Journal of Cancer Research and Therapeutic Oncology最新文献_第5页

A Pediatric Nasal Esthesioneuroblastoma Treated by Helical Tomotherapy 螺旋断层治疗儿童鼻感觉神经母细胞瘤

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2014-07-01 DOI: 10.13189/COR.2014.020501

M. F. Çetindağ, Y. Cihan, F. Altıntaş

Purpose: To compare 3-dimensional conformal radiotherapy (3DCRT) with intensity modulated radiotherapy (IMRT) in the irradiation of pediatric head and neck tumor. Case report: A 13-year old boy with the diagnosis of olfactory neuroblastoma (stage Kadish B), who had postoperative residual disease referred to our clinic for adjuvant radiotherapy (RT). A total of 60 Gy image guided (IG)-IMRT were applied in two phases (50Gy/30 fractions and 10 Gy/5 fractions). Before irradiation, RT planning was performed by in two different therapy techniques, namely 3DCRT and IMRT, and these techniques were compared regarding conformation number (CN) and homogeneity index (HI) for planning target volume (PTV), as well as maximum, minimum and mean doses for selected critical organs and PTV. Results: IMRT planning with helical tomotherapy had an apparent superiority compared to 3DCRT planning, as expected. The patient was maintaining remission after 26 months from RT and no side effect related to RT were detected. Conclusions: Today, irradiation of pediatric tumors with 3DCRT is the standard practice. However, IMRT may be required in case of tumors at close proximity to the critical organs in which high dose of irradiation is indicated.

目的:比较三维适形放疗(3DCRT)与调强放疗(IMRT)治疗小儿头颈部肿瘤的疗效。病例报告:一名13岁男孩，诊断为嗅觉神经母细胞瘤(卡迪什B期)，术后残留疾病转介至我诊所进行辅助放疗。共应用60 Gy图像引导(IG)-IMRT两阶段(50Gy/30分和10 Gy/5分)。放疗前，采用3DCRT和IMRT两种不同的治疗技术进行放疗计划，比较两种治疗技术规划靶体积(PTV)的构象数(CN)和均匀性指数(HI)，以及选定关键器官和PTV的最大、最小和平均剂量。结果:与3DCRT计划相比，螺旋ct计划具有明显的优势，正如预期的那样。患者在接受放射治疗26个月后保持缓解，未发现与放射治疗相关的副作用。结论:目前，3DCRT照射儿童肿瘤是标准做法。然而，在肿瘤靠近关键器官且需要高剂量照射的情况下，可能需要进行IMRT。

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引用次数: 0

Correlation of Breast Cancer Subtypes Based on ER, PR and HER2 Expression with Axillary Lymph Node Status 基于ER、PR和HER2表达的乳腺癌亚型与腋窝淋巴结状态的相关性

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2014-05-01 DOI: 10.13189/cor.2014.020402

Elsayed M Ali, Ahmed R. H. Ahmed, Ayman M. A. Ali

引用次数: 22

Evaluation of Melanin-Targeted Radiotherapy in Combination with Radiosensitizing Drugs for the Treatment of Melanoma 黑色素靶向放疗联合放射增敏药物治疗黑色素瘤的疗效评价

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2014-05-01 DOI: 10.13189/COR.2014.020403)

S. Hutchison, C. Rae, M. Tesson, J. Babich, M. Boyd, R. Mairs

The incidence of malignant melanoma is rising faster than that of any other cancer in the United States. An [131I]-labeled benzamide - [131I]MIP-1145 - selectively targets melanin, reduces melanoma tumor burden and increases survival in preclinical models. Our purpose was to determine the potential of radiosensitizers to enhance the anti-tumor efficacy of [131I]MIP-1145. Melanotic (A2058) and amelanotic (A375 and SK-N-BE(2c)) cells were treated with [131I]MIP-1145 as a single agent or in combination with drugs with radiosenitizing potential. Cellular uptake of [131I]MIP-1145 and toxicity were assessed in monolayer culture. The interaction between radiosensitizers and [131I]MIP-1145 was evaluated by combination index analysis in monolayer cultures and by delayed growth of multicellular tumor spheroids. [131I]MIP-1145 was taken up by and was toxic to melanotic cells but not amelanotic cells. Combination treatments comprising [131I]MIP-1145 with the topoisomerase inhibitor topotecan or the PARP-1 inhibitor AG014699 resulted in synergistic clonogenic cell kill and enhanced delay of the growth of spheroids derived from melanotic melanoma cells. The proteasome inhibitor bortezomib had no synergistic cytotoxic effect with [131I]MIP-1145 and failed to enhance the delay of spheroid growth. Following combination treatment of amelanotic cells, neither synergistic clonogenic cell kill nor enhanced growth delay of spheroids was observed.

