Conventional chemotherapy

常规化疗
  • 文章类型: Journal Article
    节制化学疗法是指以较低剂量频繁施用化学治疗剂,并以令人鼓舞的反应率提供了常规化学疗法的有吸引力的替代方案。然而,治疗的时间表,包括药物的剂量,通常基于经验主义。肿瘤-内皮-免疫相互作用在药物节律给药过程中的混杂效应尚未被详细探讨。导致对药物剂量和频率评估的评估不完整。本研究旨在使用数学模型对节拍化疗的不同作用进行机械理解。我们已经建立了一种分析条件,用于确定药物的剂量和频率,这取决于其完全消除肿瘤的清除率。该模型还提出了在化学治疗剂的节拍给药期间免疫介导的肿瘤清除。全局敏感性分析的结果表明,在节拍计划期间,药物和免疫介导的杀伤因子对肿瘤人群的敏感性增加。我们的结果强调了最大耐受剂量(MTD)的节拍计划,并定义了一种基于模型的方法,用于近似最佳的药物给药计划,以消除肿瘤,同时最大程度地减少对免疫细胞和患者身体的伤害。
    Metronomic chemotherapy refers to the frequent administration of chemotherapeutic agents at a lower dose and presents an attractive alternative to conventional chemotherapy with encouraging response rates. However, the schedule of the therapy, including the dosage of the drug, is usually based on empiricism. The confounding effects of tumor-endothelial-immune interactions during metronomic administration of drugs have not yet been explored in detail, resulting in an incomplete assessment of drug dose and frequency evaluations. The present study aimed to gain a mechanistic understanding of different actions of metronomic chemotherapy using a mathematical model. We have established an analytical condition for determining the dosage and frequency of the drug depending on its clearance rate for complete tumor elimination. The model also brings forward the immune-mediated clearance of the tumor during the metronomic administration of the chemotherapeutic agent. The results from the global sensitivity analysis showed an increase in the sensitivity of drug and immune-mediated killing factors toward the tumor population during metronomic scheduling. Our results emphasize metronomic scheduling over the maximum tolerated dose (MTD) and define a model-based approach for approximating the optimal schedule of drug administration to eliminate tumors while minimizing harm to the immune cells and the patient\'s body.
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  • 文章类型: Journal Article
    由于其高死亡率,癌症代表了重大的全球健康和经济负担。虽然在某些情况下有效,传统化疗往往不能完全根除各种癌症。由于对健康细胞的伤害,它可能会引起严重的副作用。两种治疗方法已经上升到解决这些限制的最前沿:节拍化疗(MCT)和药物再利用。节制化疗是一种创新的方法,打破了传统模式。它涉及低剂量的化疗方案,没有以前是这种治疗标志的长期无药间隔。该方法提供了副作用的显著降低和改善的疾病管理。同时,药物再利用在癌症治疗中获得了相当大的吸引力。这种方法涉及利用现有药物,最初开发用于其他治疗目的,作为潜在的癌症治疗方法。由于预先存在的安全性和剂量数据,已知药物在新环境中的应用加速了从实验室到患者的时间表。这两种策略的交集产生了一种名为“Metronomics”的新颖治疗方法。这种方法囊括了MCT和药物再利用的好处,导致毒性降低,口服给药的潜力,改善患者生活质量,加快临床实施,和增强的负担能力。许多临床研究已经认可了节拍化疗的疗效,具有可耐受的副作用,强调了Metronomics在更好的癌症管理中的潜力,特别是在低收入和中等收入国家。这篇综述强调了节拍化疗和药物再利用的益处和应用。特别是在乳腺癌的背景下,展示临床前和临床研究的有希望的结果。然而,我们承认有必要进行额外的临床研究,以明确确定节拍化疗与其他治疗方法在癌症综合治疗中的作用.
