21 activated kinase 1; TGF-β: tumor growth factor β; MEG3: maternally expressed gene 3.
The downregulated expression levels of RNAs in GDM and the possible mechanism involved in GDM.
| Sample | Downregulated | Related mechanism | Publication |
|---|---|---|---|
| Plasma | miR-574-5p and miR-3135b | Associate with insulin signaling pathway | [ |
| Placenta tissues | miR-362-5p | Promote cell proliferation and inhibited apoptosis via targeting GSR and activating PI3K/Akt pathway | [ |
| Placenta | miR-30d | Affect trophoblast cell functions by targeting RAB8A | [ |
| Placenta and plasma | miR-96-5p | Increased the viability of trophoblasts | [ |
| Placenta-derived macrophages | miR-6869-5p | Prevent from inflammation and inducing M2 macrophages | [ |
| Placenta villous | miR-9 and miR-22 | Alter placental glucose metabolism by targeting GLUT1 and HK2 | [ |
| Blood leukocytes | miR-4646 | — | [ |
| Placental tissue and peripheral blood | miR-345-3p | Inhibit HTR8-/SVneo cell apoptosis and promote cell proliferation and migration by targeting BAK1 | [ |
| Leukocytes | miR-155-5p | — | [ |
| Peripheral blood | miR-193b | Inhibit autophagy and apoptosis by targeting IGFBP5 | [ |
| Serum | miR-29a/b | — | [ |
| Serum and placenta | miR-21 | Inhibit cell growth and infiltration by upregulating PPAR- | [ |
| Placenta | miR-29b | HIF3A: a direct target of miR-29b | [ |
| Serum and placenta | miR-185 | HOMA-IR ↓ | [ |
| Serum and placenta | miR-132 | Enhance the trophoblast cell proliferation | [ |
| Placental of rats | miRNA-221 | Regulate proliferation, apoptosis and insulin secretion in islet | [ |
| Placenta tissues | miR-96 | Regulate PAK1 expression, insulin secretion, and | [ |
| Blood | miR-494 | Improve pancreatic | [ |
| Plasma | hsa_circRNA_102893 | — | [ |
| Plasma | circ_0001173 | — | [ |
| Placenta and plasma | hsa_circ_0005243 | Induce trophoblast cell dysfunction and inflammation by the | [ |
| Placenta | circ_5824, circ_3636, and circ_0395 | — | [ |
| Plasma | SNHG17 | — | [ |
| Umbilical cord blood exosomes | Lnc-TBC1D30-4:1, ENST00000596839.1, lncZNF800-1 : 1, lnc-EIF4ENIF1-1 : 1, and lnc-ATP8B3-3 : 1 | Most of the exosomal lncRNAs harbored miRNA binding sites | [ |
| Placenta | PVT1 | Disrupt the function of trophoblast cells through PI3K/Akt pathway | [ |
| Blood leukocytes | Pax8-AS1 | — | [ |
Abbreviations: GSR: glutathione-disulfide reductase; PI3K: phosphatidylinositol 3-kinase; Akt: protein kinase B; BAK1: BCL2-antagonist/killer 1; IGFBP5: insulin-like growth factor-binding protein 5; HOMA: homeostasis model assessment; IR: insulin resistance; PAK1: p21-activated kinase 1; PTEN: phosphatase and tensin homolog; NF-κB: nuclear factor κB; Pax8-AS1: paired box 8 antisense 1.