Rebuttal to Correspondence on “Are Biobased Microfibers Less Harmful than Conventional Plastic Microfibers: Evidence from Earthworms”

IF 10.8 1区 环境科学与生态学 Q1 ENGINEERING, ENVIRONMENTAL
W. Courtene-Jones, F. De Falco, F. Burgevin, R. D. Handy, R. C. Thompson
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Our approach had multiple steps in the testing strategy: an acute exposure to derive dose–response curves for mortality following OCED TG 207, (3) followed by chronic exposure in natural soil following the OECD TG 222 earthworm reproduction test (4) with additional biochemical, histopathological, and behavioral end points to examine individual and likely population-level effects with respect to reproductive success and animal health. The OECD TG 207, like other OECD ecotoxicity tests, was written, validated (e.g., via interlaboratory testing), and approved by the international scientific community. So, under the Mutual Acceptance of Data principle, (5) one should accept the results of the OECD TG 207, when it is conducted correctly, as we have done. In the context of the OECD scheme, the filter paper contact method in OECD TG 207 earthworm acute toxicity test (3) constitutes a robust, initial assessment to identify chemicals of concern, preceding further testing. Of course, for research, the context often extends beyond individual standardized tests that are used commercially to provide hazard data to support environmental safety submissions to regulatory agencies. In addition to the growth, mortality, and reproduction assays specified in OECD TG 222 (4) for soil exposure, we included biochemical, histopathological, and behavioral end points, as these measurements provide mechanistic insights into the effect of pollutants on organisms, e.g., on cellular processes. It is also important to note that a negative (no addition of fibers) and a positive organic chemical control (used to confirm the responsiveness of the test systems) were included throughout our experiments. The inclusion of the positive control and the additional end points exceed the requirements in the OECD guidance, underscoring the robust approaches implemented and the weight of evidence reported. Similarly, OECD TG 207 and/or TG 222 have been widely used in published research, with additional end points to understand biological mechanisms, including particulate materials and fibers (e.g., refs (6−9)). Furthermore, our considerations on protocol amendments to earthworm tests for nanomaterials (10) have recently been extended to plastics. (11) Regarding the suggestion by Kogler et al. (2025) (1) that an artificial soil should be used, we much prefer the environmental realism of a natural soil, notably the Lufa 2.2 soil that is widely used in earthworm studies (e.g., refs (12−14)). Kogler et al. (2025) (1) also state that it is not plausible for a substance to be toxic at low concentration, but not at the higher concentrations in an acute test. Such thinking is derived from solute chemistry and does not consider the bioaccessibility, bioavailability, or the behavior of the material in the exposure media. Microplastic particles, and other forms of particulate pollutants (e.g., nanoparticles, soot particles, sparingly soluble metal oxides), are colloids in water and do not behave like solutes (see Handy et al., 2008 (15) on colloid theory and ecotoxicity). For example, at lower concentrations, particulates may be more dispersed and therefore have a greater total surface area for bioavailability than at higher concentrations. At high particle number concentrations, aggregation behavior could greatly reduce bioaccessibility and therefore bioavailability and toxicity. For these reasons, the dose–response curve is not necessarily going to be like that for a solute, and the metrics used for dosimetry in particle toxicology have been extensively discussed (e.g., Hull et al. 2012 (16)). It is, therefore, by no means implied that higher exposure automatically translates to greater harmful effects. In recognition of those uncertainties in the dose metric, the toxicity data presented in our study were reported as both particle number concentration and mass concentration. In their comment, Kogler et al. (2025) (1) suggest that for biodegradable materials, toxicity testing should be performed on the degradation products rather than the parent material. For historical reasons, polymers, including those made of plastics, are regulated in a different way than other chemicals. In the EU, polymers have been mostly classified as so-called “<i>polymers of low concern</i>” on the assumption of low toxicity and therefore not usually subject to the Registration, Evaluation, Authorisation, and Restriction of Chemicals (REACH) regulations, EC 1907/2006, unless they contain 2% or more of monomers that might behave as a solute and the polymer production exceed one tonne per annum. This view is being challenged by the scientific community (e.g., Groh et al. 2023 (17)). The REACH regulations have recently been amended to include polymers from (micro)plastics (regulation EU 2023/2055), and this reporting will likely become mandatory during 2025. Regardless of historic regulatory requirements, it remains of key environmental relevance to determine the hazard of a product in the form in which it is released into the environment. In the case of fibers, and polymers used in this study, the application of sewage-derived biosolids directly introduces substantial quantities into terrestrial systems each year. (18,19) Further, colored fibers, including those of biobased origins, are widely documented in the environment including in regions far from input sources, such as in deep-sea sediments (20) and Arctic ice cores, (21) indicating their persistence and the precedence for testing the particles themselves. Moreover, one must perform a study before the degradation products can be determined. Any degradation products emitted from the materials during our 56-days of chronic exposure (28 days adult exposure, with a further 28 days for fecundity assessments) would have been contained within the soil experimental system, with earthworms subsequently exposed to these. Due to the technical barriers of conducting such analytical chemistry of potentially multiple breakdown products and/or metabolites in complex environmental matrices, there are no requirements to measure these in OECD ecotoxicity test guidelines in the exposed organisms, and this was not practical in our study for the same reasons; nonetheless, the biological end points in a controlled laboratory experiment can confirm if exposure to a hazardous substance(s) has occurred. The evidence of tissue repair in the histology presented in our original article, the absence of glutathione depletion, and normal concentrations for most of the electrolytes measured, indicate that the animals were meeting the bioenergetic cost of toxicity. (2) As stated in our original article, the aim was not to determine the detailed mechanisms of toxicity but to perform ecologically relevant experiments examining the individual and likely population level effects of the fibers. Inevitably, full mechanistic understanding will come after more experiments, with additional end points and approaches, beyond the scope of a single paper. It is also important to recognize that effects vary between species, and more complete understanding on toxicity of biobased materials such as these will require further testing with other species and in other environmental settings. 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引用次数: 0

