Riley Philip, Glenny Anne-Marie, Worthington Helen V, Littlewood Anne, Fernandez Mauleffinch Luisa M, Clarkson Jan E, McCabe Martin G
Cochrane Oral Health, Division of Dentistry, School of Medical Sciences, Faculty of Biology, Medicine and Health, The University of Manchester, JR Moore Building, Oxford Road, Manchester, UK, M13 9PL.
Cochrane Database Syst Rev. 2017 Nov 28;11(11):CD011990. doi: 10.1002/14651858.CD011990.pub2.
Oral mucositis is a side effect of chemotherapy, head and neck radiotherapy, and targeted therapy, affecting over 75% of high-risk patients. Ulceration can lead to severe pain and difficulty with eating and drinking, which may necessitate opioid analgesics, hospitalisation and supplemental nutrition. These complications may disrupt cancer therapy, which may reduce survival. There is also a risk of death from sepsis if pathogens enter the ulcers of immunocompromised patients. Ulcerative oral mucositis can be costly to healthcare systems, yet there are few preventive interventions proven to be beneficial. Cytokines and growth factors may help the regeneration of cells lining of the mouth, thus preventing or reducing oral mucositis and its negative effects.
To assess the effects of cytokines and growth factors for preventing oral mucositis in patients with cancer who are receiving treatment.
Cochrane Oral Health's Information Specialist searched the following databases: Cochrane Oral Health's Trials Register (searched 10 May 2017); the Cochrane Central Register of Controlled Trials (CENTRAL; 2017, Issue 4) in the Cochrane Library (searched 10 May 2017); MEDLINE Ovid (1946 to 10 May 2017); Embase Ovid (7 December 2015 to 10 May 2017); CINAHL EBSCO (Cumulative Index to Nursing and Allied Health Literature; 1937 to 10 May 2017); and CANCERLIT PubMed (1950 to 10 May 2017). The US National Institutes of Health Ongoing Trials Register (ClinicalTrials.gov) and the World Health Organization International Clinical Trials Registry Platform were searched for ongoing trials.
We included parallel-design randomised controlled trials (RCTs) assessing the effects of cytokines and growth factors in patients with cancer receiving treatment.
Two review authors independently screened the results of electronic searches, extracted data and assessed risk of bias. For dichotomous outcomes, we reported risk ratios (RR) and 95% confidence intervals (CI). For continuous outcomes, we reported mean differences (MD) and 95% CIs. We pooled similar studies in random-effects meta-analyses. We reported adverse effects in a narrative format.
We included 35 RCTs analysing 3102 participants. Thirteen studies were at low risk of bias, 12 studies were at unclear risk of bias, and 10 studies were at high risk of bias.Our main findings were regarding keratinocyte growth factor (KGF) and are summarised as follows.There might be a reduction in the risk of moderate to severe oral mucositis in adults receiving bone marrow/stem cell transplantation after conditioning therapy for haematological cancers (RR 0.89, 95% CI 0.80 to 0.99; 6 studies; 852 participants; low-quality evidence). We would need to treat 11 adults with KGF in order to prevent one additional adult from developing this outcome (95% CI 6 to 112). There might be a reduction in the risk of severe oral mucositis in this population, but there is also some possibility of an increase in risk (RR 0.85, 95% CI 0.65 to 1.11; 6 studies; 852 participants; low-quality evidence). We would need to treat 10 adults with KGF in order to prevent one additional adult from developing this outcome (95% CI 5 to prevent the outcome to 14 to cause the outcome).There is probably a reduction in the risk of moderate to severe oral mucositis in adults receiving radiotherapy to the head and neck with cisplatin or fluorouracil (RR 0.91, 95% CI 0.83 to 1.00; 3 studies; 471 participants; moderate-quality evidence). We would need to treat 12 adults with KGF in order to prevent one additional adult from developing this outcome (95% CI 7 to infinity). It is very likely that there is a reduction in the risk of severe oral mucositis in this population (RR 0.79, 95% CI 0.69 to 0.90; 3 studies; 471 participants; high-quality evidence). We would need to treat 7 adults with KGF in order to prevent one additional adult from developing this outcome (95% CI 5 to 15).It is likely that there is a reduction in the risk of moderate to severe oral mucositis in adults receiving chemotherapy alone for mixed solid and haematological cancers (RR 0.56, 95% CI 0.45 to 0.70; 4 studies; 344 participants; moderate-quality evidence). We would need to treat 4 adults with KGF in order to prevent one additional adult from developing this outcome (95% CI 3 to 6). There might be a reduction in the risk of severe oral mucositis in this population (RR 0.30, 95% CI 0.14 to 0.65; 3 studies; 263 participants; low -quality evidence). We would need to treat 10 adults with KGF in order to prevent one additional adult from developing this outcome (95% CI 8 to 19).Due to the low volume of evidence, single-study comparisons and insufficient sample sizes, we found no compelling evidence of a benefit for any other cytokines or growth factors and there was no evidence on children. There did not appear to be any serious adverse effects of any of the interventions assessed in this review.
