Xeroderma pigmentosum group D polymorphisms and esophageal cancer susceptibility: A meta-analysis based on case-control studies

AIM: To clarify the effects of the xeroderma pigmentosum group D(XPD) Asp312 Asn and Lys751 Gln gene polymorphisms on the risk of esophageal cancer(EC).METHODS: A computerised literature search was conducted to identify the relevant studies from the PUBMED and EMBASE databases, reviews, and reference lists of relevant articles. Odds ratios(ORs) with 95% confidence intervals(CIs) were used to assess the associations between the XPD Asp312 Asn and/or Lys751 Gln polymorphisms and EC susceptibility. Statistical analyses were performed using the software Stata 12.0. A fixed or random effects model was selected based on a heterogeneity test. Publication bias was estimated using funnel plots and Egger's linear regression method. Subgroup analyses were performed based on histological type and ethnicity.RESULTS: Thirteen case-control studies with a total of 10 comparisons for the Asp312 Asn polymorphism, including 2373 cases and 3175 controls, and 15 comparisons for the Lys751 Gln polymorphism, including 3226 cases and 5237 controls, were recruited for the meta-analysis. In terms of the XPD Asp312 Asn polymorphism, significantly increased EC risks were identified in the Asp/Asn vs Asp/Asp comparison(OR = 1.17, 95%CI: 1.02-1.33, P = 0.03) and in the dominantmodel comparison(Asn/Asn+Asp/Asn vs Asp/Asp: OR = 1.18, 95%CI: 1.04-1.34, P = 0.01). However, no significant associations were found in the Asn/Asn vs Asp/Asp comparison(OR = 1.30, 95%CI: 1.00-1.70, P = 0.05) or in the recessive-model comparison(Asn/Asn vs Asp/Asn + Asp/Asp: OR = 1.17, 95%CI: 0.91-1.50, P = 0.22). In terms of the XPD Lys751 Gln polymorphism, a significant association with EC susceptibility was found under the recessive model(Gln/Gln vs Lys/Gln+Lys/Lys: OR = 1.21, 95%CI: 1.02-1.43, P = 0.03). However, no associations were identified in the other comparisons(co-dominant model: Lys/Gln vs Lys/Lys: OR = 1.11, 95%CI: 0.94-1.31, P = 0.20; Gln/Gln vs Lys/Lys: OR = 1.31, 95%CI: 0.98-1.75, P = 0.07; dominant model: OR = 1.14, 95%CI: 0.96-1.35, P = 0.14).CONCLUSION: The results of this meta-analysis suggest that the XPD Asp312 Asn and Lys751 Gln gene polymorphisms are associated with a significantly increased risk for EC.

Xeroderma Pigmentosa: High Risk for Ocular Neoplasia

Aim of Work: The aim of our work was early cytological and laboratory detection of any ocular surface malignant changes in xeroderma pigmentosa. Patients and Methods: Eighteen cases with xeroderma pigmentosa were included in this study. All cases were subjected to full ophthalmolog-ical examination, conjunctival biopsy from any abnormal lesion, polymerase chain reaction assay and impression cytology. Results: All cases were boys;the mean age was 11 years old. The main ocular presentation was dryness and abnormal epibulbar masses in different locations. Polymerase chain reaction represents precipitation of malignant cells which was confirmed by impression cytology. Conclusion: PCR and impression cytology are beneficial investigations for detection of any malignant changes in xeroderma pigmentosa.