在美国，恶性黑色素瘤的发病率上升速度比任何其他癌症都要快。一种[131I]标记的苯甲酰胺- [131I]MIP-1145 -选择性靶向黑色素，减少黑色素瘤肿瘤负担，提高临床前模型的生存率。我们的目的是确定放射增敏剂增强[131I]MIP-1145抗肿瘤疗效的潜力。[131I]MIP-1145单独或与具有放射致敏潜力的药物联合治疗黑色素瘤(A2058)和无色素瘤(A375和SK-N-BE(2c))细胞。在单层培养中评估[131I]MIP-1145的细胞摄取和毒性。放射增敏剂与[131I]MIP-1145之间的相互作用通过单层培养的联合指数分析和多细胞肿瘤球体的延迟生长来评估。[131I]MIP-1145被黑色素细胞吸收并对其有毒性，但对无色素细胞没有毒性。由[131I]MIP-1145与拓扑异构酶抑制剂topotecan或PARP-1抑制剂AG014699组成的联合治疗可协同杀死克隆细胞，并增强延迟黑素黑色素瘤细胞衍生的球体的生长。蛋白酶体抑制剂硼替佐米(bortezomib)与[131I]MIP-1145没有协同细胞毒作用，也不能增强延缓球体生长。在无色素细胞联合处理后，既没有观察到增效克隆细胞杀伤作用，也没有观察到球体生长延迟的增强。

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引用次数: 3

Effectiveness of Health Belief Model in Motivating for Tobacco Cessation and to Improving Knowledge, Attitude and Behavior of Tobacco Users 健康信念模型在激励戒烟及改善烟草使用者知识、态度和行为方面的有效性

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2014-05-01 DOI: 10.13189/COR.2014.020401

P. Renuka, K. Pushpanjali, Ramaiah Dental

There is an alarming increase in tobacco use in younger generation & it is responsible for 90% of oral cancers. A quasi-experimental study was conducted in dental health care settings to assess the effectiveness of health education in improving knowledge, attitude and behaviors of current tobacco users, towards tobacco use, among the patients visiting dental health settings. Study comprised of 20-35 years 88 current tobacco users. Health education was based on the Health Belief Model (HBM). Questionnaire was used to assess knowledge, attitude, and behavior of subjects. Leaflet and video were prepared for aid in health education Descriptive analysis, Paired t-test, Stratified analysis, Pearson Correlation analysis were employed. Improvement in decision to enl in to the tobacco cessation program was 33.7%. There was a statistical significant improvement in knowledge and attitude, of all subjects, in behavior domain significant improvement seen in subjects aged between 20-25 years, literate, smokers, and those utilizing dental health care services more than once in a year. Results of this study concluded that health education based on HBM was effective in motivating to enroll in to tobacco cessation program and improving knowledge and attitude of the tobacco users towards tobacco use and in improving behaviors of younger subjects, literates, smokers and subjects utilizing the dental health services more than once in year.

年轻一代中烟草使用的增加令人震惊&它是导致90%口腔癌的原因。本研究在牙科保健机构进行了一项准实验研究，以评估健康教育在改善牙科保健机构患者当前烟草使用者对烟草使用的知识、态度和行为方面的有效性。研究对象为20-35岁的88名目前的烟草使用者。健康教育基于健康信念模型(HBM)。采用问卷对被试的知识、态度和行为进行评估。采用描述性分析、配对t检验、分层分析、Pearson相关分析。决定参加戒烟计划的改善率为33.7%。所有受试者在知识和态度方面均有统计学意义上的显著改善，在行为方面，年龄在20-25岁之间、识字、吸烟和每年使用一次以上牙科保健服务的受试者有显著改善。本研究结果表明，以HBM为基础的健康教育在激励吸烟者参加戒烟计划、改善吸烟者对烟草使用的知识和态度以及改善年轻受试者、文盲、吸烟者和每年使用一次以上牙科保健服务的受试者的行为方面是有效的。

