前列腺癌前病变中MiR-155-5p过表达及巨噬细胞数量增加

Health Science Journal of Indonesia Pub Date : 2020-12-18 DOI:10.22435/hsji.v11i2.3952
Rachmasari Putri, Sari Eka Pratiwi, D. S. Heriyanto, Danarto Danarto, I. Astuti, N. Arfian, S. Haryana
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Ekspresi mRNA SOCS-1 dianalisis menggunakan reverse transcriptase PCR. Penanda pan makrofag, anti CD-68 monoclonal antibody(MoAb) digunakan untuk mendeteksi populasi makrofag pada jaringan dengan imunohistokimia. \nHasil: Ekspresi miR-155 lebih tinggi pada HGPIN dibandingkan BPH dan PRAD (p=0,14). Ekspresi mRNA SOCS1 pada HGPIN paling rendah diantara ketiga sampel (p=0,96). Terdapat korelasi negative antara miR-155 dan mRNA SOCS1 (p=0,02). Terdapat peningkatan persentase populasi makrofag yang signifikan pada HGPIN (6,03 persen) dibandingkan BPH (0.89 persen) dengan p=0,00. \nKesimpulan: Pada penelitian ini, terdapat perubahan persentase makrofag dan miR-155 pada HGPIN. Variasi ekspresi miR-155 dan persentase populasi makrofag dapat disebabkan karena perubahan epigenetik. 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The expression of miR-155 was analyzed using real-time qPCR and calculated using the Livak method. The expression of SOCS1 mRNA was analyzed using reverse transcriptase PCR. The macrophage pan-marker, anti-CD68 monoclonal antibody (MoAb), was used to detect macrophage population in tissues by immunohistochemistry. \nResults: The expression of miR-155 was higher in HGPIN than BPH and PRAD (p=0.14). The expression of SOCS1 mRNA in HGPIN was the lowest among the three samples (p=0.96). There was a negative correlation between miR-155 and SOCS1 mRNA (p=0.02). There was a significant increase in the percentage of the macrophage population in HGPIN (6.03 percent) compared to BPH (0.89 percent) with p=0.00. \nConclusion: In this study, there were changes in the percentage of macrophage and miR-155 in HGPIN. The variation in miR-155 expression and the percentage of the macrophage may be caused by epigenetic changes. 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引用次数: 1

