Osteosarcoma is the most common type of bone cancer in children and adolescents. MicroRNAs (miRNAs) play important roles in the development, differentiation, and function of different cell types and in the pathogenesis of various human diseases. miRNAs are differentially expressed in normal and cancer cells. The investigation of miRNA expression between healthy subjects and patients with osteosarcoma is crucial for future clinical trials. In this study, the expression levels of miRNAs were detected by qRT-PCR. Correlation between expression levels of tow miRNAs and different clinicopathological characteristics were analyzed using the Ï�2 test. Survival rate was detected using the log-rank test and Kaplanâ��Meier method. qRT-PCR was shown that expression levels of miR-29b and miR-422a were strongly decreased in osteosarcoma bone tissue compared with noncancerous bone tissues. Our result indicated that the low expression levels of miR-29b and miR-422a showed strong correlation with large tumor size (P = 0.20; 0.029), advanced TNM stage (P = 0.001; 0.012), distant metastasis (P = 0.008; 0.019), and grade of tumor (P = 0.009; 0.016). Kaplanâ��Meier survival analysis showed that the low expressions of miR-29b/miR-422a were correlated with shorter time overall survival (log-rank test, P = 0.009; P = 0.013). Moreover, multivariate Cox proportional hazards model indicated that miR-29b and miR-422a (P = 0.024; P = 0.016) were independent prognostic markers of overall survival of patients. Our result indicated that downregulation of miR-29b and miR-422a may be linked to the prediction of poor prognosis, indicating that miR-29b and miR-422a may be a valuable prognostic marker for osteosarcoma patients. Â© 2015, International Society of Oncology and BioMarkers (ISOBM)

Bahador, R.

Goudarzi, P.K.

Mirghasemi, A.

Shakeri, M.

Taheriazam, A.

Torkaman, A.

Yahaghi, E.

