Current concepts in ameloblastoma-targeted therapies in B-raf proto-oncogene serine/threonine kinase V600E mutation: Systematic review

BACKGROUND Ameloblastomas are common benign epithelial odontogenic neoplasms that present an aggressive and unpredictable behavior that may modify treatment strategies.Different signaling pathways that participate in the progression of these tumors have been identified.B-raf proto-oncogene serine/threonine kinase(BRAF)is a protein involved in the behavior of ameloblastomas,and it is related to many cell mechanisms.BRAF gene mutations have been identified in ameloblastomas,of which the BRAF V600E(valine substituted by glutamic acid at amino acid 600)mutation has been the most common and can be present concomitantly with other mutations that may be involved in its behavior.Targeted therapies have been used as an alternative in the case of resistance or contraindications to conventional treatments.AIM To document the presence of BRAF V600E and additional mutations,their behavior,and targeted therapies in these tumors.METHODS An electronic literature search was conducted according to PRISMA guidelines in PubMed/MEDLINE,Cochrane,EMBASE,and SpringerLink using the terms“ameloblastomas”,“BRAF V600E”,“additional mutations”,and“targeted therapies”.Ameloblastomas were classified according to WHO guidelines.Inclusion criteria were articles in English,published not more than 10 years ago,and studies with laboratory works related to BRAF V600E.Articles were evaluated by two independent reviewers and retrieved for full-text evaluation.The EBLIP Critical Appraisal Checklist was used to evaluate the quality of the eligible studies.Descriptive statistical analysis was performed.RESULTS Two independent reviewers,with a substantial concordance indicated by a kappa coefficient of k=0.76,evaluated a total of 19 articles that were included in this study.The analysis registered 521 conventional ameloblastomas(AM),81 unicystic ameloblastomas(UA),13 ameloblastic carcinomas(AC),three metastatic ameloblastomas(MA),and six peripheral ameloblastomas(PA),of which the histopathological type,anatomic location,laboratory tests,expression of BRAF mutation,and additional mutations were registered.The BRAF V600E mutation was found in 297 AM(57%),63 UA(77.7%),3 AC(23%),1 MA(50%),and 5 PA(83.3%).Follicular type predominated with a total of 116 cases(40%),followed by plexiform type with 63 cases(22.1%).Furthermore,both types presented additional mutations,in which alterations in JAK3 P132T,SMARCB1,PIK3CA,CTNNB1,SMO,and BRAF G606E genes were found.Four case reports were found with targeted therapy to BRAF V600E.CONCLUSION The identification of BRAF V600E and additional mutations as an aid in targeted therapies has been a breakthrough in alternative treatments of ameloblastomas where surgical treatments are contraindicated.

Effects of Cadmium on Hepatocellular DNA Damage,Proto-Oncogene Expression and Apoptosis in Rats

Objective To study the effects of cadmium on hepatocellular DNA damage, expression of proto-oncogenes c-myc, c-fos, and c-jun as well as apoptosis in rats. Methods Cadmium chloride at the doses of 5, 10, and 20 μmol/kg was given to rats by i.p. and there were 5 male SD rats in each group. Hepatocellular DNA damage was measured by single cell gel electrophoresis （or comet assay）, while expression of proto-oncogenes c-myc, c-fos, and c-jun in rat hepatocytes were measured by Northern dot hybridization. C-Myc, c-Fos, and c-Jun were detected with immuno-histochemical method. Hepatocellular apoptosis was determined by TUNEL （TdT-mediated dUTP Nick End Labelling） and flow cytometry. Results At the doses of 5, 10, and 20 μmol/kg, cadmium chloride induced DNA damage in rat hepatocytes and the rates of comet cells were 50.20%, 88.40%, and 93.80%, respectively. Results also showed an obvious dose-response relationship between the rates of comet cells and the dose of cadmium chloride （r=0.9172, P〈0.01）. Cadmium chloride at the doses of 5, 10, and 20 μmol/kg induced expression of proto-oncogenes c-myc, c-fos, and c-jun. The positive brown-yellow signal for c-myc, c-fos, and c-jun was mainly located in the cytoplasm of hepatocytes with immunohistochemical method. TUNEL-positive cells were detected in cadmium-treated rat livers. Apoptotic rates （%） of cadmium-treated liver cells at the doses of 5, 10, and 20 μmol/kg were （17.24 ±2.98）, （20.58± 1.35）, and （24.06±1.77） respectively, being significantly higher than those in the control. The results also displayed an obvious dose-response relationship between apoptotic rates and the dose of cadmium chloride （r=0.8619, P〈0.05）. Conclusion Cadmium at 5-20 μmol/kg can induce hepatocellular DNA damage, expression of proto-oncogenes c-myc, c-fos, and c-jun as well as apoptosis in rats.