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引用次数: 28

Anti-Neoplastic Cytotoxicity of Gemcitabine-(C₄-amide)-[anti-EGFR] in Dual-combination with Epirubicin-(C₃-amide)-[anti-HER2/neu] against Chemotherapeutic-Resistant Mammary Adenocarcinoma (SKBr-3) and the Complementary Effect of Mebendazole. 吉西他滨-(C4-酰胺)-[抗EGFR]与表柔比星-(C3-酰胺)-[抗HER2/neu]双重组合对化疗耐药乳腺腺癌（SKBr-3）的抗肿瘤细胞毒性及甲苯咪唑的辅助作用

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2014-04-09 DOI: 10.17303/jcrto.2014.203

C P Coyne, Toni Jones, Ryan Bear

Aims: Delineate the feasibility of simultaneous, dual selective "targeted" chemotherapeutic delivery and determine if this molecular strategy can promote higher levels anti-neoplastic cytotoxicity than if only one covalent immunochemotherapeutic is selectively "targeted" for delivery at a single membrane associated receptor over-expressed by chemotherapeutic-resistant mammary adenocarcinoma.

Methodology: Gemcitabine and epirubicin were covalently bond to anti-EGFR and anti-HER2/neu utilizing a rapid multi-phase synthetic organic chemistry reaction scheme. Determination that 96% or greater gemcitabine or epirubicin content was covalently bond to immunoglobulin fractions following size separation by micro-scale column chromatography was established by methanol precipitation analysis. Residual binding-avidity of gemcitabine-(C₄-amide)-[anti-EG-FR] applied in dual-combination with epirubicin-(C₃-amide)-[anti-HER2/neu] was determined by cell-ELIZA utilizing chemotherapeutic-resistant mammary adenocarcinoma (SKBr-3) populations. Lack of fragmentation or polymerization was validated by SDS-PAGE/immunodetection/chemiluminescent autoradiography. Anti-neoplastic cytotoxic potency was determined by vitality stain analysis of chemotherapeutic-resistant mammary adenocarcinoma (SKBr-3) monolayers known to uniquely over-express EGFR (2 × 10⁵/cell) and HER2/neu (1 × 10⁶/cell) receptor complexes. The covalent immunochemotherapeutics gemcitabine-(C₄-amide)-[anti-EGFR] and epirubicin-(C₃-amide)-[anti-HER2/neu] were applied simultaneously in dual-combination to determine their capacity to collectively evoke elevated levels of anti-neoplastic cytotoxicity. Lastly, the tubulin/microtubule inhibitor mebendazole evaluated to determine if it's potential to complemented the anti-neoplastic cytotoxic properties of gemcitabine-(C4-amide)-[anti-EGFR] in dual-combination with epirubicin-(C₃-amide)-[anti-HER2/neu].

Results: Dual-combination of gemcitabine-(C₄-amide)-[anti-EGFR] with epirubicin-(C₃-amide)-[anti-HER2/neu] produced greater levels of anti-neoplastic cytotoxicity than either of the covalent immunochemotherapeutics alone. The benzimidazole microtubule/tubulin inhibitor, mebendazole complemented the anti-neoplastic cytotoxicity of gemcitabine-(C₄-amide)-[anti-EGFR] in dual-combination with epirubicin-(C₃-amide)-[anti-HER2/neu].

Conclusions: The dual-combination of gemcitabine-(C₄-amide)-[anti-EGFR] with epirubicin-(C₃-amide)-[anti-HER2/neu] produced higher levels of selectively "targeted" anti-neoplastic cytotoxicity against chemotherapeutic-resistant mammary adenocarcinoma (SKBr-3) than either covalen