eprints Iran University of Medical Sciences

ORIGINAL ARTICLETissue expression levels of miR-29b and miR-422a in children,adolescents, and young adults’ age groupsand their association with prediction of poor prognosisin human osteosarcomaReza Bahador1 & Afshin Taheriazam2 & Alireza Mirghasemi3 & Ali Torkaman4 &Mohammadreza Shakeri1 & Emad Yahaghi5 & Peyman Karimi Goudarzi6Received: 8 August 2015 /Accepted: 25 August 2015 /Published online: 1 October 2015# International Society of Oncology and BioMarkers (ISOBM) 2015Abstract Osteosarcoma is the most common type of bonecancer in children and adolescents. MicroRNAs (miRNAs)play important roles in the development, differentiation, andfunction of different cell types and in the pathogenesis ofvarious human diseases. miRNAs are differentially expressedin normal and cancer cells. The investigation of miRNA ex-pression between healthy subjects and patients with osteosar-coma is crucial for future clinical trials. In this study, the ex-pression levels of miRNAs were detected by qRT-PCR.Correlation between expression levels of tow miRNAs anddifferent clinicopathological characteristics were analyzedusing the χ2 test. Survival rate was detected using the log-rank test and Kaplan–Meier method. qRT-PCR was shownthat expression levels of miR-29b and miR-422a were strong-ly decreased in osteosarcoma bone tissue compared with non-cancerous bone tissues. Our result indicated that the lowexpression levels of miR-29b and miR-422a showed strongcorrelation with large tumor size (P=0.20; 0.029), advancedTNM stage (P=0.001; 0.012), distant metastasis (P=0.008;0.019), and grade of tumor (P=0.009; 0.016). Kaplan–Meiersurvival analysis showed that the low expressions ofmiR-29b/miR-422a were correlated with shorter time overall survival(log-rank test, P=0.009; P=0.013). Moreover, multivariateCox proportional hazards model indicated that miR-29b andmiR-422a (P=0.024; P=0.016) were independent prognosticmarkers of overall survival of patients. Our result indicatedthat downregulation of miR-29b and miR-422a may be linkedto the prediction of poor prognosis, indicating that miR-29band miR-422a may be a valuable prognostic marker for oste-osarcoma patients.Keywords miR-29b andmiR-422a . Survival . PCR .Osteosarcoma . PathologyIntroductionOsteosarcoma (OS) is a destructive primary bone tumor inchildren and adolescents that is a tumor with high metastaticpotential [1, 2]. Despite advances of therapeutic strategiessuch as surgery and chemotherapy, long time survival rate ofpatients suffering from advanced osteosarcoma remains verylow to date [3, 4]. Therefore, it is required to identify bio-markers, molecular mechanisms, and therapeutic targets forosteosarcoma. MicroRNAs (miRNAs) are small, non-codingRNAmolecules that are significant markers for prognosis anddiagnosis of cancer and promising targets for treatment.miRNAs have important roles in a number of biological func-tions such as embryogenesis, cell fate specification, cellularproliferation, differentiation, and apoptosis through alteration* Peyman Karimi GoudarziPedram_kg@yahoo.com1 Department of Orthopaedic and Trauma Surgery, Birjand Universityof Medical Sciences, Birjand, Iran2 Department of Orthopedics Surgery, Tehran Medical SciencesBranch, Islamic Azad University, Tehran, Iran3 Department of Orthopedics, Qom University of Medical Sciences,Qom, Iran4 Department of Orthopedics, Firoozgar Hospital, Iran University ofMedical Sciences, Tehran, Iran5 Department of Molecular Biology, Baqiyatallah University ofMedical Sciences, Tehran, Iran6 Department of Neurosurgery, AJA University of Medical Sciences,Tehran, IranTumor Biol. (2016) 37:3091–3095DOI 10.1007/s13277-015-4140-5RETRACTED ARTICLEof the targets expression by both downregulation and up-regulation [5, 6]. Dysregulation of different microRNAshas been reported in various human cancers [6, 7]. It isclear that they can function either as tumor-suppressor oroncogene in different human malignancies depending ontheir target mRNAs [8, 9]. Nevertheless, the roles ofmiRNAs in biology of cancer are still required to be stud-ied. Downregulation of miR-29b has been suggested inmany kinds of cancer, and most