Malignant and Pre-Malignant Manifestations of Xeroderma Pigmentosum in Ghanaians

Introduction: Xeroderma pigmentosum is an autosomal recessive disease with sun sensitivity, photophobia, early onset of freckling, and subsequent neoplastic changes on sun-exposed surfaces. There is cellular hypersensitivity to UV radiation and to certain chemicals in association with abnormal DNA repair. Patients with defective DNA nucleotide excision repair (NER) have defects in one of seven NER genes;xeroderma pigmentosum variants have normal NER and a defect in a polymerase gene. Study design: This is a case presentation of five patients with the features of xeroderma pigmentosum, aged 48, 26, 15, 14 and 8 years. The first and last patients were males. Each of the first four patients presented with areas of hyper- and hypo-pigmentation over sun exposed body surfaces. Each of them had a minimum of two cutaneous malignancies, distributed on the upper chest, face or scalp. The fifth patient had skin atrophy, with mottled hyperpigmentation and hypopigmentation but had no malignant lesions. Result: The first, second and fourth patients had their lesions surgically excised and the defects were skin grafted. The third patient was treated with radiotherapy. All the lesions were confirmed histologically as squamous cell carcinoma. No recurrence has been observed. Conclusion: Xeroderma pigmentosum in Ghanaians presents with squamous cell carcinoma involving the head, neck and upper trunk. A minimum period of exposure to UV radiation, not precisely known, is required for the development of the lesions. Education on sun avoidance and protective clothing is necessary to prevent morbidity and mortality.

Xeroderma Pigmentosum with Desquamative Gingivitis a Rare Case Report and Detailed Review of Literature

In xeroderma pigmentosum, a rare genodermatosis, transmitted as an autosomal recessive disorder, excessive solar damage to the skin develops at an early age. The disease is characterized by cutaneous, ocular, neurological and oral changes. Oral features in the form of early development of Squamous cell carcinoma, usually at the lower lip and tip of the tongue may be seen. The disorder is associated more commonly in populations where marriage of close blood relatives is common. Treatment of the disorder includes avoidance of Ultra violet radiation, topical application of 5 fluorouracil to treat actinic keratoses, and regular evaluation by an optholmologist, dermatologist, and neurologist. Genetic counseling is an important aspect as an increased incidence of consanguineous marriages have been reported with this disorder. Here, we report an interesting case of xeroderma pigmentosum in an 18 year old male patient who presented with characterstic desquamation of gingiva, fissured tongue and geoghraphic tongue.

Xeroderma pigmentosa with ocular association: Case report

Xeroderma pigmentosum is a rare, autosomal recessive disease caused by a defect in DNA repair. Patients with xeroderma pigmentosum often have cutaneous and ocular sun sensitivity, freckle-like skin pigmentation, multiple skin and eye cancers, and, in some patients, progressive neurodegeneration. Xeroderma pigmentosum predominantly affects the ultraviolet (UV) exposed ocular surface, resulting in eyelid atrophy and cancers, corneal dryness, exposure keratopathy, and conjunctival tumors. General features included parental consanguinity (40%), familiarity (60%), onset of symptoms in the first 2 years (50%), malignant skin neoplasms (60%), and carcinoma of the tongue (20%). Among the ocular features, 50% of patients presented with photophobia. Lid freckles or atrophic skin lesions were seen in all patients. Lower lid tumours were seen in 30%, chronic conjunctival congestion in 40%, corneal opacification in 40%, squamous cell carcinoma of limbus in 20%, bilateral pterygium in 40%, and visual impairment in 50%. We report the clinical history and ocular pathology of a boy who is having xeroderma pigmentosum with ocular manifestations. The ophthalmic manifestations of xeroderma pigmentosum are discussed and reviewed with respect to this report and other cases in the literature. These cases illustrate the role of DNA repair in protection of the eyes from UV damage and neuron degeneration of the retina.

Xeroderma pigmentosum group D 751 polymorphism as a predictive factor in resected gastric cancer treated with chemo-radiotherapy

AIM: To evaluate the potential association of xeroderma pigmentosum group D (XPD) codon 751 variant with outcome after chemo-radiotherapy in patients with resected gastric cancer. METHODS: We used PCR-RFLP to evaluate the genetic XPD Lys751Gln polymorphisms in 44 patients with stage Ⅲ (48%) and Ⅳ (20%) gastric cancer treated with surgery following radiation therapy plus 5-fluorouracil/ leucovorin based chemotherapy. RESULTS: Statistical analysis showed that 75% (12 of 16) of relapse patients showed Lys/Lys genotype more frequently (P = 0.042). The Lys polymorphism was an independent predictor of high-risk relapse-free survival from Cox analysis (HR: 3.07, 95% CI: 1.07-8.78, P = 0.036) and Kaplan-Meir test (P = 0.027, log-rank test). CONCLUSION: XPD Lys751Gln polymorphism may be an important marker in the prediction of clinical outcome to chemo-radiotherapy in resected gastric cancer patients.