    Cancer represents a significant global health and economic burden due to its high mortality rates. While effective in some instances, traditional chemotherapy often falls short of entirely eradicating various types of cancer. It can cause severe side effects due to harm to healthy cells. Two therapeutic approaches have risen to the forefront to address these limitations: metronomic chemotherapy (MCT) and drug repurposing. Metronomic chemotherapy is an innovative approach that breaks from traditional models. It involves the administration of chemotherapeutic regimens at lower doses, without long drug-free intervals that have previously been a hallmark of such treatments. This method offers a significant reduction in side effects and improved disease management. Simultaneously, drug repurposing has gained considerable attraction in cancer treatment. This approach involves utilizing existing drugs, initially developed for other therapeutic purposes, as potential cancer treatments. The application of known drugs in a new context accelerates the timeline from laboratory to patient due to pre-existing safety and dosage data. The intersection of these two strategies gives rise to a novel therapeutic approach named \'Metronomics.\' This approach encapsulates the benefits of both MCT and drug repurposing, leading to reduced toxicity, potential for oral administration, improved patient quality of life, accelerated clinical implementation, and enhanced affordability. Numerous clinical studies have endorsed the efficacy of metronomic chemotherapy with tolerable side effects, underlining the potential of Metronomics in better cancer management, particularly in low- and middle-income countries. This review underscores the benefits and applications of metronomic chemotherapy and drug repurposing, specifically in the context of breast cancer, showcasing the promising results of pre-clinical and clinical studies. However, we acknowledge the necessity of additional clinical investigations to definitively establish the role of metronomic chemotherapy in conjunction with other treatments in comprehensive cancer management.
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  • 文章类型: Journal Article
    背景:化疗是妊娠滋养细胞肿瘤(GTN)的推荐治疗方法。提倡第二次刮治,以避免不必要的化疗和减少化疗的疗程;然而,尚未达成共识,因为有论点声称它无法诱导完全回归。
    目的:本研究旨在阐明第二次刮宫术对避免不必要的化疗和减少后磨牙GTN患者化疗疗程的有效性。
    方法:搜索了七个主要的电子数据库,包括四个英文数据库和三个中文数据库,从每个数据库开始到2023年1月31日。
    方法:如果研究是:(1)人类,(2)明确表示暴露于第二次刮宫,(3)明确表示控制常规化疗,(4)明确表示参与者是妊娠滋养细胞肿瘤(GTN)患者,和(5)将感兴趣的结果作为化疗疗程的数量进行比较。
    方法:两位作者独立提取和分析数据。第三作者通过审查全文来调和分歧。研究地点的数据,数据收集,研究设计,参与人数,干预策略,控制策略,后续阶段,结果,对不良事件进行分析.
    结果:关于避免不必要的化疗,与常规化疗组相比,第二次刮宫组的总体合并效应大小具有显著优势,OR为0.02(95%CI:0.00~0.06).同时,为了减少化疗疗程的数量,与常规化疗组相比,第二次刮宫组的总体合并效应大小具有显著优势,平均差异为-2.11(95%CI:-3.72~-0.51).
    结论:第二刮宫组在避免不必要的化疗和减少化疗疗程数上比常规化疗组有显著优势。应进行更多更大的多中心随机对照试验,以证实我们的结果,并明确磨牙后GTN患者第二次刮治的最佳患者组。
    BACKGROUND: Chemotherapy is the recommended treatment for gestational trophoblastic neoplasia (GTN). Second curettage had been advocated to avoid unnecessary chemotherapy and to reduce the courses of chemotherapy; however, consensus has not been reached as there are arguments claiming its inability of inducing complete regression.
    OBJECTIVE: The present study was performed to clarify the effectiveness of second curettage for avoiding unnecessary chemotherapy and lowering the number of chemotherapy courses in patients with post-molar GTN.
    METHODS: Seven predominant electronic databases were searched, including four English databases and three Chinese databases, from the inception of each database until January 31, 2023.
    METHODS: Studies were included if they were: (1) human, (2) explicitly indicated exposure to second curettage, (3) explicitly indicated control to conventional chemotherapy, (4) explicitly indicated the participants were patients with gestational trophoblastic neoplasia (GTN), and (5) compared the outcome of interest as the number of the course of chemotherapy.
    METHODS: Two authors extracted and analyzed the data independently. Disagreements were reconciled by reviewing the full text by a third author. The data of study location, data collection, study design, number of participants, intervention strategy, control strategy, the follow-up period, outcome, adverse events were analyzed.
    RESULTS: With regard to avoiding unnecessary chemotherapy, the overall pooled effect size of the second curettage group had a significant advantage over the conventional chemotherapy group with an OR of 0.02 (95% CI: 0.00-0.06). Meanwhile, for reducing the number of chemotherapy courses, the overall pooled effect size of the second curettage group had significant advantage over the conventional chemotherapy group with a mean difference of -2.11 (95% CI: -3.72 to -0.51).
    CONCLUSIONS: The second curettage group had a significant advantage over the conventional chemotherapy group in avoiding unnecessary chemotherapy and reducing the number of chemotherapy courses. Further larger multi-center randomized controlled trials should be conducted to confirm our results and to clarify the optimal patients\' group for second curettage in patients with post-molar GTN.