of the mentioned studiesfocused on the mechanism by which miR-29b acts asinhibitor of tumorigenesis [10, 11, 12]. A recent studyindicated that miR-422a was downregulated in OS tissues,and it could be a valuable diagnostic and predictive mark-er [13]. However, the roles of miR-29b and miR-422a inosteosarcoma and their relationship with clinicopatholog-ical factors need further investigation. We aimed the ex-pression pattern of miR-29b and miR-422a in osteosarco-ma tissues and their relationship with clinicopathologicalfactors.Materials and methodsPatients and clinical specimensWe recruited 51 patients with osteosarcoma from different hos-pitals in Tehran, Iran, between April 2009 and December 2014.In addition, adjacent normal bone tissues were also collected.Patients underwent surgery without chemotherapy or ra-diotherapy before surgery. Clinical data was obtained fromthe database of the patients. The tissues were obtained fromsurgical specimens reviewed by pathologist. All the speci-mens were stored at −80 °C until use. This study was con-firmed by the research ethics committee, and the clinicopath-ological features were categorized in Table 1.Quantitative reverse transcriptase PCRWe used quantitative real-time PCR to assess the expressionlevel of miR-29b and miR-422a in osteosarcoma patients andTable 1 The relationship of miR-29b and miR-422a expression with clinicopathological factors of osteosarcomaClinicopathological features No. of cases (51) Expression of miR-29b expression of miR-422a P value of miR-29b P value of miR-422aLow=31 High=20 Low=29 High=22GenderMale 30 18 12 19 11 0.672 0.618Female 21 13 8 10 11AgeChildren, adolescents 20 13 7 15 5 0.528 0.412Young adults 31 18 13 14 17Tumor diameter (cm)≤5 33 14 19 18 15 0.020 0.029>5 18 17 1 11 7LocationDistal 24 13 11 10 14 0.412 0.406Proximal 27 18 9 17 10Tumor gradeLow 22 11 11 10 12 0.009 0.016High 29 20 9 19 10Histological typeOsteoblastic 23 14 9 13 10 0.454 0.483Chondroblastic 14 8 6 8 6Telangiectatic 10 6 4 5 5Fibroblastic 4 3 1 3 1TNM stageI+II 34 15 19 14 20 0.001 0.012III+IV 17 16 1 15 2Distant metastasisYes 18 13 5 13 5 0.008 0.019No 33 18 15 16 173092 Tumor Biol. (2016) 37:3091–3095RETRACTED ARTILEnormal tissues. In brief, total RNAwas extracted from tissuesusing TRIzol reagent (Invitrogen, Carlsbad, CA). The expres-sion levels of miRNAs were quantitated using the TaqManmiRNA assay kit (Applied Biosystems). Real-time PCR wasperformed using Rotor Gene 6000 Real-Time PCR (Qiagen,Germany) with an Invitrogen kit and a TaqMan universal PCRmaster mix was also applied. U6 snRNA was utilized as anendogenous control. Fold change expression of miRNAs werecalculated using ΔΔ-CT method (ΔΔCt=ΔCttumorsamples–ΔCtcontrol sample).Statistical analysisAll data presented as mean±SD. SPSS 18.0 software(SPSS Inc., USA) were used to analyze all variables.Differences between groups were evaluated usingStudent’s t test. Moreover, the relationship betweenmiRNA expression and various clinicopathological fac-tors was analyzed using the χ2 test. Survival time wasfollowed up to the date of death, and survival rate wasdetermined using the log-rank test and Kaplan–Meiermethod. Prognostic values of clinicopathological factorswere evaluated using Cox proportional hazards model.P<0.05 was statistically significant.ResultsDownregulation of miRNAsThe expression levels of miR-29b and miR-422a in patientswere compared with those of adjacent normal bone tissues.qRT-PCR has shown that expression levels of miR-29b andmiR-422a were strongly decreased in osteosarcoma bone tis-sue (mean±SD, 3.17±1.39; 1.74±0.57) compared with non-cancerous bone tissues (mean±SD, 9.67±2.55; 6.16±1.03;P=0.001; P=0.006; Fig. 1).Association with clinicopathologic featuresThe patients were divided into low- and high-expressiongroups according to the median expression level.Donregulation of miR-29b and miR-422a expression levelsshowed strong correlation with large tumor size (P=0.20;0.029), advanced TNM stage (P=0.001; 0.012), distant me-tastasis (P=0.008; 0.019), and grade of tumor (P=0.009;0.016).No significant correlation was found between miR-29b/miR-422a expression levels and age groups (P=0.528;0.412), gender (P=0.672; 