目的：探讨同时、双重选择性 "靶向 "递送化疗药物的可行性，并确定与只选择性地 "靶向 "一种共价免疫疗法相比，这种分子策略是否能提高抗肿瘤细胞毒性：方法：利用快速多相合成有机化学反应方案，将吉西他滨和表柔比星与抗表皮生长因子受体（anti-EGFR）和抗甲状腺素受体（anti-HER2/neu）共价结合。通过甲醇沉淀分析确定，在微尺度柱层析法进行尺寸分离后，96% 或更高含量的吉西他滨或表柔比星与免疫球蛋白馏分共价结合。利用化疗耐药乳腺腺癌（SKBr-3）细胞ELIZA测定了吉西他滨-（C4-酰胺）-[抗EG-FR]与表柔比星-（C3-酰胺）-[抗HER2/neu]双重结合的残余结合活性。通过 SDS-PAGE/免疫检测/化学发光自显影验证了其不存在碎裂或聚合现象。通过对化疗耐药乳腺腺癌（SKBr-3）单层细胞进行活力染色分析，确定了其抗新生物细胞毒性的效力，已知这些单层细胞独特地过度表达表皮生长因子受体（2×105/细胞）和HER2/neu（1×106/细胞）受体复合物。共价免疫疗法吉西他滨-(C4-酰胺)-[抗表皮生长因子受体]和表柔比星-(C3-酰胺)-[抗 HER2/neu]以双重组合方式同时应用，以确定它们共同唤起更高水平的抗肿瘤细胞毒性的能力。最后，对微管蛋白/微管抑制剂甲苯咪唑进行了评估，以确定它是否有潜力补充吉西他滨-(C4-酰胺)-[抗EGFR]与表柔比星-(C3-酰胺)-[抗HER2/neu]双重组合的抗肿瘤细胞毒性特性：结果：吉西他滨-(C4-酰胺)-[抗EGFR]与表柔比星-(C3-酰胺)-[抗HER2/neu]双重组合产生的抗肿瘤细胞毒性水平高于单独使用其中一种共价免疫化学治疗药物。苯并咪唑类微管/管蛋白抑制剂甲苯咪唑可补充吉西他滨-(C4-酰胺)-[抗EGFR]与表柔比星-(C3-酰胺)-[抗HER2/neu]双重组合的抗肿瘤细胞毒性：结论：吉西他滨-(C4-酰胺)-[抗 EGFR]与表柔比星-(C3-酰胺)-[抗 HER2/neu]的双重组合对具有化疗耐药性的乳腺腺癌（SKBr-3）产生的选择性 "靶向 "抗肿瘤细胞毒性高于单独使用其中一种共价免疫疗法。苯并咪唑类小管蛋白/微管抑制剂甲苯咪唑也对耐化疗的乳腺腺癌（SKBr-3）具有抗肿瘤细胞毒性，并补充了吉西他滨-(C4-酰胺)-[抗EGFR]与表柔比星-(C3-酰胺)-[抗HER2/neu]双重组合的效力和疗效。

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引用次数: 0

FOLFIRINOX in Advanced Pancreatic Cancer, NEMROCK Experience FOLFIRINOX用于晚期胰腺癌，NEMROCK经验

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2014-03-01 DOI: 10.13189/cor.2014.020302

Elghonemy E., Selim H., S. A, Shukur H.

引用次数: 0

Survival Outcome of Rhabdomyosarcoma (RMS) in Egyptian Children: Experience of the National Cancer Institute-Egypt 埃及儿童横纹肌肉瘤(RMS)的生存结局:埃及国家癌症研究所的经验

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2014-02-01 DOI: 10.13189/COR.2014.020202

M. Fawzy, M. Sedki, Hosam El Zomor, Hanaa M. Rashad, A. Mohamed, A. Nasr

Background. Survival rates of pediatric Rhabdomyosarcoma (RMS) have been tremendously improved during the last decade by the development of risk stratification. This has favored tailoring treatment using multi-therapeutic modalities. Methods. Upfront surgical resection was followed by systemic chemotherapy using Vincristine/Actinomycine-D/Cyclophosphamide (VAC) regimen with subsequent further local control by surgery and or radiotherapy according to risk stratification status. Results. Study included 40 patients; their median age was 3.5 years (range: 8 m to 17 yrs) with M/F: 28/12. The 2 years Overall Survival (OS) and Event Free Survival (EFS) for all study patients was 87% and 45% respectively. By univariate analysis, OS was 100% if CR (complete response) versus 92% if PR (partial response) (p=0.03), and was 94% if no distant metastasis versus 66% if present (p=0.024). On the other hand, EFS was 88% with CR versus 46% in PR patients (p <0.001), and was 80% if upfront surgery was done versus 33% if only simple biopsy taken (p=0.03). Local radiotherapy versus no radiotherapy was highly associated with EFS difference as well (75% versus 0%, respectively; p<0.001). In multivariate analysis, local radiotherapy found to be an independent prognostic factor of EFS (95% CI: 2.5-31). Conclusion. Disease extent as well as treatment response are two important factors influenced survival in our RMS patients. Local control measures including surgical resection as well as radiotherapy are crucial variables that predicted EFS. The poor outcome of patients with metastatic disease necessitates further therapeutic approaches.