Modeling xeroderma pigmentosum associated neurological pathologies with patients-derived iPSCs

Xeroderma pigmentosum （XP） is a group of genetic disorders caused by mutations of XP-associated genes, resulting in impairment of DNA repair. XP patients frequently exhibit neurological degeneration, but the underlying mechanism is unknown, in part due to lack of proper disease models. Here, we generated patientspecific induced pluripotent stem cells （iPSCs） harboring mutations in five different XP genes including XPA, XPB, XPC, XPG, and XPV. These iPSCs were further differentiated to neural cells, and their susceptibility to DNA damage stress was investigated. Mutation of XPA in either neural stem cells （NSCs） or neurons resulted in severe DNA damage repair defects, and these neural cells with mutant XPA were hyper-sensitive to DNA damage-induced apoptosis. Thus, XP-mutant neural cells represent valuable tools to clari the molecular mechanisms of neurological abnormalities in the XP patients.

COL4A1促进肝癌细胞的增殖、迁移、侵袭和上皮-间质转化

目的探讨Ⅳ型胶原蛋白1(COL4A1)对肝癌细胞增殖、迁移、侵袭和上皮-间质转化(EMT)的作用,及其上游调控机制。方法将COL4A1过表达载体、人着色性干皮病基因(XPD)过表达载体、miR-29a-3p模拟物、miR-29a-3p抑制物、Si-COL4A1、Si-XPD按实验目的转染各组细胞,以空载质粒、NC-模拟物、NC-抑制物、NC-SiRNA作为相应的对照组;qRT-PCR检测COL4A1和XPD mRNA水平;蛋白质印迹法检测COL4A1、XPD和EMT相关蛋白质水平;MTT检测细胞活力;Transwell实验检测各组细胞的迁移、侵袭能力;萤光素酶报告基因实验验证miR-29a-3p和COL4A1的靶向关系。结果肝癌组织中COL4A1 mRNA[(3.25±1.10)vs(0.88±0.45),P<0.01]和蛋白质[(2.58±0.50)vs(1.00±0.14),P<0.01]水平均高于癌旁组织。SMMC-7721、HepG2(P<0.01)和Hep3B(P<0.05)细胞株的COL4A1 mRNA和蛋白质水平均高于L02细胞。与Hep3B+空载质粒相比,过表达COL4A1促进了Hep3B细胞增殖[(0.48±0.06)vs(0.76±0.09),P<0.01]、迁移[(109.00±9.17)个vs(199.33±15.04)个,P<0.01]、侵袭[(84.67±8.02)个vs(133.00±11.53)个,P<0.01]和EMT(P<0.05)。与HepG2+NC-SiRNA相比,沉默COL4A1抑制了HepG2细胞增殖[(0.62±0.09)vs(0.42±0.03),P<0.01]、迁移[(173.00±12.00)个vs(75.00±7.94)个,P<0.01]、侵袭[(105.33±7.51)个vs(47.00±5.57)个,P<0.01]和EMT(P<0.05)。过表达XPD后,HepG2细胞的COL4A1 mRNA[(1.00±0.09)vs(0.55±0.06),P<0.01]和蛋白质[(1.00±0.09)vs(0.33±0.04),P<0.01]水平较HepG2+空载质粒组下降,沉默XPD在Hep3B细胞中出现了相反的结果[与Hep3B+NC-SiRNA相比:mRNA,(1.00±0.08)vs(2.52±0.25);蛋白质,(1.00±0.09)vs(2.56±0.36),P<0.01]。转染miR-29a-3p模拟物后,HepG2细胞中COL4A1 mRNA[(1.00±0.13)vs(0.47±0.07),P<0.01]和蛋白质[(1.00±0.15)vs(0.36±0.09),P<0.01]水平较NC-模拟物+HepG2下降;而miR-29a-3p抑制物在Hep3B细胞中出现了相反的结果[与NC-抑制剂+Hep3B相比:mRNA,(1.00±0.13)vs(3.30±0.41),P<0.01;蛋白质,(1.00±0.14)vs(2.91±0.30),P<0.01]。miR-29a-3p模拟物逆转了沉默XPD介导的Hep3B细胞COL4A1上调(P<0.01)。结论COL4A1促进肝癌细胞的增殖、迁移、侵袭和EMT,并受XPD-miR-29a-3p轴的负性调控。