干扰B-Raf基因对绵羊毛囊干细胞增殖和凋亡的影响

本研究旨在探讨编码丝氨酸/苏氨酸蛋白激酶(Serine/Threonine-Protein Kinase)的B-Raf基因对绵羊毛囊干细胞(HFSCs)增殖和凋亡的影响。将si-B-Raf转染至HFSCs,通过RT-qPCR实验技术检测B-Raf基因、Erk1/2基因和STAT3基因的表达水平,通过Western Blot实验技术检测B-Raf蛋白、Erk1/2蛋白、p-Erk1/2蛋白和STAT3蛋白的表达水平,通过EdU细胞增殖法和CCK-8细胞增殖检测法检测HFSCs的增殖情况,通过流式细胞仪检测HFSCs的凋亡情况。结果表明,si-B-Raf转染细胞后,B-Raf基因的表达量显著降低,Erk1/2基因和STAT3基因的表达量也显著降低;Western Blot实验结果表明,B-Raf蛋白、Erk1/2蛋白、p-Erk1/2蛋白和STAT3蛋白的表达水平显著降低;EdU和CCK-8结果发现细胞增殖受到抑制,细胞增殖水平显著下降;流式细胞仪检测到细胞凋亡水平显著上升。综上,干扰B-Raf基因表达显著抑制HFSCs增殖并促进其凋亡,可能是通过MAPK/Erk1/2通路进行的,研究可为进一步阐明绵羊毛囊发育机制提供科学参考。

Expressions of estrogen receptor subtypes and c-met proto-oncogene in endometrial carcinoma and their correlation

Objective To investigate the expressions of estrogen receptor(ER)subtypes and c-met proto-oncogene in human endometrial carcinomas and to assess the clinical significance of ER and c-met in this carcinoma.Methods Reverse transcription PCR(RT-PCR)was used to detect the expressions of ERα,ERβ and c-met proto-oncogene mRNA in 30 samples of endometrial carcinoma and 11 samples of normal endometrium.Results The expression of ERα in endometrial carcinoma(0.70±0.40)was significantly reduced in comparison to that in normal endometrium(1.14±0.56,P<0.05).A similar finding was made for the expression of ERβ in carcinoma(0.24±0.18)versus normal tissues(0.48±0.20,P<0.05).In contrast,c-met mRNA expression was increased in endometrial carcinoma(1.45±0.72)compared to that in normal endometrium(0.42±0.31,P<0.01).A decrease tendency of the expression of ERα was also found from Stage Ⅰ(0.82±0.41)to a more severe Stag Ⅱ-Ⅲ of endometrial carcinoma(0.42±0.17,P<0.05).The analysis of ERα and ERβ mRNA revealed a decrease tendency from shallow to deep invasion of the uterine muscles(P<0.05).We found that the expressions of ERα and ERβ were negatively correlated with c-met proto-oncogene with a coefficient correlation of-0.63(P<0.01)and-0.32(P<0.05),respectively.Conclusion ERα and ERβ are both involved in mutagenic action of carcinogen.C-met proto-oncogene plays an important role in the carcinogenesis and development of endometrial carcinoma.C-met and ER expressions show a negative correlation in the development of endometrial carcinoma.

