James Wyatt, Sean M Fernando, Simon George Powell, Christopher J Hill, Ilyas Arshad, Chris Probert, Shakil Ahmed, Dharani K Hapangama
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The evidence base is large, but no comprehensive reviews exist to summarize our understanding and highlight the overarching themes to further our understanding and suggest future directions of study for the field.</p><p><strong>Study design size duration: </strong>This systematic review with a thematic analysis retrieved studies from the PubMed, Embase, Web of Science, and Cochrane Library databases and searches were conducted from inception through to August 2022. Human and animal studies published in the English language were included and identified using a combination of exploded MeSH terms ('Iron' and 'Endometriosis') and free-text search terms ('Iron', 'Ferric', 'Ferrous', 'Endometriosis', 'Endometrioma').</p><p><strong>Participants/materials setting methods: </strong>This review was reported in accordance with the PRISMA guidelines. All studies reporting original data concerning the role of iron or iron complexes in the pathophysiology of endometriosis were included. Studies that did not report original data or provided a review of the field were excluded. Bias analysis was completed for each included study by using the Newcastle-Ottawa scoring system.</p><p><strong>Main results and the role of chance: </strong>There were 776 records identified and these were screened down to 53 studies which met the eligibility criteria, including 6 animal and 47 human studies, with 3556 individual participants. Iron excess is demonstrated in various tissues and fluids, including ovarian endometriomas, ovarian follicles, ectopic endometriotic lesions, and peritoneal fluid. Markers of oxidative stress are strongly associated with high iron levels, and aberrant expression of iron-transport proteins has been demonstrated. Abnormal resistance to ferroptosis is likely. Iron-mediated oxidative stress is responsible for a pro-inflammatory micro-environment and is linked to subfertility, symptom severity, and, possibly, malignant transformation.</p><p><strong>Limitations reasons for caution: </strong>A minority of the included studies were of objectively low quality with a high risk of bias and may lead to misleading conclusions. Additionally, multiple studies failed to appropriately characterize the included patients by known confounding variables, such as menstrual cycle phase, which may introduce bias to the findings.</p><p><strong>Wider implications of the findings: </strong>Current literature depicts a central role of aberrant iron mechanics and subsequent oxidative stress in endometriosis. It is likely that iron excess is at least partly responsible for the persistence and proliferation of ectopic endometriotic lesions. As such, iron mechanics represent an attractive target for novel therapeutics, including iron chelators or effectors of the iron-oxidative stress pathway. There are significant gaps in our current understanding, and this review highlights and recommends several topics for further research. These include the role of iron chelation, resistance to ferroptosis, the relationship between iron excess and localized hypoxia, systemic iron pathophysiology in endometriosis, and the role of oxidative stress in malignant transformation.</p><p><strong>Study funding/competing interests: </strong>J.W. and S.G.P. are supported by clinical fellowships at Liverpool University Hospital NHS Foundation trust. No additional funding was requested or required for the completion of this work. C.J.H. is supported by a Wellbeing of Women project grant (RG2137). D.K.H. is supported by a Wellbeing of Women project grant (RG2137) and an MRC clinical research training fellowship (MR/V007238/1). The authors have no conflicts of interest to declare.</p><p><strong>Registration number: </strong>A protocol was prospectively registered with the PROSPERO database in August 2021 (CRD42021272818).</p>","PeriodicalId":73264,"journal":{"name":"Human reproduction open","volume":"2023 3","pages":"hoad033"},"PeriodicalIF":8.3000,"publicationDate":"2023-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10457727/pdf/","citationCount":"2","resultStr":"{\"title\":\"The role of iron in the pathogenesis of endometriosis: a systematic review.\",\"authors\":\"James Wyatt, Sean M Fernando, Simon George Powell, Christopher J Hill, Ilyas Arshad, Chris Probert, Shakil Ahmed, Dharani K Hapangama\",\"doi\":\"10.1093/hropen/hoad033\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Study question: </strong>What is the role of iron in the pathophysiology of endometriosis?</p><p><strong>Summary answer: </strong>Iron excess is demonstrated wherever endometriotic tissues are found and is associated with oxidative stress, an inflammatory micro-environment, and cell damage; the iron-mediated oxidative stress is independently linked to subfertility, symptom severity, and malignant transformation.</p><p><strong>What is known already: </strong>Iron is found in excess in endometriotic tissues, and multiple mechanisms have been studied and posited to explain this. 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引用次数: 2
摘要