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  • 文章类型: Journal Article
    细胞毒性化疗仍然是癌症治疗的关键方式。这些疗法,成功使用了几十年,每天继续改变癌症患者的生活。随着当前肿瘤药物开发的高流失率,再加上大多数新疗法不能取代标准治疗,许多医疗保健系统负担不起这些新疗法的知识;细胞毒性化疗将在未来许多年仍然是癌症治疗的重要组成部分。这些疗法的临床价值通常在临床前癌症研究社区中被低估。这种不同类型的药物通常被归类为非特异性细胞毒物,仅根据增殖率杀死肿瘤细胞;然而,这是不准确的。这篇综述文章旨在重申将研究工作重点放在提高我们对这些药物如何起作用的基本理解上的重要性。讨论它们靶向癌细胞中泛必需途径的能力,这与化疗窗口的关系,并强调可用于完善其用途的基础科学方法。
    Cytotoxic chemotherapy remains a key modality in cancer treatment. These therapies, successfully used for decades, continue to transform the lives of cancer patients daily. With the high attrition rate of current oncology drug development, combined with the knowledge that most new therapies do not displace standard-of-care treatments and that many healthcare systems cannot afford these new therapies; cytotoxic chemotherapies will remain an important component of cancer therapy for many years to come. The clinical value of these therapies is often under-appreciated within the pre-clinical cancer research community, where this diverse class of agents are often grouped together as non-specific cellular poisons killing tumor cells based solely upon proliferation rate; however, this is inaccurate. This review article seeks to reaffirm the importance of focusing research efforts upon improving our basic understanding of how these drugs work, discussing their ability to target pan-essential pathways in cancer cells, the relationship of this to the chemotherapeutic window, and highlighting basic science approaches that can be employed towards refining their use.
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  • 文章类型: Journal Article
    血栓性微血管病(TMA)代表了内皮和足细胞生物学的复杂相互作用,肾单位生理学,补充遗传学,和肿瘤治疗与宿主免疫学。各种因素的复杂性,如分子原因,基因表达,和免疫系统模仿,还有不完整的外显率,很难找到一个简单的解决方案。因此,诊断可能会有所不同,study,和治疗方法,达成共识可能具有挑战性。这里,我们回顾了分子生物学,药理学,免疫学,分子遗传学,以及癌症背景下各种TMA综合征的病理学。在病因学上有争议,命名法,以及需要进一步临床治疗的点,翻译,并讨论了实验室研究。补体介导的TMA,化疗药物介导的TMA,单克隆丙种球蛋白病中的TMAs,和其他TMA中心的健康实践进行了详细的审查。此外,随后讨论了美国食品和药物管理局管道内已建立和新兴的疗法。最后,对临床医师和非典型溶血性尿毒综合征研究人员的研究种子进行了全面的回顾,对临床医师和研究种子具有实用价值。
    Thrombotic microangiopathies (TMAs) represent a complex interaction of endothelial and podocyte biology, nephron physiology, complement genetics, and oncologic therapies with host immunology. The complexity of various factors, such as molecular causes, genetic expressions, and immune system mimicking, along with incomplete penetrance, make it difficult to find a straightforward solution. As a result, there may be variations in diagnosis, study, and treatment approaches, and achieving a consensus can be challenging. Here, we review the molecular biology, pharmacology, immunology, molecular genetics, and pathology of the various TMA syndromes in the setting of cancer. Controversies in etiology, nomenclature, and points requiring further clinical, translational, and bench research are discussed. Complement-mediated TMAs, chemotherapy drug-mediated TMAs, TMAs in monoclonal gammopathy, and other TMAs central to onconephrology practice are reviewed in detail. In addition, established and emerging therapies within the US Food and Drug Administration pipeline subsequently are discussed. Finally, a comprehensive review of critical areas of onconephrology clinical practice is presented as practical value to the clinical practitioner and seeds of investigation to be sown among the community of atypical hemolytic uremic syndrome researchers.