AUTHORS' CONCLUSIONS: We are confident that KGF is beneficial in the prevention of oral mucositis in adults who are receiving: a) radiotherapy to the head and neck with cisplatin or fluorouracil; or b) chemotherapy alone for mixed solid and haematological cancers. We are less confident about a benefit for KGF in adults receiving bone marrow/stem cell transplant after conditioning therapy for haematological cancers because of multiple factors involved in that population, such as whether or not they received total body irradiation (TBI) and whether the transplant was autologous (the patients' own cells) or allogeneic (cells from a donor). KGF appears to be a relatively safe intervention.Due to limited research, we are not confident that there are any beneficial effects of other cytokines and growth factors. There is currently insufficient evidence to draw any conclusions about the use of cytokines and growth factors in children.
口腔黏膜炎是化疗、头颈部放疗及靶向治疗的一种副作用,影响超过75%的高危患者。溃疡会导致剧痛以及进食和饮水困难,这可能需要使用阿片类镇痛药、住院治疗及补充营养。这些并发症可能会干扰癌症治疗,进而可能降低生存率。如果病原体进入免疫功能低下患者的溃疡处,还存在因败血症而死亡的风险。溃疡性口腔黏膜炎会给医疗系统带来高昂成本,但几乎没有经证实有益的预防干预措施。细胞因子和生长因子可能有助于口腔黏膜细胞的再生,从而预防或减轻口腔黏膜炎及其负面影响。
评估细胞因子和生长因子对正在接受治疗的癌症患者预防口腔黏膜炎的效果。
Cochrane口腔健康信息专家检索了以下数据库:Cochrane口腔健康试验注册库(检索日期:2017年5月10日);Cochrane图书馆中的Cochrane对照试验中心注册库(CENTRAL;2017年第4期)(检索日期:2017年5月10日);MEDLINE Ovid(1946年至2017年5月10日);Embase Ovid(2015年12月7日至2017年5月10日);CINAHL EBSCO(护理学与健康相关文献累积索引;1937年至2017年5月10日);以及CANCERLIT PubMed(1950年至2017年5月10日)。检索了美国国立卫生研究院正在进行的试验注册库(ClinicalTrials.gov)和世界卫生组织国际临床试验注册平台以查找正在进行的试验。
我们纳入了评估细胞因子和生长因子对正在接受治疗的癌症患者效果的平行设计随机对照试验(RCT)。
两位综述作者独立筛选电子检索结果、提取数据并评估偏倚风险。对于二分法结局,我们报告风险比(RR)和95%置信区间(CI)。对于连续性结局,我们报告平均差(MD)和95% CI。我们在随机效应荟萃分析中合并了相似的研究。我们以叙述形式报告不良反应。
我们纳入了35项RCT,分析了3102名参与者。13项研究偏倚风险低,12项研究偏倚风险不明确,10项研究偏倚风险高。我们的主要发现涉及角质形成细胞生长因子(KGF),总结如下:接受血液系统癌症预处理治疗后进行骨髓/干细胞移植的成年人中,中重度口腔黏膜炎的风险可能降低(RR 0.89,95% CI:0.80至0.99;6项研究;852名参与者;低质量证据)。为预防1例额外的成年人出现此结局,我们需要用KGF治疗11名成年人(95% CI:6至112)。该人群中严重口腔黏膜炎的风险可能降低,但也有风险增加的可能性(RR 0.85,95% CI:0.65至1.11;6项研究;852名参与者;低质量证据)。为预防1例额外的成年人出现此结局,我们需要用KGF治疗10名成年人(95% CI:5例预防此结局至14例导致此结局)。接受顺铂或氟尿嘧啶进行头颈部放疗的成年人中,中重度口腔黏膜炎的风险可能降低(RR 0.91,95% CI:0.83至1.00;3项研究;471名参与者;中等质量证据)。为预防1例额外的成年人出现此结局,我们需要用KGF治疗12名成年人(95% CI:7至无穷大)。该人群中严重口腔黏膜炎的风险很可能降低(RR 0.79,95% CI:0.69至0.90;3项研究;471名参与者;高质量证据)。为预防1例额外的成年人出现此结局,我们需要用KGF治疗7名成年人(95% CI:5至15)。单独接受化疗的实体和血液系统混合癌症成年人中,中重度口腔黏膜炎的风险可能降低(RR 0.56,95% CI:0.45至0.70;4项研究;344名参与者;中等质量证据)。为预防1例额外的成年人出现此结局,我们需要用KGF治疗4名成年人(95% CI:3至6)。该人群中严重口腔黏膜炎的风险可能降低(RR 0.30,95% CI:0.14至0.65;3项研究;263名参与者;低质量证据)。为预防1例额外的成年人出现此结局,我们需要用KGF治疗10名成年人(95% CI:8至19)。由于证据量少、单研究比较及样本量不足,我们未发现任何其他细胞因子或生长因子有益的有力证据,且没有关于儿童的证据。本综述评估的任何干预措施似乎均未出现任何严重不良反应。
我们确信,KGF对正在接受以下治疗的成年人预防口腔黏膜炎有益:a)用顺铂或氟尿嘧啶进行头颈部放疗;或b)单独接受化疗的实体和血液系统混合癌症。对于接受血液系统癌症预处理治疗后进行骨髓/干细胞移植的成年人,我们对KGF的益处信心不足,因为该人群涉及多种因素,如是否接受全身照射(TBI)以及移植是自体(患者自身细胞)还是异体(供体细胞)。KGF似乎是一种相对安全的干预措施。由于研究有限,我们不确定其他细胞因子和生长因子是否有任何有益效果。目前没有足够证据就细胞因子和生长因子在儿童中的应用得出任何结论。