背景。在过去的十年中，由于风险分层的发展，儿童横纹肌肉瘤(RMS)的生存率得到了极大的提高。这有利于采用多种治疗方式进行定制治疗。方法。术前手术切除后采用长春新碱/放线菌素- d /环磷酰胺(VAC)方案进行全身化疗，随后根据风险分层情况通过手术和/或放疗进一步进行局部控制。结果。研究纳入40例患者;年龄中位数为3.5岁(范围:8 - 17岁)，年龄比为28/12。所有研究患者的2年总生存率(OS)和无事件生存率(EFS)分别为87%和45%。通过单因素分析，CR(完全缓解)为100%，PR(部分缓解)为92% (p=0.03)，无远处转移为94%，存在远处转移为66% (p=0.024)。另一方面，CR患者的EFS为88%，PR患者为46% (p <0.001)，如果做了前期手术，EFS为80%，如果只做了简单的活检，EFS为33% (p=0.03)。局部放疗与非放疗也与EFS差异高度相关(分别为75%对0%;p < 0.001)。在多变量分析中，发现局部放疗是EFS的独立预后因素(95% CI: 2.5-31)。结论。疾病程度和治疗反应是影响RMS患者生存的两个重要因素。局部控制措施包括手术切除和放疗是预测EFS的关键变量。转移性疾病患者预后不佳，需要进一步的治疗方法。

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引用次数: 0

Prevalence of Risk Factors Related to Head and Neck Squamous Cell Carcinoma (HNSCC) Among College Students 大学生头颈部鳞状细胞癌(HNSCC)相关危险因素的流行

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2014-01-01 DOI: 10.13189/COR.2014.020102

Sloane C. Burke, Karen Smith, S. Sharmin, Cr Winkelman

The incidence of head and neck cancers among young individuals is increasing in the United States. Various sexual behaviors, heavy tobacco and alcohol use, HPV infection, and lack of HPV vaccination may increase the risk of head and neck cancer in the younger male population. The study was conducted to identify the risk factors for head and neck squamous cell cancers (HNSCC) among college students. A convenience sample of 1,685 students from an undergraduate health course was selected for the study. The self-reported, anonymous electronic questionnaire included items on the following risk factors: tobacco and alcohol use, HPV infection and/or presence of genital warts, oral hygiene, open-mouth kissing, and practice of various sexual behaviors. Statistical results showed that among college-aged males, the use of tobacco products and alcohol is much higher than females (P=0.000). Significance was also found between gender and sexual behaviors in one's lifetime and within the past 12 months (P=0.000). On average, males have higher numbers of vaginal and oral sex partners than females. In addition, males reported having twice the number of open-mouth kissing partners compared to their female counterparts (6 as opposed to 3). Importantly, the percentage of males who completed all three HPV vaccinations in the series is much lower (10.1%) than females (89.9%) which make them more vulnerable to HPV transmission, thus increasing the risk of HNSCC. College-aged males seem to be engaged in more high-risk activities related to HNSCC compared to their female counterparts. Integration of preventive public health strategies should be considered.

在美国，年轻人头颈癌的发病率正在上升。各种性行为、大量吸烟和饮酒、HPV感染以及缺乏HPV疫苗接种可能会增加年轻男性患头颈癌的风险。该研究旨在确定大学生头颈部鳞状细胞癌(HNSCC)的危险因素。本研究选取了1,685名本科健康课程学生作为方便样本。自我报告的匿名电子问卷包括以下风险因素:吸烟和饮酒、HPV感染和/或生殖器疣的存在、口腔卫生、张嘴接吻和各种性行为的实践。统计结果显示，在大学适龄男性中，烟草制品和酒精的使用远远高于女性(P=0.000)。性别与一生及过去12个月内的性行为也存在显著性差异(P=0.000)。平均而言，男性比女性拥有更多的阴道和口交性伴侣。此外，男性报告的张嘴接吻次数是女性的两倍(6对3)。重要的是，在这一系列中，完成所有三次HPV疫苗接种的男性比例(10.1%)远低于女性(89.9%)，这使得他们更容易感染HPV，从而增加了患HNSCC的风险。与女性相比，大学年龄的男性似乎参与了更多与HNSCC相关的高风险活动。应考虑整合预防性公共卫生战略。