0.618), location (P=0.412; 0.406),and histological type (P=0.454; 0.483; Table 1).Association of miRNA expression with prognosisin patientsThe low expressions of miR-29b/miR-422a were correlatedwith shorter time overall survival (log-rank test, P=0.009;P=0.013; Figs. 2 and 3) based on Kaplan–Meier survivalanalysis. According to the multivariate Cox proportional haz-ards model, miR-29b and miR-422a (P=0.024; P=0.016)were independent prognostic markers for overall survival ofpatients (Tables 2 and 3)DiscussionTo date, there are no available biomarkers routinely utilized thathave diagnostic and predictive values. Therefore, more specificprognostic biomarkers are required for advancing the therapeuticstrategies for osteosarcoma patients. qRT-PCR has shown thatexpression levels of miR-29b and miR-422a were strongly de-creased in osteosarcoma bone tissue compared with noncancer-ous bone tissues. Moreover, decreased expression of miR-29bandmiR-422a was strongly linked to large tumor size, advancedFig. 2 Correlation between miR-29b expression and survival time inpatientsFig. 1 The relative expression of miRNAs in osteosarcoma tissues andtheir corresponding normal samplesTumor Biol. (2016) 37:3091–3095 3093RETRACTED ARTICLETNM stage distant metastasis, and grade of tumor. These resultindicated that low expression of miRNAs may be correlatedwith progression of osteosarcoma. Dysregulation of differentmicroRNAs has been suggested in osteosarcoma tissues [7, 14,15, 16]. Previous studies have reported that miR-29b was down-regulated in many kinds of cancer [11, 12, 17, 18]. MiR-29bdirectly regulatesVEGF as tumor-suppressive gene, a chaperoneinvolved in the tumorigenesis in osteosarcoma tissues. It hasreported that restoration of miR-29b inhibited cell proliferation,migration, and invasion in cancer. Cheng et al. suggested thatmiR-29b has oncogenic potential and targets the TET2 gene,which acts as tumor-suppressor frequently mutated in hemato-poietic malignancies [18]. It has been reported that miR-29bfunctions as a regulator in many kinds of cancers, through itstargeting. It acts as a tumor-suppressor and inhibits cell prolifer-ation, differentiation, metastasis, and chemosensitivity [19]. Onthe other hand, Gougelet et al. suggested that miR-422a wasdownregulated in OS tissues, and it could be a valuable diag-nostic and predictive marker [13]. There have been some studieswhich indicated that miR-422a play an important role in humandiseases. Previous studies indicated that decreased expression ofmiR-422amay play a protective role in colorectal tumor and canact as inhibitor of pathways that stimulate tumor cell prolifera-tion in osteosarcoma [19, 20]. In the current study, the lowexpressions of miR-29b/miR-422a were correlated with shortertime overall survival based on Kaplan–Meier survival analysis.Multivariate Cox proportional hazards model showed that miR-29b and miR-422a were independently correlated with overallsurvival of patients, suggesting that these miRNAs could be asindependent prognostic factor of overall survival in patient suf-fering from osteosarcoma.In conclusion, our result indicated that downregulation ofmiR-29b and miR-422a may be linked to the prediction ofpoor prognosis, indicating that miR-29b and miR-422a maybe a valuable prognostic marker for osteosarcoma patients.Acknowledgments We wish to thank Dr. Javanbakht for attentive En-glish language editing of our manuscript.Conflicts of interest NoneReferences1. Ottaviani G, Jaffe N. The epidemiology of osteosarcoma. CancerTreat Res. 2009;152:3–13.2. Broadhead ML, Clark JC, Myers DE, Dass CR, Choong PF. Themolecular pathogenesis of osteosarcoma: a review. Sarcoma.2011;2011:959248.3. Leary SE, Wozniak AW, Billups CA, Wu J, McPherson V, NeelMD. Survival of pediatric patients after relapsed osteosarcoma: theSt. Jude Children’s Research Hospital experience. Cancer.2013;119(14):2645–53.4. Kager L, Zoubek A, Kastner U, Kempf-Bielack B, Potratz J, KotzR. Skip metastases in osteosarcoma: experience of the CooperativeOsteosarcoma Study Group. J Clin Oncol. 2006;24(10):1535–41.5. Henry JC, Park JK, Jiang J, Kim JH, Nagorney DM, Roberts LR,et al. miR-199a-3p targets CD44 and reduces proliferation of CD44positive hepatocellular carcinoma cell lines. Biochem Biophys ResCommun. 