摘要

背景:微小RNA(miR)调节的中断和慢性炎症可以通过细胞和基因组的变化将肿瘤转变为癌症和转移的癌症。癌症前执照有33.3%的机会癌症。本研究旨在研究miR-155-5p对抗信使核糖核酸SOCS1和巨噬细胞群体对抗与良性前列腺增生(BPH)、高级前列腺上皮内增生(HGPIN)和前列腺腺癌(PRAD)相关的疾病进展的作用。方法:本研究分为三组,即BPH、HGPIN和PRAD。从TURP Action获得的网络样本。使用qPCR分析MiR-155的表达,并使用Livak方法计算。使用逆转录酶PCR分析SOCS-1的mRNA表达。巨噬细胞泛标志物,抗CD-68单克隆抗体(MoAb)用于通过免疫组织化学检测网络中的巨噬细胞群体。结果:MiR-155在HGPIN中的表达高于BPH和PRAD(p=0.014)。在三个样本中,HGPIN上的mRNA SOCS1表达最低(p=0.96)。miR-155与信使核糖核酸SOCS1呈负相关(p=0.02)。与BPH(0.89%)相比,HGPIN中巨噬细胞群的百分比显著增加(6.03%),p=0.00。结论:在本研究中,巨噬细胞和miR-155在HGPIN中的百分比发生了变化。miR-155表达和巨噬细胞群百分比的变化可能是由表观遗传学变化引起的。因此,需要进一步的研究来验证这些结果,并了解成为前列腺癌前病变生物标志物的可能性。关键词:前列腺全上皮增生症,miR-155,Macrofage摘要背景:微小RNA(miR)调节受损和慢性炎症可通过细胞和基因组变化转移,将肿瘤转化为癌症和癌症。癌前病变癌变的几率为33.3%。本研究探讨了与SOCS1 mRNA和巨噬细胞群相关的miR-155在良性前列腺增生(BPH)、高级别前列腺上皮内增生(HGPIN)和前列腺腺癌(PRAD)相关疾病进展中的作用。方法:这是一项横断面研究,使用了三组样本,即BPH、HGPIN和PRAD。组织样本取自TURP Action。使用实时qPCR分析miR-155的表达,并使用Livak方法计算。利用逆转录聚合酶链式反应分析SOCS1 mRNA的表达。巨噬细胞泛标志物,抗CD68单克隆抗体(MoAb),用于通过免疫组织化学检测组织中的巨噬细胞群体。结果:miR-155在HGPIN中的表达高于BPH和PRAD(p=0.14)。SOCS1 mRNA在三个样本中的表达最低(p=0.96)。miR-155与SOCS1 mRNA之间呈负相关(p=0.02)。与BPH(0.89%)(p=0.00)相比,HGPIN中巨噬细胞群的百分比显著增加(6.03%)。结论:在本研究中,巨噬细胞和miR-155在HGPIN中的百分比发生了变化。miR-155表达和巨噬细胞百分比的变化可能是由表观遗传学变化引起的。因此,需要进一步的研究来验证这些结果,并了解其作为前列腺癌前疾病生物标志物的可能性。关键词:前列腺上皮内肿瘤,miR-155,巨噬细胞
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Overexpression of MiR-155-5p and increased number of macrophage population in precancerous prostatic disease
Latar Belakang: Gangguan regulasi mikroRNA(miR) dan inflamasi kronik dapat mengubah tumor menjadi karsinoma dan kanker dengan metastasis melalui perubahan seluler dan genomik. Lesi prekanker memiliki peluang 33,3 persen menjadi kanker. Penelitian ini bertujuan untuk mengkaji peran miR-155-5p terhadap mRNA SOCS1 dan populasi makrofag terhadap progresivitas penyakit yang berhubungan dengan Benign Prostate Hyperplasia (BPH), High Grade Prostatic Intraepithelial Neoplasia (HGPIN), dan Prostate Adenocarcinoma (PRAD). Metode: Penelitian ini merupakan penelitian potong lintang dengan 3 kelompok, yaitu BPH,HGPIN, dan PRAD. Sampel jaringan didapatkan dari Tindakan TURP. Ekspresi miR-155 dianalisis menggunakan qPCR dan dikalkulasi menggunakan metode Livak. Ekspresi mRNA SOCS-1 dianalisis menggunakan reverse transcriptase PCR. Penanda pan makrofag, anti CD-68 monoclonal antibody(MoAb) digunakan untuk mendeteksi populasi makrofag pada jaringan dengan imunohistokimia. Hasil: Ekspresi miR-155 lebih tinggi pada HGPIN dibandingkan BPH dan PRAD (p=0,14). Ekspresi mRNA SOCS1 pada HGPIN paling rendah diantara ketiga sampel (p=0,96). Terdapat korelasi negative antara miR-155 dan mRNA SOCS1 (p=0,02). Terdapat peningkatan persentase populasi makrofag yang signifikan pada HGPIN (6,03 persen) dibandingkan BPH (0.89 persen) dengan p=0,00. Kesimpulan: Pada penelitian ini, terdapat perubahan persentase makrofag dan miR-155 pada HGPIN. Variasi ekspresi miR-155 dan persentase populasi makrofag dapat disebabkan karena perubahan epigenetik. Oleh sebab itu, perlu penelitian lebih lanjut untuk memvalidasi hasil tersebut dan memahami  kemungkinan menjadi biomarker pada penyakit prekanker pada prostat. Kata Kunci: Prostatic Intaepithelial Neoplasia, miR-155, Makrofag   Abstract   Background: Impaired microRNA(miR) regulation and chronic inflammation could transform tumors into carcinoma and cancer by metastasis through cellular and genomic changes. Precancerous lesions have a 33.3 percent chance of becoming cancerous. This study investigated the role of miR-155 related to SOCS1 mRNA and macrophage population in disease progression associated  with Benign Prostate Hyperplasia (BPH), High-Grade Prostatic Intraepithelial Neoplasia (HGPIN), and Prostate Adenocarcinoma (PRAD). Methods: This was a cross-sectional study using three groups of samples, namely BPH, HGPIN, and PRAD. Tissue samples were obtained from TURP Action. The expression of miR-155 was analyzed using real-time qPCR and calculated using the Livak method. The expression of SOCS1 mRNA was analyzed using reverse transcriptase PCR. The macrophage pan-marker, anti-CD68 monoclonal antibody (MoAb), was used to detect macrophage population in tissues by immunohistochemistry. Results: The expression of miR-155 was higher in HGPIN than BPH and PRAD (p=0.14). The expression of SOCS1 mRNA in HGPIN was the lowest among the three samples (p=0.96). There was a negative correlation between miR-155 and SOCS1 mRNA (p=0.02). There was a significant increase in the percentage of the macrophage population in HGPIN (6.03 percent) compared to BPH (0.89 percent) with p=0.00. Conclusion: In this study, there were changes in the percentage of macrophage and miR-155 in HGPIN. The variation in miR-155 expression and the percentage of the macrophage may be caused by epigenetic changes. Therefore, further research is needed to validate these results and understand the possibility of being a biomarker in precancerous disease of the prostate. Keywords: Prostatic Intraepithelial Neoplasia, miR-155, Macrophage
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来源期刊
Health Science Journal of Indonesia
Health Science Journal of Indonesia
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