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引用次数: 4

Multiple Functional Motifs Are Required for the Tumor Suppressor Activity of a Constitutively-Active ErbB4 Mutant 一个组成型活性ErbB4突变体的肿瘤抑制活性需要多个功能基序

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2013-08-22 DOI: 10.17303/JCRTO.2013.1.104

D. Riese, Richard M. Gallo, Ianthe N. Bryant, Christopher P. Mill, Steven Kaverman

ErbB4 (HER4) is a member of the ErbB family of receptor tyrosine kinases, which includes the Epidermal Growth Factor Receptor (EGFR/ErbB1), ErbB2 (HER2/Neu), and ErbB3 (HER3). Mounting evidence indicates that ErbB4, unlike EGFR or ErbB2, functions as a tumor suppressor in many human malignancies. Previous analyses of the constitutively-dimerized and –active ErbB4 Q646C mutant indicate that ErbB4 kinase activity and phosphorylation of ErbB4 Tyr1056 are both required for the tumor suppressor activity of this mutant in human breast, prostate, and pancreatic cancer cell lines. However, the cytoplasmic region of ErbB4 possesses additional putative functional motifs, and the contributions of these functional motifs to ErbB4 tumor suppressor activity have been largely underexplored. Here we demonstrate that ErbB4 BH3 and LXXLL motifs, which are thought to mediate interactions with Bcl family proteins and steroid hormone receptors, respectively, are required for the tumor suppressor activity of the ErbB4 Q646C mutant. Furthermore, abrogation of the site of ErbB4 cleavage by gamma-secretase also disrupts the tumor suppressor activity of the ErbB4 Q646C mutant. This last result suggests that ErbB4 cleavage and subcellular trafficking of the ErbB4 cytoplasmic domain may be required for the tumor suppressor activity of the ErbB4 Q646C mutant. Indeed, here we demonstrate that mutants that disrupt ErbB4 kinase activity, ErbB4 phosphorylation at Tyr1056, or ErbB4 cleavage by gamma-secretase also disrupt ErbB4 trafficking away from the plasma membrane and to the cytoplasm. This supports a model for ErbB4 function in which ErbB4 tumor suppressor activity is dependent on ErbB4 trafficking away from the plasma membrane and to the cytoplasm, mitochondria, and/or the nucleus.

ErbB4 (HER4)是ErbB受体酪氨酸激酶家族的一员，该家族包括表皮生长因子受体(EGFR/ErbB1)、ErbB2 (HER2/Neu)和ErbB3 (HER3)。越来越多的证据表明，与EGFR或ErbB2不同，ErbB4在许多人类恶性肿瘤中起肿瘤抑制作用。先前对组成二聚体和活性ErbB4 Q646C突变体的分析表明，ErbB4激酶活性和ErbB4 Tyr1056的磷酸化都是该突变体在人乳腺癌、前列腺癌和胰腺癌细胞系中抑制肿瘤活性所必需的。然而，ErbB4的细胞质区域具有其他假定的功能基序，并且这些功能基序对ErbB4肿瘤抑制活性的贡献在很大程度上尚未得到充分探索。在这里，我们证明ErbB4 BH3和LXXLL基序是ErbB4 Q646C突变体肿瘤抑制活性所必需的，它们被认为分别介导与Bcl家族蛋白和类固醇激素受体的相互作用。此外，γ -分泌酶去除ErbB4切割位点也会破坏ErbB4 Q646C突变体的抑瘤活性。最后的结果表明，ErbB4细胞质区域的分裂和亚细胞运输可能是ErbB4 Q646C突变体的肿瘤抑制活性所必需的。事实上，我们在这里证明了破坏ErbB4激酶活性、ErbB4 Tyr1056位点磷酸化或γ分泌酶切割ErbB4的突变体也会破坏ErbB4从质膜到细胞质的运输。这支持了一个ErbB4功能模型，其中ErbB4肿瘤抑制活性依赖于ErbB4从质膜转运到细胞质、线粒体和/或细胞核。