研究问题:铁在子宫内膜异位症病理生理中的作用是什么?总结回答:无论子宫内膜异位症组织在哪里,铁含量都会过量,并与氧化应激、炎症微环境和细胞损伤有关;铁介导的氧化应激与低生育能力、症状严重程度和恶性转化独立相关。已知情况:在子宫内膜异位症组织中发现了过量的铁,已经研究并提出了多种机制来解释这一点。很明显,铁过量在促进氧化应激和细胞损伤中起着至关重要的作用。证据基础很大,但没有全面的综述来总结我们的理解,并强调总体主题,以进一步我们的理解,并为该领域的未来研究方向提出建议。研究设计规模持续时间:本系统综述采用专题分析,检索了PubMed、Embase、Web of Science和Cochrane图书馆数据库的研究,检索时间从开始到2022年8月。用英语发表的人类和动物研究被包括在内,并使用爆炸MeSH术语(“铁”和“子宫内膜异位症”)和自由文本搜索术语(“铁”、“铁”、“铁”、“子宫内膜异位症”、“子宫内膜异位症”)的组合进行识别。受试者/材料设置方法:本综述按照PRISMA指南报道。所有报道铁或铁复合物在子宫内膜异位症病理生理作用的原始数据的研究都被纳入。未报告原始数据或未提供该领域综述的研究被排除在外。采用纽卡斯尔-渥太华评分系统对每个纳入的研究进行偏倚分析。主要结果和偶然性的作用:共有776条记录被确定,这些记录被筛选到53项符合资格标准的研究,包括6项动物研究和47项人类研究,共有3556名个体参与者。铁过量存在于多种组织和液体中,包括卵巢子宫内膜异位症、卵巢卵泡、异位子宫内膜病变和腹膜液。氧化应激标志物与高铁水平密切相关,铁转运蛋白的异常表达已被证实。对铁下垂的异常抵抗是可能的。铁介导的氧化应激负责促炎微环境,与生育能力低下、症状严重以及可能的恶性转化有关。局限性:少数纳入的研究客观上质量较低,存在高偏倚风险,可能导致误导性结论。此外,多项研究未能通过已知的混杂变量(如月经周期)适当地描述纳入的患者,这可能会对研究结果产生偏倚。研究结果的更广泛意义:目前的文献描述了异常铁力学和随后的氧化应激在子宫内膜异位症中的核心作用。这可能是铁过量至少部分负责的持续和增殖异位子宫内膜病变。因此,铁力学代表了一个有吸引力的新治疗靶点,包括铁螯合剂或铁氧化应激途径的效应器。在我们目前的理解中存在显著的差距,这篇综述强调并推荐了几个进一步研究的主题。这些包括铁螯合的作用,对铁下沉的抵抗,铁过量与局部缺氧的关系,子宫内膜异位症的全身铁病理生理,以及氧化应激在恶性转化中的作用。研究资金/竞争利益:J.W.和S.G.P.由利物浦大学医院NHS基金会信托的临床奖学金支持。没有为完成这项工作要求或需要额外的经费。C.J.H.得到了妇女福利项目补助金(RG2137)的支持。D.K.H.由妇女福利项目资助(RG2137)和MRC临床研究培训奖学金(MR/V007238/1)支持。作者无利益冲突需要申报。注册编号:该协议已于2021年8月在PROSPERO数据库中前瞻性注册(CRD42021272818)。
The role of iron in the pathogenesis of endometriosis: a systematic review.
Study question: What is the role of iron in the pathophysiology of endometriosis?
Summary answer: Iron excess is demonstrated wherever endometriotic tissues are found and is associated with oxidative stress, an inflammatory micro-environment, and cell damage; the iron-mediated oxidative stress is independently linked to subfertility, symptom severity, and malignant transformation.
What is known already: Iron is found in excess in endometriotic tissues, and multiple mechanisms have been studied and posited to explain this. It is clear that iron excess plays a vital role in promoting oxidative stress and cell damage. The evidence base is large, but no comprehensive reviews exist to summarize our understanding and highlight the overarching themes to further our understanding and suggest future directions of study for the field.
Study design size duration: This systematic review with a thematic analysis retrieved studies from the PubMed, Embase, Web of Science, and Cochrane Library databases and searches were conducted from inception through to August 2022. Human and animal studies published in the English language were included and identified using a combination of exploded MeSH terms ('Iron' and 'Endometriosis') and free-text search terms ('Iron', 'Ferric', 'Ferrous', 'Endometriosis', 'Endometrioma').
Participants/materials setting methods: This review was reported in accordance with the PRISMA guidelines. All studies reporting original data concerning the role of iron or iron complexes in the pathophysiology of endometriosis were included. Studies that did not report original data or provided a review of the field were excluded. Bias analysis was completed for each included study by using the Newcastle-Ottawa scoring system.
Main results and the role of chance: There were 776 records identified and these were screened down to 53 studies which met the eligibility criteria, including 6 animal and 47 human studies, with 3556 individual participants. Iron excess is demonstrated in various tissues and fluids, including ovarian endometriomas, ovarian follicles, ectopic endometriotic lesions, and peritoneal fluid. Markers of oxidative stress are strongly associated with high iron levels, and aberrant expression of iron-transport proteins has been demonstrated. Abnormal resistance to ferroptosis is likely. Iron-mediated oxidative stress is responsible for a pro-inflammatory micro-environment and is linked to subfertility, symptom severity, and, possibly, malignant transformation.
Limitations reasons for caution: A minority of the included studies were of objectively low quality with a high risk of bias and may lead to misleading conclusions. Additionally, multiple studies failed to appropriately characterize the included patients by known confounding variables, such as menstrual cycle phase, which may introduce bias to the findings.
Wider implications of the findings: Current literature depicts a central role of aberrant iron mechanics and subsequent oxidative stress in endometriosis. It is likely that iron excess is at least partly responsible for the persistence and proliferation of ectopic endometriotic lesions. As such, iron mechanics represent an attractive target for novel therapeutics, including iron chelators or effectors of the iron-oxidative stress pathway. There are significant gaps in our current understanding, and this review highlights and recommends several topics for further research. These include the role of iron chelation, resistance to ferroptosis, the relationship between iron excess and localized hypoxia, systemic iron pathophysiology in endometriosis, and the role of oxidative stress in malignant transformation.
Study funding/competing interests: J.W. and S.G.P. are supported by clinical fellowships at Liverpool University Hospital NHS Foundation trust. No additional funding was requested or required for the completion of this work. C.J.H. is supported by a Wellbeing of Women project grant (RG2137). D.K.H. is supported by a Wellbeing of Women project grant (RG2137) and an MRC clinical research training fellowship (MR/V007238/1). The authors have no conflicts of interest to declare.
Registration number: A protocol was prospectively registered with the PROSPERO database in August 2021 (CRD42021272818).
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