1889例结直肠癌MSI、K-ras、N-ras和B-raf基因状态以及临床病理特征分析

目的通过对1889例结直肠癌微卫星不稳定(MSI)、K-ras、N-ras和B-raf基因检测,分析其基因状态与临床病理特征之间的关联性。方法收集东部战区总医院病理科结直肠癌患者手术切除大标本共计1889例,通过PCR荧光法联合毛细管电泳法对1889例结直肠癌进行MSI、K-ras、N-ras和B-raf检测,分析其基因状态与临床病理特征之间的关系,以及MSI与K-ras、N-ras和B-raf之间的关联性分析,并且对MSI自身位点的相关性分析。结果1889例结直肠癌患者中,微卫星高度不稳定(MSI-H)更易发生于右侧结肠(16.4%)、黏液腺癌(14.9%)、分化程度较低(18.7%)、年龄偏低(8.3%)、淋巴结未转移(9.1%)以及B-raf突变(5.2%)的患者中,K-ras突变更易发生于右侧结肠(50.7%)、黏液腺癌(50.7%)、分化程度较高(52.1%)、微卫星低度不稳定或稳定型(42.2%)的患者中,而B-raf突变更易发生在MSI-H(6.9%)的患者中,而N-ras基因则与临床病特征关联性不强。结论结直肠癌患者的MSI、K-ras和B-raf基因状态与临床病理特征存在着高度的关联性,因此通过分析其基因状态与临床病理特征之间的关系可以为临床靶向治疗以及预后提供更加可靠的依据。

THE PRELIMINARY APPLICATION OF IN SITU HYBRIDI-ZATION IN DETECTING PROTO-ONCOGENES EXPRESSION IN HUMAN LEUKEMIC CELLS

An in situ hybridization technique with 35S labelled proto-oncogene probes (c-myc & c-fes) was used to detect their expression in bone marrow cells of 22 cases of leukemia of various types and immature granulocytes and erythroblasts of 16 nomal myelograms as controls. Both c-myc and c-fes were detectable in leukemic cells as well as in immature granulocytes and erythroblasts of normal bone marrow, but the expression extent varied in different cases. The levels of c-myc expression in leukemic cells were higher than those in controls (P<0.001). There was no difference of c-fes expression in two groups of bone marrow cells (P>0.05). This technique provides us a new method in studying variations of proto-oncogene expression in leukemic cells.

Malignant pheochromocytoma in neurofibromatosis; mutation screening of RET proto-oncogene, VHL and SDH gene

AIM: To investigate pathogenic mutations related to malignant pheochromocytoma in neurofibromatosis(NF).METHODS: We present a patient with NF and metastatic pheochromocytoma in whom genetic screening for presence of pathogenic mutations in RET protooncogene, von Hippel-Lindau(VHL) and succinate dehydrogenase complex subunits B(SDHB) genes were investigated. RET proto-oncogene mutation screening for exons 10, 11, 13, 14, 15, 16 were examined by polymerase chain reaction(PCR) and direct DNA sequencing in patient. Mutation screening for exons 1, 2, 3 of VHL gene was carried out. Both forward and reverse strandswere subjected to direct sequencing after PCR amplification. The entire coding sequence of SDHB gene was screened for the presence of pathogenic mutations by PCR-sequencing.RESULTS: A 45-year-old man presented with abdominal pain and hypertension over the previous year. The patient was a known case of neurofibromatosis type 1(NF1) who presented at the age of 15 years with hyperpigmented and hypopigmented lesions. After complete evaluation for hypertension, biochemical tests and imagings indicated a malignant pheochromocytoma of 120 mm × 70 mm in size. The patient underwent left adrenalectomy, nephrectomy and splenectomy. After surgery the symptoms improved and blood pressure was controlled. After 5 years he was admitted again for evaluation of hypertensive crisis. Biochemical tests were again consistent with pheochromocytoma and disease relapse. Imaging studies and liver biopsy confirmed metastatic pheochromocytoma to the liver and para-aortic area. 131 Iodine-metaiodobenzylguanidine therapy was carried out. Genetic screening of VHL(exons 1, 2, 3), RET proto-oncogene(exons 10, 11, 13, 14, 15, 16) and SDH complex subunits revealed no pathogenic mutation. CONCLUSION: We conclude that mutations in the NF1 gene are responsible for the patient's clinical findings. However, would be helpful to further examine somatic mutations for a more precise study of genotypephenotype correlation.