XPC rs2228000位点多态性与乳腺癌发病的关系

目的探讨DNA损伤修复基因着色性干皮病基因组C(XPC)rs2228000位点多态性与乳腺癌发病的相关性。方法选取女性乳腺癌患者562例(乳腺癌组)、女性体检健康者572名(正常对照组)。收集所有研究对象的一般资料和乳腺癌患者的临床病理资料。采用聚合酶链反应(PCR)-限制性片段长度多态性(RFLP)检测XPC基因。采用Logistic回归分析评估XPC rs2228000位点多态性与乳腺癌发病的关系。结果乳腺癌组XPC rs2228000位点CC基因型(野生型)、CT基因型(杂合型)和TT基因型(纯合型)的分布频率分别为33.2%、50.9%、15.9%,正常对照组分别为43.2%、48.4%、8.4%,2个组各基因型的分布频率差异有统计学意义(χ^(2)=14.59,P<0.01);2个组之间等位基因C和T的分布频率差异有统计学意义(χ^(2)=10.5,P<0.01)。Logistic回归分析结果显示,携带T等位基因的个体乳腺癌发生风险是携带C等位基因个体的1.52倍[比值比(OR)值=1.52,95%可信区间(CI)为1.37~1.94]。雌激素受体(ER)阳性、病理类型为浸润性导管癌的乳腺癌患者XPC rs2228000位点基因型分布分别与ER阴性、其他病理类型的患者比较,差异均有统计学意义(P<0.05);不同年龄、绝经状态、孕激素受体(PR)表达、BRCA1基因表达的乳腺癌患者之间XPC rs2228000位点基因型分布差异均无统计学意义(P>0.05)。结论XPC rs2228000位点多态性与乳腺癌发病有一定关系。

着色性干皮病39例临床分析

目的获取我国着色性干皮病(XP)患者更多的临床定量描述数据。方法回顾分析了我国39例XP患者的临床资料。结果3岁以内发病者占2/3。28.2%的XP患者出现眼部病变,20.5%的患者出现神经病变。恶性肿瘤的平均发病年龄为19.3岁。患者父母为近亲结婚者占61.3%,1/3患者中有兄弟姊妹同患本病。兄弟姊妹同患本病者,父母近亲结婚达72.7%。结论本组XP患者发生恶性肿瘤的平均年龄(19.3岁)大于国外平均发病年龄(8岁)。本组XP患者的存活年龄比国外患者大。近亲结婚者后代出现XP患者,兄弟姊妹同患本病比非近亲结婚者可能性大。

