Complex Evaluation of Tissue Factors in Pediatric Cholesteatoma

Dambergs, Kristaps; Sumeraga, Gunta; Pilmane, Māra

doi:10.3390/children8100926

Cited by 5 publications

(10 citation statements)

References 51 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Furthermore, a significant correlation was found between TLR4 and activated NF-κB [ 37 ] in MEC tissue, and we assume, that the same could be shown for RAGE as well. Further, another study demonstrated a correlation between NF-kB and biomarkers of angiogenesis and osteolysis in MEC tissue isolated from patients [ 84 ]. In addition to this, the DNA-binding protein inhibitor Id1, known to be induced by chronic TLR4 signalling [ 85 ], was proven to be abundantly expressed in MEC epithelium [ 86 ] where it accelerates proliferation and survival of keratinocytes in vitro via NF-κB signalling [ 87 ].…”

Section: Applicable Targets In Precision Medicine For Mec Therapymentioning

confidence: 99%

“…The most prominent is the vascular endothelial growth factor (VEGF), for which expression is upregulated in compared to normal skin [ 241 , 282 ]. A correlation between NF-κB driven inflammation and VEGF was shown to promote the neovascularisation in MEC tissue [ 84 ]. VEGF signalling can be inhibited by approved drugs on the level of intracellular signalling by drugs like sunitinib [ 288 ] or axitinib [ 289 ], which are approved for treatment of renal cell carcinoma or nintedanib applied against pulmonary fibrosis [ 290 ] or lucitanib used in clinical trials against cancer [ 291 ].…”

Section: Applicable Targets In Precision Medicine For Mec Therapymentioning

confidence: 99%

“…These MMPs are well known to be crucial for the decomposition of the extracellular matrix making the tissue susceptible for vascular outgrowth. An immunofluorescence correlation study in cholesteatoma tissue demonstrated, that correlations between NF-κB and these MMPs causes the intensification of angiogenesis in MEC [ 84 ] and can be targeted by drugs described in the previous subchapter.…”

Section: Applicable Targets In Precision Medicine For Mec Therapymentioning

confidence: 99%

See 2 more Smart Citations

Review of potential medical treatments for middle ear cholesteatoma

2022

View full text Add to dashboard Cite

Middle ear cholesteatoma (MEC), is a destructive, and locally invasive lesion in the middle ear driven by inflammation with an annual incidence of 10 per 100,000. Surgical extraction/excision remains the only treatment strategy available and recurrence is high (up to 40%), therefore developing the first pharmaceutical treatments for MEC is desperately required. This review was targeted at connecting the dysregulated inflammatory network of MEC to pathogenesis and identification of pharmaceutical targets. We summarized the numerous basic research endeavors undertaken over the last 30+ years to identify the key targets in the dysregulated inflammatory pathways and judged the level of evidence for a given target if it was generated by in vitro, in vivo or clinical experiments. MEC pathogenesis was found to be connected to cytokines characteristic for Th1, Th17 and M1 cells. In addition, we found that the inflammation created damage associated molecular patterns (DAMPs), which further promoted inflammation. Similar positive feedback loops have already been described for other Th1/Th17 driven inflammatory diseases (arthritis, Crohn’s disease or multiple sclerosis). A wide-ranging search for molecular targeted therapies (MTT) led to the discovery of over a hundred clinically approved drugs already applied in precision medicine. Based on exclusion criteria designed to enable fast translation as well as efficacy, we condensed the numerous MTTs down to 13 top drugs. The review should serve as groundwork for the primary goal, which is to provide potential pharmaceutical therapies to MEC patients for the first time in history.

show abstract

Section: Applicable Targets In Precision Medicine For Mec Therapymentioning

confidence: 99%

Section: Applicable Targets In Precision Medicine For Mec Therapymentioning

confidence: 99%

Section: Applicable Targets In Precision Medicine For Mec Therapymentioning

confidence: 99%

See 1 more Smart Citation

Review of potential medical treatments for middle ear cholesteatoma

2022

View full text Add to dashboard Cite

show abstract

“…However, additional information on how HβD-2 acts in cholesteatoma tissue is needed. There are limited data about the importance of HβD-4 in cholesteatoma, but our previous study showed that HβD-2 is more heavily expressed in pediatric cholesteatoma tissue than HβD-4 [ 26 ].…”

Section: Introductionmentioning

confidence: 99%

“…Chiang et al proved that the loss of Shh causes external- and middle -ear pathologies [ 28 ]. However, the exact role of Shh in cholesteatoma tissue is not yet clear, although our previous study showed the upregulation of Shh in cholesteatoma compared to skin tissue [ 26 ].…”