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引用次数: 0

Multiple Functional Motifs Are Required for the Tumor Suppressor Activity of a Constitutively-Active ErbB4 Mutant. 一个组成型活性ErbB4突变体的肿瘤抑制活性需要多个功能基序。

Journal of Cancer Research and Therapeutic Oncology

Pub Date : 2013-08-22

Richard M Gallo, Ianthe N Bryant, Christopher P Mill, Steven Kaverman, David J Riese

ErbB4 (HER4) is a member of the ErbB family of receptor tyrosine kinases, which includes the Epidermal Growth Factor Receptor (EGFR/ErbB1), ErbB2 (HER2/Neu), and ErbB3 (HER3). Mounting evidence indicates that ErbB4, unlike EGFR or ErbB2, functions as a tumor suppressor in many human malignancies. Previous analyses of the constitutively-dimerized and -active ErbB4 Q646C mutant indicate that ErbB4 kinase activity and phosphorylation of ErbB4 Tyr1056 are both required for the tumor suppressor activity of this mutant in human breast, prostate, and pancreatic cancer cell lines. However, the cytoplasmic region of ErbB4 possesses additional putative functional motifs, and the contributions of these functional motifs to ErbB4 tumor suppressor activity have been largely underexplored. Here we demonstrate that ErbB4 BH3 and LXXLL motifs, which are thought to mediate interactions with Bcl family proteins and steroid hormone receptors, respectively, are required for the tumor suppressor activity of the ErbB4 Q646C mutant. Furthermore, abrogation of the site of ErbB4 cleavage by gamma-secretase also disrupts the tumor suppressor activity of the ErbB4 Q646C mutant. This last result suggests that ErbB4 cleavage and subcellular trafficking of the ErbB4 cytoplasmic domain may be required for the tumor suppressor activity of the ErbB4 Q646C mutant. Indeed, here we demonstrate that mutants that disrupt ErbB4 kinase activity, ErbB4 phosphorylation at Tyr1056, or ErbB4 cleavage by gamma-secretase also disrupt ErbB4 trafficking away from the plasma membrane and to the cytoplasm. This supports a model for ErbB4 function in which ErbB4 tumor suppressor activity is dependent on ErbB4 trafficking away from the plasma membrane and to the cytoplasm, mitochondria, and/or the nucleus.

ErbB4 (HER4)是ErbB受体酪氨酸激酶家族的一员，该家族包括表皮生长因子受体(EGFR/ErbB1)、ErbB2 (HER2/Neu)和ErbB3 (HER3)。越来越多的证据表明，与EGFR或ErbB2不同，ErbB4在许多人类恶性肿瘤中起肿瘤抑制作用。先前对组成二聚体和活性ErbB4 Q646C突变体的分析表明，ErbB4激酶活性和ErbB4 Tyr1056的磷酸化都是该突变体在人乳腺癌、前列腺癌和胰腺癌细胞系中抑制肿瘤活性所必需的。然而，ErbB4的细胞质区域具有其他假定的功能基序，并且这些功能基序对ErbB4肿瘤抑制活性的贡献在很大程度上尚未得到充分探索。在这里，我们证明ErbB4 BH3和LXXLL基序是ErbB4 Q646C突变体肿瘤抑制活性所必需的，它们被认为分别介导与Bcl家族蛋白和类固醇激素受体的相互作用。此外，γ -分泌酶去除ErbB4切割位点也会破坏ErbB4 Q646C突变体的抑瘤活性。最后的结果表明，ErbB4细胞质区域的分裂和亚细胞运输可能是ErbB4 Q646C突变体的肿瘤抑制活性所必需的。事实上，我们在这里证明了破坏ErbB4激酶活性、ErbB4 Tyr1056位点磷酸化或γ分泌酶切割ErbB4的突变体也会破坏ErbB4从质膜到细胞质的运输。这支持了一个ErbB4功能模型，其中ErbB4肿瘤抑制活性依赖于ErbB4从质膜转运到细胞质、线粒体和/或细胞核。

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引用次数: 0