细菌衍生黑素对长波紫外线诱导人皮肤成纤维细胞凋亡和坏死的保护

目的:探讨细菌衍生黑素(b-melanin)对长波紫外线(UVA)诱导人成纤维细胞凋亡和坏死产生的光保护作用,为今后将其用作皮肤光保护剂提供依据。方法:正常人成纤维细胞(NL-FB)和着色性干皮病患者成纤维细胞(XP-FB)经UVA照射12h后,以四甲基偶氮唑蓝(MTT)法检测细胞存活率,Hoechst33258染色法观察早期凋亡细胞核形态学变化,二氯荧光素二酯(DCFH-DA)标记法测定细胞内活性氧基(ROS)水平。结果:UVA照射诱导细胞的半数致死剂量,XP-FB大约为30J/cm2,而NL-FB>40J/cm2。为了观察不同浓度(0,25,50,100,200,400,和800μg/mL)的b-melanin是否对细胞存在光保护作用,给予半数致死剂量(30J/cm2)UVA照射后,经100～400μg/mLb-melanin处理的XP-FB的细胞存活率均较未处理组明显增高(P<0.01),而NL-FB的细胞存活率变化不明显。细胞内ROS测定结果显示100、400μg/mL的b-melanin能明显清除UVA诱导产生的ROS。100μg/mL b-melanin即能阻止非致死剂量(16J/cm2)UVA照射诱导的早期凋亡细胞核改变。结论:b-melanin能对UVA诱导人成纤维细胞凋亡和坏死提供有效的光保护,这一作用很可能关系到b-melanin对ROS的清除。本研究还首次提出核酸切除修复机制缺陷的XP-FB是一敏感的可用于测试UVA光损伤作用的体外细胞模型。

13例着色性干皮病临床及部分随访报告

报告了１９８４～１９９２年宁夏地区６家系１３例着色性干皮病（ＸＰ）患者的临床及两家系４例患者长达８年的随访情况。结合文献，就ＸＰ患者的临床、分型、血缘关系及肿瘤的发生进行了分析讨论。

着色性干皮病基因组D和胞苷脱氨酶基因单核苷酸多态性与肺癌易感性的关系

目的探讨着色性干皮病基因组D(XPD)和胞苷脱氨酶(CDA)基因单核苷酸多态性与肺癌易感性及其病理类型的关系,并探讨吸烟与基因多态性的交互作用对肺癌发病风险的影响。方法采用病例-对照研究方法纳入肺癌患者和健康对照者各103人,采用聚合酶链反应-限制性片段长度多态性(PCR-RFLP)法分析两组人群XPD基因外显子10G→A(Asp312Asn)、23A→C(Lys751Gln)以及CDA基因外显子1上79A→C(Lys27Gln)、208G→A(Ala70 Thr)的基因型。结果两组XPD312和XPD751位点的基因分布频率比较差异均无统计学意义(P>0.05);但吸烟合并XPD第751位点突变个体发生肺癌的风险显著增加(P=0.044);同时发生XPD第312和751两个位点突变的肺癌风险增加6.13倍(P=0.047)。两组CDA Lys27Gln和CDAAla70 Thr基因分布频率差异无统计学意义(P>0.05)。XPD和CDA在不同病理类型中的基因分布频率差异无统计学意义(P>0.05)。结论吸烟可使XPD第751位点发生突变的个体发生肺癌的风险增加,XPD基因第312和751两个位点同时突变使肺癌发生的风险增加。