Effect of cisplatin-based concurrent radiochemotherapy on malignant degree of advanced cervical cancer and expression of proto-oncogene and tumor suppressor genes

Objective:To study the effect of cisplatin-based concurrent radiochemotherapy on the malignant degree of advanced cervical cancer and the expression of proto-oncogene and tumor suppressor genes.Methods: A total of 82 patients with advanced cervical cancer who were treated in our hospital between July 2013 and December 2016 were collected and divided into control group and observation group according to random number table, with 41 cases in each group. The control group of patients received radiotherapy alone, while the observation group of patients received cisplatin-based concurrent radiochemotherapy. Tumor marker levels in serum as well as proto-oncogene and tumor suppressor gene expression in tumor tissue were compared between two groups of patients before and after treatment.Results:Before treatment, differences in tumor marker levels in serum as well as proto-oncogene and tumor suppressor gene expression in tumor tissue were not statistically significant between two groups of patients. After treatment, serum tumor markers SCC, CA50, CA724 and CEA levels of observation group were significantly lower than those of control group;proto-oncogene DEK, c-myc and PIK3CA mRNA expression in tumor tissue were significantly lower than those of control group;tumor suppressor genes p53, SOCS-1, FHIT and PTEN mRNA expression in tumor tissue were significantly higher than those of control group.Conclusions:Cisplatin-based concurrent radiochemotherapy can effectively reduce the tumor malignancy and balance the proto-oncogene / tumor suppressor gene expression in patients with advanced cervical cancer.

RET proto-oncogene mutation analysis in a pedigree with multiple endocrine neoplasia 2A

Objective To discuss clinical diagnosis and treatment of multiple endocrine neoplasia ( MEN) 2A,and report the mutation of RET proto-oncogene in a pedigree of three patients with MEN 2A. Methods Bilateral adrenalectomy was performed on two of the three

基于分子对接和QSAR方法预测B-Raf Ⅱ型抑制剂活性

B-Raf激酶在促分裂素原活化蛋白激酶(MAPK)信号转导通路中起着重要作用,已被确定为癌症治疗非常有吸引力的靶标.新型高效B-Raf抑制剂的开发成为癌症治疗的一个热门研究领域.本文以结构多样的B-Raf II型抑制剂为研究对象,联合应用分子对接和定量构效关系(QSAR)模型研究其定量构效关系去探讨抑制活性的起源.两个主题作为研究重点:生物活性构象和描述符.首先对分子对接方法(Glide、Gold、Ligand Fit、Cdocker和Libdock)进行准确性评价,后将研究的对象分子对接到B-Raf活性位点并获得生物活性构象.基于准确的对接结果,计算得到16个打分评价函数和21个能量描述符,以此构建定量构效关系模型.QSAR结果表明模型具有高度精确的拟合和强的预测能力(模型M1:r2=0.852,=0.790,=0.864;模型M2:r2=0.738,=0.812,=0.8605).同时探讨了对抑制活性有重要影响的描述符,结果表明打分评价函数(G_Score,-ECD,Dock_Score,PMF)与能量描述符(S(hb_ext),DE(int),Emodel)对抑制活性影响非常大.通过虚拟筛选和QSAR模型理论预测,一些新的具有潜在抑制活性的化合物作为B-Raf II型抑制剂被获得.上述信息对于进一步设计新颖高效的B-Raf II型抑制剂提供了有用的指导.

甲状腺乳头状癌中B-raf基因V600E突变的检测方法对比分析

甲状腺癌是最常见的内分泌恶性肿瘤，女性多于男性，约90％甲状腺癌为甲状腺乳头状癌（papillary thyroid careinoma,PTC）。近年，甲状腺癌的发病率呈上升趋势，B—raf基因与PTC密切相关，最多见的突变位点为V600E，是目前分析和检测的热点。本文回顾性分析136例PTC的B—raf基因V600E突变，并采用免疫组化Ventana BenchMark法和RT．PCR法进行检测，分析两种方法的一致性，

B-RAF基因特异的siRNA干扰对胃癌BGC823细胞的影响

为探讨B-RAF基因特异的siRNA干扰对胃癌BGC823细胞的增殖和凋亡的影响,设计并合成B-RAF小分子干扰RNA(B-RAF-siRNA)和阴性对照siRNA,用TransMessenger介导转染胃癌BGC823细胞,RT-PCR分析检测胃癌BGC823细胞中B-RAF基因以及Bcl-2基因的表达;MTT检测胃癌BGC823细胞增殖情况;流式细胞仪检测细胞凋亡情况,并与对照组进行比较。TransMessenger能够有效介导B-RAF-siRNA和阴性对照siRNA转染胃癌BGC823细胞,TransMessenger介导的B-RAF-siRNA有效地抑制胃癌BGC823细胞B-RAF以及Bcl-2基因的表达,与对照组相比,抑制率达90.0%以上,最高达100%;同时明显抑制胃癌BGC823细胞增殖;促进胃癌BGC823细胞的凋亡(P<0.01)。B-RAF基因特异的siRNA干扰能有效地抑制胃癌BGC823细胞中B-RAF基因以及Bcl-2基因的表达,同时促进胃癌细胞凋亡和抑制胃癌细胞增殖。