Section: Introductionmentioning

confidence: 99%

Morphopathogenesis of Adult Acquired Cholesteatoma

2023

Self Cite

View full text Add to dashboard Cite

Background and Objectives. The aim of this study was to compare the distribution of proliferation markers (Ki-67, NF-κβ), tissue-remodeling factors (MMP-2, MMP-9, TIMP-2, TIMP-4), vascular endothelial growth factor (VEGF), interleukins (IL-1 and IL-10), human beta defensins (HβD-2 and HβD-4) and Sonic hedgehog gene protein in cholesteatoma and control skin. Methods. Nineteen patient cholesteatoma tissues and seven control skin materials from cadavers were included in the study and stained immunohistochemically. Results. Statistically discernible differences were found between the following: the Ki-67 in the matrix and the Ki-67 in the skin epithelium (p = 0.000); the Ki-67 in the perimatrix and the Ki-67 in the connective tissue (p = 0.010); the NF-κβ in the cholesteatoma matrix and the NF-κβ in the epithelium (p = 0.001); the MMP-9 in the matrix and the MMP-9 in the epithelium (p = 0.008); the HβD-2 in the perimatrix and the HβD-2 in the connective tissue (p = 0.004); and the Shh in the cholesteatoma’s perimatrix and the Shh in the skin’s connective tissue (p = 0.000). Conclusion. The elevation of Ki-67 and NF-κβ suggests the induction of cellular proliferation in the cholesteatoma. Intercorrelations between VEGF, NF-κβ and TIMP-2 induce neo-angiogenesis in adult cholesteatoma. The similarity in the expression of IL-1 and IL-10 suggests the dysregulation of the local immune status in cholesteatoma. The overexpression of the Sonic hedgehog gene protein in the cholesteatoma proves the selective local stimulation of perimatrix development.

show abstract

N6-methyladenosine methylation analysis of circRNAs in acquired middle ear cholesteatoma

He,

Mahmoudi,

Yao

et al. 2024

Front. Genet.

View full text Add to dashboard Cite

IntroductionMiddle ear cholesteatoma is a chronic middle ear disease characterized by severe hearing loss and adjacent bone erosion, resulting in numerous complications. This study sought to identify pathways involved in N6-methyladenosine (m6A) modification of circRNA in middle ear cholesteatoma.MethodsA m6A circRNA epitranscriptomic microarray analysis was performed in middle ear cholesteatoma tissues (n = 5) and normal post-auricular skin samples (n = 5). Bioinformatics analyses subsequently explored the biological functions (Gene Ontology, GO) and signaling pathways (Kyoto Encyclopedia of Genes and Genomes, KEGG) underlying middle ear cholesteatoma pathogenesis. Methylated RNA immunoprecipitation qPCR (MeRIP-qPCR) was performed to verify the presence of circRNAs with m6A modifications in middle ear cholesteatoma and normal skin samples.ResultsMicroarray analysis identified 3,755 circRNAs as significantly differentially modified by m6A methylation in middle ear cholesteatoma compared with the normal post-auricular skin. Among these, 3,742 were hypermethylated (FC ≥ 2, FDR < 0.05) and 13 were hypomethylated (FC ≤ 1/2, FDR < 0.05). GO analysis terms with the highest enrichment score were localization, cytoplasm, and ATP-dependent activity for biological processes, cellular components, and molecular functions respectively. Of the eight hypermethylated circRNA pathways, RNA degradation pathway has the highest enrichment score. Peroxisome Proliferator-Activated Receptor (PPAR) signaling pathway was hypomethylated. To validate the microarray analysis, we conducted MeRIP-qPCR to assess the methylation levels of five specific m6A-modified circRNAs: hsa_circRNA_061554, hsa_circRNA_001454, hsa_circRNA_031526, hsa_circRNA_100833, and hsa_circRNA_022382. The validation was highly consistent with the findings from the microarray analysis.ConclusionOur study firstly presents m6A modification patterns of circRNAs in middle ear cholesteatoma. This finding suggests a direction for circRNA m6A modification research in the etiology of cholesteatoma and provides potential therapeutic targets for the treatment of middle ear cholesteatoma.

show abstract

Complex Evaluation of Tissue Factors in Pediatric Cholesteatoma

Cited by 5 publications

References 51 publications

Review of potential medical treatments for middle ear cholesteatoma

Review of potential medical treatments for middle ear cholesteatoma

Morphopathogenesis of Adult Acquired Cholesteatoma

N6-methyladenosine methylation analysis of circRNAs in acquired middle ear cholesteatoma

Contact Info

Product

Resources

About