GSTP1、XPG基因多态性与晚期非小细胞肺癌患者铂类药物化疗疗效及生存期的关系

背景与目的:本文旨在探讨谷胱甘肽S转移酶P1(glutathione S-transferase P1,GSTP1)基因A105G和人着色性干皮病G组(xeroderma pigmentatosum group G,XPG)基因C46T多态性与晚期非小细胞肺癌(non-small cell lung cancer,NSCLC)患者对以铂类药物为主方案的化疗疗效及生存期的关系。方法:经病理学确诊的晚期NSCLC患者85例,化疗前取静脉血采用DNA测序法检测GSTP1 A105G和XPG C46T多态性,给予以铂类药物为主方案的化疗,2个周期后进行临床疗效评价(RECIST标准)并统计疾病进展时间(time to progression,TTP)和总生存时间(overall survival,OS),分析GSTP1 A105G和XPG C46T多态性与化疗疗效及生存期的关系。结果:85例晚期NSCLC患者中,GSTP1 A/G+G/G基因型和A/A基因型患者化疗有效率分别为43.59%和19.57%,差异有统计学意义(χ2=5.738,P<0.05);XPG C/C基因型和C/T+T/T基因型患者化疗有效率分别为42.86%和18.60%,差异有统计学意义(χ2=5.886,P<0.05);联合多态性分析显示,同时携带GSTP1 A/G+G/G和XPG C/C基因型患者化疗有效率最高为44.74%,组间比较差异有统计学意义(P<0.05)。至随访结束,81例患者中位TTP为6.5个月,其中GSTP1 A/G+G/G基因型为8.0个月,A/A基因型为6.0个月,差异有显著统计学意义(χ2=14.688,P<0.01);XPG C/C基因型为7.5个月,C/T+T/T基因型为6.0个月,差异有显著统计学意义(χ2=10.897,P<0.01);联合多态性分析显示,同时携带GSTP1 A/G+G/G和XPG C/C基因型患者的中位TTP最长为8.0个月,组间比较差异有显著统计学意义(P<0.01)。78例患者中位OS为9.0个月,其中GSTP1 A/G+G/G基因型为11.0个月,A/A基因型为9.0个月,差异有显著统计学意义(χ2=14.522,P<0.01);XPG C/C基因型为10.5个月,C/T+T/T基因型为9.0个月,差异有显著统计学意义(χ2=12.136,P<0.01);联合多态性分析显示,同时携带GSTP1 A/G+G/G和XPG C/C基因型患者的中位OS最长为11.0个月,组间比较差异有显著统计学意义(P<0.01)。结论:GSTP1 A105G和XPG C46T多态性可单独及联合用于预测晚期NSCLC患者对以铂类药物为主方案的化疗疗效及生存期,初步提示可以根据患者基因型来指导个体化治疗。

XRCC1和XPD单核苷酸多态性与非小细胞肺癌铂类药物化疗敏感性的关系

目的研究X线修复交叉互补基因1(XRCC1)和着色性干皮病基因(XPD)单核苷酸多态性与老年晚期非小细胞肺癌(NSCLC)铂类药物化疗敏感性关系。方法应用聚合酶链反应结合限制性片段长度多态性(PCR-RFLP)的方法检测81例以铂类药物为主要化疗方案的NSCLC患者XRCC1Arg399Gln和XPDLys751Gln基因型多态性,采用非条件Logistic回归分析不同基因型与化疗疗效的关系。结果81例患者化疗总有效率为35.8%,其中完全缓解(CR)、部分缓解(PR)、稳定(SD)和进展(PD)患者分别为0、29、31、21例。携带至少1个XRCC1399Arg等位基因的患者化疗敏感性是携带Gln/Gln基因型患者的4.52倍(OR=4.52,95%CI=1.11～18.38)。未发现XPDLys751Gln遗传多态与化疗敏感性相关。结论XRCC1Arg399Gln多态可能与晚期NSCLC铂类药物化疗敏感性有关。

着色性干皮病G组基因多态性与喉癌和喉咽癌风险的相关性

目的研究DNA修复基因着色性干皮病G组基因(XPG)Asp1104His多态性与喉癌和喉咽癌风险的相关性。方法采用聚合酶链反应-限制性片段长度多态分析检测175例喉癌或喉咽癌患者和525名无肿瘤正常对照者的XPG基因型,采用多因素logistic回归模型计算各基因型携带者患喉癌和喉咽癌的风险及各基因型对肿瘤病理分级的影响。结果与Asp/Asp基因型比较,XPG1104Asp/His杂合型增加喉癌的发病风险(OR=2.46;95%CI=1.15～5.24,P<0.05),但不影响喉咽癌的发病风险(OR=1.36;95%CI=0.87～2.12,P>0.05);杂合基因型Asp/His增加高分化鳞状细胞癌的发病风险(OR=1.88;95%CI=1.05～3.40,P<0.05)。结论DNA修复基因XPG1104Asp/His多态性与喉癌的发病风险相关。