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  • 文章类型: Journal Article
    背景:胃癌是全球最常见的癌症之一,5年生存率仅为20%。胃癌的发病年龄符合癌症的一般规律。大多数发生在中年以后,大多在40到60岁之间,平均年龄约50岁,只有5%的患者年龄在30岁以下。男性发病率高于女性。
    目的:探讨化疗联合伊立替康治疗晚期胃癌的近期疗效及影响因素。
    方法:选取我院2019年1月至2022年1月收治的晚期胃癌患者80例。采用信封法将患者分为观察组(n=40)和对照组(n=40)。对照组给予术前常规化疗。观察组在对照组化疗的基础上给予伊立替康治疗。两组治疗的近期疗效,以及治疗前后的肿瘤标志物水平和生活质量进行评价。
    结果:观察组近期治疗效果优于对照组(P<0.05)。总有效率为57.50%。观察组化疗无效的肿瘤淋巴结转移(TNM)IV期患者的年龄和比例分别为(65.12±5.71)岁和52.94%,分别,显著高于化疗有效患者(P<0.05),Karnofsky绩效量表得分为(67.70±3.83)分,明显低于化疗有效患者(P<0.05)。经过3个月的治疗,SF-36量表的生理功能评分,能源,情感功能,观察组心理健康分别为65.12±8.14、54.76±6.70、47.58±7.22和66.16±8.11分,分别,显著高于对照组(P<0.05)。观察组III-IV级腹泻和III-IV级血小板减少发生率分别为32.50%和25.00%,分别,显著高于对照组(P<0.05)。
    结论:化疗联合伊立替康治疗晚期胃癌近期疗效较好,可显著降低患者血清肿瘤标志物水平,提高患者生活质量。疗效可能受患者年龄和TNM分期的影响,其长期疗效有待进一步研究。
    BACKGROUND: Gastric cancer is one of the most common cancers worldwide, with a 5-year survival rate of only 20%. The age of onset of gastric cancer is in line with the general rule of cancer. Most of them occur after middle age, mostly between 40 and 60 years old, with an average age of about 50 years old, and only 5% of patients are under 30 years old. The incidence of male is higher than that of female.
    OBJECTIVE: To investigate the short-term efficacy and influencing factors of chemotherapy combined with irinotecan in patients with advanced gastric cancer.
    METHODS: Eighty patients with advanced gastric cancer who were treated in our hospital from January 2019 to January 2022 were selected. The patients were divided into an observation group (n = 40) and control group (n = 40) by the envelope method. The control group was given preoperative routine chemotherapy. The observation group was treated with irinotecan in addition to the chemotherapy given to the control group. The short-term efficacy of treatment in the two groups, as well as tumor marker levels and quality of life before and after treatment were evaluated.
    RESULTS: The short-term treatment effect in the observation group was better than that in the control group (P < 0.05), and the total effective rate was 57.50%. The age and proportion of tumor node metastasis (TNM) stage IV patients with ineffective chemotherapy in the observation group were (65.12 ± 5.71) years and 52.94%, respectively, which were notably higher than those of patients with effective chemotherapy (P < 0.05), while the Karnofsky Performance Scale score was (67.70 ± 3.83) points, which was apparently lower than that of patients with effective chemotherapy (P < 0.05). After 3 mo of treatment, the SF-36 scale scores of physiological function, energy, emotional function, and mental health in the observation group were 65.12 ± 8.14, 54.76 ± 6.70, 47.58 ± 7.22, and 66.16 ± 8.11 points, respectively, which were considerably higher than those in the control group (P < 0.05). The incidence rates of grade III-IV diarrhea and grade III-IV thrombocytopenia in the observation group were 32.50% and 25.00%, respectively, which were markedly higher than those in the control group (P < 0.05).
    CONCLUSIONS: Chemotherapy combined with irinotecan in patients with advanced gastric cancer has a good short-term efficacy and can significantly reduce serum tumor markers and improve the quality of life of patients. The efficacy may be affected by the age and TNM stage of the patients, and its long-term efficacy needs further study.
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  • 文章类型: Journal Article
    视网膜母细胞瘤是一种罕见的,有时是遗传性的,儿科癌症。在高收入国家,这种疾病的存活率接近100%,而在低收入和中等收入国家,约80%的病例的预后是致命的。根据疾病的阶段,采用不同的治疗方案。在更晚期的疾病中,手术切除整个眼球及其眼内内容物(摘除)是,不幸的是,必要的,而在其他情况下,通常使用常规化疗。为了克服传统化疗药物的副作用和疗效降低,最近已经开发了确保药物持续释放并管理到达目标部位的纳米递送系统。这篇综述考虑了纳米药物在治疗视网膜母细胞瘤中的当前用途和进展,并讨论了包含常规药物和天然产物的纳米颗粒制剂。此外,讨论了视网膜母细胞瘤治疗的未来发展。
    Retinoblastoma is a rare, sometimes hereditary, pediatric cancer. In high-income countries this disease has a survival rate approaching 100%, while in low- and middle-income countries the prognosis is fatal for about 80% of cases. Depending on the stage of the disease, different therapeutic protocols are applied. In more advanced forms of the disease, surgical removal of the entire globe and its intraocular contents (enucleation) is, unfortunately, necessary, whereas in other cases, conventional chemotherapy is normally used. To overcome the side-effects and reduced efficacy of traditional chemotherapic drugs, nanodelivery systems that ensure a sustained drug release and manage to reach the target site have more recently been developed. This review takes into account the current use and advances of nanomedicine in the treatment of retinoblastoma and discusses nanoparticulate formulations that contain conventional drugs and natural products. In addition, future developments in retinoblastoma treatment are discussed.