2010;403:120–5.6. Baumhoer D, Zillmer S, Unger K, Rosemann M, Atkinson MJ,Irmler M. MicroRNA profiling with correlation to gene expressionrevealed the oncogenic miR-17-92 cluster to be up-regulated inosteosarcoma. Cancer Genet. 2012;205(5):212–9.Table 3 Multivariate analysis of miR-422a expression for prognosticfactorsClinicopathological characteristics HR 95 % CI P valueGender 0.925 1.275–2.128 0.673Age 1.143 1.056–2.478 0.567Tumor grade 3.015 2. 352–9.215 0.005Location 0.874 0.738–2.843 0.512Distant metastasis 3.601 2.632–14.129 0.002TNM stage 3.972 2.991–14.103 0.001Histological type 2.127 1.425–3.120 0.401miR-422a 2.918 1.731–9.698 0.016Table 2 Multivariate analysis of miR-29b expression for prognosticfactorsClinicopathological characteristics HR 95 % CI P valueGender 1.217 0.683–1.839 0.741Age 1.374 0.593–3.373 0.431Tumor grade 3.194 2. 235–11.216 0.009Location 0.792 0.734–3.021 0.583Distant metastasis 3.945 2.383–13.326 0.003TNM stage 3.642 2.684–12.127 0.004Histological type 2.439 1.321–3.484 0.453miR-29b expression 2.778 1.453–8.793 0.024Fig. 3 Correlation between miR-422a expression and survival time inpatients3094 Tumor Biol. (2016) 37:3091–3095RETRACTED ARTICLE7. Jin J, Cai L, Liu ZM, Zhou XS. miRNA-218 Inhibits osteosarcomacell migration and invasion by down-regulating of TIAM1, MMP2and MMP9. Asian Pac J Cancer Prev. 2013;14(6):3681–4.8. Jones KB, Salah Z, Del Mare S, Galasso M, Gaudio E, Nuovo GJ.miRNA signatures associate with pathogenesis and progression ofosteosarcoma. Cancer Res. 2012;72(7):1865–77.9. Sun Y, Fang R, Li C, Li L, Li F, Ye X. Hsa-mir-182 suppresseslung tumorigenesis through down regulation of RGS17 expres-sion in vitro. Biochem Biophys Res Commun. 2010;396(2):501–7.10. Kwiecinski M, Elfimova N, Noetel A, Tox U, Steffen HM, HackerU, et al. Expression of platelet-derived growth factor-c and insulin-like growth factor i in hepatic stellate cells is inhibited by miR-29.Lab Invest. 2012;92:978–87.11. Dai N, Zhong ZY, CunYP, QingY, Chen C, Jiang P, et al. Alterationof the microRNA expression profile in human osteosarcoma cellstransfected with APE1 siRNA. Neoplasma. 2013;60:384–94.12. Hong Q, Fang J, Pang Y. Prognostic value of the microRNA-29family in patients with primary osteosarcomas. Med Oncol.2014;31:37.13. Gougelet A, Pissaloux D, Besse A, Perez J, Duc A. Micro-RNAprofiles in osteosarcoma as a predictive tool for ifosfamide re-sponse. Int J Cancer. 2011;129:680–90.14. Wu XJ, Li Y, Liu D, Zhao LD, Bai B, Xue MH. MiR-27a as anoncogenic microRNA of hepatitis B virus-related hepatocellularcarcinoma. Asian Pac J Cancer Prev. 2013;14:885–9.15. Zhao G, Cai C, Yang T. MicroRNA-221 induces cell survival andcisplatin resistance through PI3K/Akt pathway in human osteosar-coma. PLoS One. 2013;8(1):e53906.16. Huang J, Gao K, Lin J. MicroRNA-100 inhibits osteosarcoma cellproliferation by targeting Cyr61. Tumor Biol. 2014;35(2):1095–100.17. Sandhu R, Rivenbark AG,Mackler RM, Livasy CA, ColemanWB.Dysregulation of microRNA expression drives aberrant DNAhypermethylation in basal-like breast cancer. Int J Oncol.2014;44:563–72.18. Cheng J, Guo S, Chen S. An extensive network of TET2-targetingmicroRNAs regulates malignant hematopoiesis. Cell Rep.2013;5(2):471–81.19. Faltejskova P, Svoboda M, Srutova K, Mlcochova J, Besse A.Identification and functional screening of microRNAs highlyderegulated in colorectal cancer. J Cell Mol Med. 2012;16:2655–66.20. Yan B, Guo Q, Fa-jun F, Wang Z, Yin Z, Wei Y-b, et al. The role ofmiR-29b in cancer: regulation, function, and signaling. OncoTargets Ther. 2015;8:539–48.Tumor Biol. (2016) 37:3091–3095 3095RETRACTED ARTICLE

Tissue expression levels of miR-29b and miR-422a in children, adolescents, and young adultsâ�� age groups and their association with prediction of poor prognosis in human osteosarcoma

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Tissue expression levels of miR-29b and miR-422a in children, adolescents, and young adultsâ�� age groups and their association with prediction of poor prognosis in human osteosarcoma

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