人着色性干皮病D组基因的克隆及其真核表达

着色性干皮病D组蛋白(Xeroderma pigmentosum group D,XPD)是基础转录因子ⅡH(Transcript factorⅡH,TFⅡH)复合体的第二大亚基,它在转录和核苷酸剪切修复过程中都发挥着重要作用。我们利用人宫颈鳞癌上皮细胞(HeLa细胞)中提取的总RNA进行逆转录酶-聚合酶链反应(Reverse transcriptase-polymerase chain reac-tion,RT-PCR),克隆出人全长XPD cDNA,把此基因按野生型插入表达绿色荧光蛋白的pEGFP-N2质粒,构建了pEGFP-N2/XPD重组体质粒,并将其转染入整合有乙肝病毒X蛋白(Hepatitis B virus X protein,HBx)的人肝癌细胞Hep3B,分析重组细胞的XPD表达水平、HBx表达水平和细胞增殖力,为进一步研究XPD的各种生物学活性及作用机制奠定了基础。

着色性干皮病并发黑素瘤和血管肉瘤

报告1例着色性干皮病。患者男,26岁。全身泛发色素斑、雀斑样损害20余年,头面部及下眼睑肿物2年,日光曝露部位皮肤色素进行性增加。皮损组织病理检查诊断为血管肉瘤和黑素瘤。

核苷酸切除修复基因XPA反义RNA增强肺癌细胞对顺铂的敏感性

背景与目的:目前认为,肿瘤细胞自身核苷酸切除修复(nucleotideexcisionrepair,NER)能力增强是肿瘤细胞产生耐药性最重要的机制之一。着色性干皮病A(xerodermapigmentosungroupA,XPA)基因在核苷酸切除修复早期发挥核心作用。本研究拟探讨XPA基因表达与肺癌细胞株对顺铂敏感性的关系。方法:将XPA的反义RNA稳定转染人肺癌细胞株A549,用有限稀释法筛选阳性细胞克隆。分别用Northernblot和Westernblot法检测阳性细胞克隆XPAmRNA和蛋白水平;MTT法检测肿瘤细胞对顺铂敏感性;宿主细胞再活化反应(hostcellreactivation,HCR)检测肿瘤细胞DNA损伤修复能力。结果:筛选得到6个阳性克隆AS1～AS6,其中AS3～AS6细胞克隆的XPAmRNA和蛋白水平均明显降低。剂量依赖实验表明,顺铂对A549细胞与AS1～AS6细胞克隆的半数抑制浓度(IC50)分别为8.1、7.6、4.7、3.2、1.9、2.8、4.1滋g/ml。统计学分析表明,与A549细胞相比,AS3～AS6细胞对顺铂的敏感性明显增强(F=9.75、9.14、7.39、8.91,P=0.005、0.006、0.012、0.006),而且XPAmRNA表达水平与细胞IC50值呈显著相关(r=0.927,P=0.003)。处理24、48、72h后,AS3～AS6细胞对顺铂的敏感性同样显著增强。HCR实验结果表明,AS3～AS6细胞的NER能力显著减弱,而且XPAmRNA表达水平与细胞NER能力呈?

荧光偏振技术分析全血XPD基因单核苷酸多态性的研究

将荧光偏振与非对称基因扩增技术联用,建立了可用于检测全血XPD基因单核苷酸多态性的新方法。用不等量(1∶5)的XPD基因上、下游引物对含单核苷酸多态性位点的目的片段进行非对称扩增,再用两种单核苷酸多态性序列特异的荧光标记探针对扩增产物进行检测。由于扩增得到的单链片段能够与各自不同的荧光标记探针特异结合,使荧光标记分子的分子量增加,偏振值(FP)增高。通过检测增高的FP值,可确定目的片段单核苷酸多态性。采用本方法对98例全血的XPD基因第751位密码子进行了单核苷酸多态性分析,并与传统的荧光偏振检测方法进行了比较,取得满意结果。