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  • 文章类型: Case Reports
    一名52岁的快速进行性截瘫患者出现椎旁肿瘤。行椎板切除术伴肿瘤切除,肿瘤的病理分析显示,间变性浆细胞样细胞紧密增殖。肿瘤的G带分析显示了复杂的核型,包括IgH/MYC易位。患者被诊断为MYC排列的间变性多发性骨髓瘤(AMM),细胞毒性化疗和自体造血干细胞移植导致长期无病缓解。这是第一份描述MYC重排的从头AMM病例的报告,这表明常规化疗可能是这种可怕疾病的治疗选择。
    A 52-year-old man with rapidly progressive paraplegia was presented to us with paravertebral tumors. Laminectomy with tumor resection was performed, and pathological analysis of the tumor revealed compact proliferation of anaplastic plasmacytoid cells. G-band analysis of the tumor revealed a complex karyotype, including IgH/MYC translocation. The patient was diagnosed with anaplastic multiple myeloma (AMM) with MYC arrangement, and cytotoxic chemotherapy followed by autologous hematopoietic stem cell transplantation resulted in long-term disease-free remission. This is the first report describing a case of de novo AMM with MYC rearrangement, suggesting that conventional chemotherapy could be a treatment option for this formidable disease.
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  • 文章类型: Journal Article
    Since patients with acute myeloid leukemia (AML) in the real world have a much different clinical picture than patients recruited in the clinical trials, obtaining real-world evidence of medication adoption is important for therapeutic efficiency and safety. This study used three population-based data in Taiwan, the National Health Insurance Research Database, Taiwan Cancer Registry, and National Death Registry, between 2001 and 2015, to investigate the effect of conventional chemotherapy (CCT) versus non-conventional chemotherapy (NCCT) on the overall survival (OS) of patients with AML (n = 7,763). Cox proportional hazard regression was used to estimate the hazard ratios (HR) of different treatments on the risk of mortality. To reduce the potential selection bias, we used the inverse probability of treatment weighting based on the propensity score to balance the baseline characteristics between patients receiving CCT and NCCT. The median survival time for CCT and NCCT arms was 10.2 months (95% confidence interval (95% CI): 9.7-10.9) and 4.1 months (95% CI: 3.8-4.5), respectively. Compared to the patients received NCCT, those receiving CCT had a lower risk of mortality (HR 0.63 (95% CI: 0.59-0.67, P < 0.001). Subgroup analysis showed that CCT did benefit patients in different gender, age, comorbidity, and socioeconomic status (SES) groups. In conclusion, the real-world population-based data exhibited CCT were more likely to be prescribed for patients with AML of younger age, fewer comorbidities, diagnosed recently (2011-2015), and higher SES. In fact, CCT had better treatment outcomes than NCCT in terms of OS for adult patients diagnosed with AML.
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  • 文章类型: Journal Article
    In gastric cancer (GC), biomarkers that define prognosis and predict treatment response remain scarce. We hypothesized that the extent of CD44v6 membranous tumor expression could predict prognosis and therapy response in GC patients. Two GC surgical cohorts, from Portugal and South Korea (n = 964), were characterized for the extension of CD44v6 membranous immuno-expression, clinicopathological features, patient survival, and therapy response. The value of CD44v6 expression in predicting response to treatment and its impact on prognosis was determined. High CD44v6 expression was associated with invasive features (perineural invasion and depth of invasion) in both cohorts and with worse survival in the Portuguese GC cohort (HR 1.461; 95% confidence interval 1.002-2.131). Patients with high CD44v6 tumor expression benefited from conventional chemotherapy in addition to surgery (p < 0.05), particularly those with heterogeneous CD44v6-positive and -negative populations (CD44v6_3+) (p < 0.007 and p < 0.009). Our study is the first to identify CD44v6 high membranous expression as a potential predictive marker of response to conventional treatment, but it does not clarify CD44v6 prognostic value in GC. Importantly, our data support selection of GC patients with high CD44v6-expressing tumors for conventional chemotherapy in addition to surgery. These findings will allow better stratification of GC patients for treatment, potentially improving their overall survival.
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