伊马替尼治疗晚期恶性黑色素瘤C-kit及B-raf基因突变患者的效果研究

目的:探讨伊马替尼对晚期恶性黑色素瘤C-kit及B-raf基因突变者的临床效果。方法:选择2010年1月—2014年1月收治的124例晚期恶性黑色素瘤患者,按照随机数字法分为观察组和对照组,每组各62例。对照组患者给予达卡巴嗪,观察组在对照组治疗的基础上联合应用伊马替尼,对所有患者随访2年,观察2组患者治疗过程中发生的不良反应、疗效及无病生存时间,并比较2组患者1、2年生存率。结果:2组患者化疗不良反应的差异无统计学意义(P>0.05);观察组患者的疾病缓解率为61.29%(38/62),显著高于对照组的22.58%(14/62),差异有统计学意义(P<0.05);观察组患者无病生存时间为(10.2±1.1)个月,显著长于对照组的(5.1±0.3)个月,差异有统计学意义(P<0.05);观察组患者1年及2年生存率均明显高于对照组,差异均有统计学意义(P<0.05)。结论:伊马替尼治疗晚期恶性黑色素瘤C-kit及B-raf基因突变患者,能有效控制疾病进展速度,延长患者生存时间,且不增加治疗过程中的不良反应。

白血病细胞系中B-Raf与Raf-1的表达及活性

目的研究白血病细胞及正常人外周血淋巴细胞中的 B- Raf和 Raf- 1表达水平及激酶活性。方法利用 Western印迹法检测 B- Raf和 Raf- 1表达水平，利用免疫沉淀及 Western印迹法检测 Raf- 1及 B- Raf的激酶活性。结果 Raf- 1在白血病细胞及正常人外周血淋巴细胞中均有表达 ,表达水平基本相似，其激酶活性较低； B- Raf仅在白血病细胞中表达，且在 Jurkat和 K562细胞中的表达水平较高，其激酶活性也较高。结论在白血病细胞中， B- Raf的高表达及活化可能是白血病发病的机制之一。

K-Ras与B-Raf在前列腺癌组织表达及其与预后的关系

目的研究K-Ras和B-Raf蛋白表达与前列腺癌发生及预后的关系。方法应用免疫组织化学方法(SP法)检测74例前列腺癌和39例前列腺增生组织K-Ras和B-Raf蛋白表达。74例前列腺癌中高中分化23例,低分化51例;未浸润转移(A+B)期40例,浸润转移(C+D)期34例。结果 K-Ras在前列腺癌组织的表达(79.73%,49/74)明显高于前列腺增生(23.08%,9/39),χ2=19.025,P<0.01。在高中分化与低分化组的表达分别为(65.22%,15/23)与(66.67%,34/51),χ2=0.15,P>0.05,在(A+B)期与(C+D)期表达分别为(60.00%,24/40)与(73.53%,25/34),χ2=1.504,P>0.05;B-Raf在前列腺癌表达(64.86%,48/74)明显高于前列腺增生组织(10.26%,4/39),χ2=30.659,P<0.05。在高中分化与低分化表达分别为(43.48%,10/23)与(74.51%,38/51),χ2=6.698,P<0.05,在(A+B)期与(C+D)期表达分别为(42.50%,17/40)与(91.18%,31/34),χ2=19.107,P<0.05。K-Ras与B-Raf蛋白表达呈正相关,χ2=0.272,P<0.05。结论 K-Ras与B-Raf蛋白过表达与前列腺癌的发生有关,B-Raf蛋白高表达预示着前列腺癌的预后较差。

