תמונות העטיפה

MicroRNA and Cancer

MicroRNAs (miRs) are small noncoding RNAs that function as post-transcriptional regulators of gene expression and have important roles in almost all biological pathways. Deregulated miR expression has been detected in numerous cancers, where miRs act as both oncogene and tumor suppressors. Due to th...

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פורמט: Online
שפה:אנגלית
יצא לאור: MDPI - Multidisciplinary Digital Publishing Institute 2022
נושאים:
Breast cancer
Hypoxia inducible factor 1-alpha (HIF-1α)
MicroRNA (miRNA)
miR526b
miR655
Oxidative stress
Migration
Cyclooxygenase-2 (COX-2)
Prostaglandin E2 receptor 4 (EP4)
PI3K/Akt
adipokines
endometrial cancer
estrogens
hyperinsulinemia
insulin
insulin resistance
insulin signaling
insulin-like growth factors
microRNA
miRNA
ovarian cancer
survival
prognostic factor
serum LDH
blood biomarker
circulating microRNA
plasma
immunotherapy
immune checkpoint inhibitors
metastatic melanoma
hepatocellular carcinoma
metastasis
exosome
bioinformatics analysis
renal cancer
RCC
ccRCC
meta-analysis
miRNAs
normal B-cell development
B-CLL
miRNA-transcription factor network
regulation
biomarker
therapy
prognosis
diagnosis
progression
prediction
smoking
non-small cell lung cancer
methylation
miR-584-5p
YKT6
snoRNA
2′-O-methylation
pseudouridylation
malignant melanoma
cancer stem cell
stemness
head and neck squamous cell carcinoma
colon cancer
cancer stem cells
microRNAs
deformability
PARP
replication stress
targeted therapy
breast cancer
circulating biomarkers
medulloblastoma
brain tumour
subgroups
stem cells
n/a
thema EDItEUR::G Reference, Information and Interdisciplinary subjects::GP Research and information: general
thema EDItEUR::P Mathematics and Science::PS Biology, life sciences
גישה מקוונת:ONIX_20220706_9783036544168_28
תגים: הוספת תג
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סיכום:MicroRNAs (miRs) are small noncoding RNAs that function as post-transcriptional regulators of gene expression and have important roles in almost all biological pathways. Deregulated miR expression has been detected in numerous cancers, where miRs act as both oncogene and tumor suppressors. Due to their important roles in tumorigenesis, miRs have been investigated as prognostic and diagnostic biomarkers and as useful targets for therapeutic intervention. From a therapeutic point of view, two modalities can serve to rectify gene networks in cancer cells. For oncomiRs, a rational means is downregulation through antagomirs. Moreover, observations of the pathological reductions in tumor-suppressive miRs have inspired the concept of “miR replacement therapy” to enhance the amount of these miRs, thereby restoring them to normal levels. However, the clinical applicability of miR-based therapies is severely limited by the lack of effective delivery systems. Therefore, to understand the role of this new class of regulators, we need to identify the mRNA targets regulated by individual miRs as well as to develop specific, efficient, and safe delivery systems for therapeutic miRs.

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