BRAF V600E基因突变及B-raf蛋白表达在甲状腺乳头状癌病理诊断中的应用价值

甲状腺乳头状癌在全球范围内发病率上升较快。BRAF V600E基因突变及B-raf蛋白表达与甲状腺乳头状癌的临床病理联系近年来研究较多。本文从甲状腺乳头状癌的临床病理、BRAF V600E基因突变及B-raf蛋白表达三个方面的最新研究进展做一综述,探讨BRAF V600E基因突变及B-raf蛋白表达在甲状腺乳头癌病理诊断中的应用价值。

B-Raf蛋白在非小细胞肺癌中的表达及临床意义

目的 B-Raf蛋白表达与非小细胞肺癌发生的关系很重要,但它的表达状况尚未清楚,本试验旨在检测B-Raf蛋白在非小细胞肺癌组织和癌旁组织中的表达情况以及B-Raf蛋白与各临床病理参数的相关性。为研究非小细胞肺癌的分子靶向治疗提供更多的实验数据。方法采集大连市不同医院诊断明确的非小细胞肺癌手术切除标本95例,其中29例标本取癌旁组织,采用免疫组化方法检测各标本中B-Raf蛋白的表达。结果 B-Raf蛋白在非小细胞肺癌组织中的高表达率为64.21%,B-Raf蛋白表达与年龄显著相关(P<0.05)。结论非小细胞肺癌中存在B-Raf蛋白表达上调,B-Raf蛋白的表达随着年龄增长而增高。

细针穿刺细胞学B-raf基因检测对甲状腺乳头状癌的诊断意义

目的探讨细针穿刺细胞学B-raf基因检测对甲状腺乳头状癌的诊断意义。方法对113例B超检查提示为癌可疑结节患者术前均行B超引导下甲状腺细针穿刺,穿刺液除行细胞病理活检外同时行B-raf基因突变检查。113例患者中术后病理检查诊断为甲状腺乳头状癌患者98例,甲状腺良性病变患者15例,观察其诊断效率。结果 B-raf基因突变诊断灵敏度为40.82%,特异度为93.3%。B-raf基因是否突变与患者年龄、中央区淋巴结是否转移、颈部侧方区淋巴结是否转移、局部组织如喉返神经、肌肉是否侵犯及是否是多灶癌因素关系均不密切(均P>0.05)。结论术前联合细针穿刺细胞学检测B-raf基因突变能显著提高甲状腺乳头状癌细胞活检的诊断效率。

中国人胰腺导管内乳头状粘液性肿瘤B-RAF基因(V600E)突变的研究

胰腺导管内乳头状粘液性肿瘤（Intraductal Papillary Mucinous Neoplasms of the Pancreas,IPMNs）是胰腺癌最重要及最常见的癌前病变之一,约占临床诊断胰腺肿瘤的7%,占偶然发现的胰腺囊肿的50%[1,2]。IPMN分型包括伴轻度不典型增生、IPMN伴中度不典型增生、IPMN伴重度不典型增生及IPMN相关浸润性;

C634Y mutation in RET-induced multiple endocrine neoplasia type 2A:A case report

BACKGROUND Multiple endocrine neoplasia type 2(MEN2)is a rare,autosomal dominant endocrine disease.Currently,the RET proto-oncogene is the only gene implicated in MEN2A pathogenesis.Once an RET carrier is detected,family members should be screened to enable early detection of medullary thyroid carcinoma,pheochromocytoma,and hyperparatitity.Among these,medullary thyroid carcinoma is the main factor responsible for patient mortality.Accordingly,delineating strategies to inform clinical follow-up and treatment plans based on genes is paramount for clinical practitioners.CASE SUMMARY Herein,we present RET proto-oncogene mutations,clinical characteristics,and treatment strategies in a family with MEN2A.A family study was conducted on patients diagnosed with MEN2A.DNA was extracted from the peripheral blood of family members,and first-generation exon sequencing of the RET protooncogene was conducted.The C634Y mutation was identified in three family members spanning three generations.Two patients were sequentially diagnosed with pheochromocytomas and bilateral medullary thyroid carcinomas.A 9-yearold child harboring the gene mutation was diagnosed with medullary thyroid carcinoma.Surgical resection of the tumors was performed.All family members were advised to undergo complete genetic testing related to the C634Y mutation,and the corresponding treatments administered based on test results and associated clinical guidelines.CONCLUSION Advancements in MEN2A research are important for familial management,assessment of medullary thyroid cancer invasive risk,and deciding surgical timing.