Abstract

A recent commentary (Kogler et al. 2025) (1) on our paper entitled “Are Biobased Microfibers Less Harmful than Conventional Plastic Microfibers: Evidence from Earthworms” (2) makes assertions about our study which we clarify here. Their correspondence article also shows misunderstanding of the use of standardized ecotoxicity testing in relation to biobased/biodegradable plastics. Kolger et al. (2025) (1) raised a concern that because the Organisation for Economic Cooperation and Development (OECD) technical guidance (TG) 207 (2) is an acute screening test, it is not therefore appropriate to draw “quantitative conclusions” without more detailed testing in artificial soil. Our approach had multiple steps in the testing strategy: an acute exposure to derive dose–response curves for mortality following OCED TG 207, (3) followed by chronic exposure in natural soil following the OECD TG 222 earthworm reproduction test (4) with additional biochemical, histopathological, and behavioral end points to examine individual and likely population-level effects with respect to reproductive success and animal health. The OECD TG 207, like other OECD ecotoxicity tests, was written, validated (e.g., via interlaboratory testing), and approved by the international scientific community. So, under the Mutual Acceptance of Data principle, (5) one should accept the results of the OECD TG 207, when it is conducted correctly, as we have done. In the context of the OECD scheme, the filter paper contact method in OECD TG 207 earthworm acute toxicity test (3) constitutes a robust, initial assessment to identify chemicals of concern, preceding further testing. Of course, for research, the context often extends beyond individual standardized tests that are used commercially to provide hazard data to support environmental safety submissions to regulatory agencies. In addition to the growth, mortality, and reproduction assays specified in OECD TG 222 (4) for soil exposure, we included biochemical, histopathological, and behavioral end points, as these measurements provide mechanistic insights into the effect of pollutants on organisms, e.g., on cellular processes. It is also important to note that a negative (no addition of fibers) and a positive organic chemical control (used to confirm the responsiveness of the test systems) were included throughout our experiments. The inclusion of the positive control and the additional end points exceed the requirements in the OECD guidance, underscoring the robust approaches implemented and the weight of evidence reported. Similarly, OECD TG 207 and/or TG 222 have been widely used in published research, with additional end points to understand biological mechanisms, including particulate materials and fibers (e.g., refs (6−9)). Furthermore, our considerations on protocol amendments to earthworm tests for nanomaterials (10) have recently been extended to plastics. (11) Regarding the suggestion by Kogler et al. (2025) (1) that an artificial soil should be used, we much prefer the environmental realism of a natural soil, notably the Lufa 2.2 soil that is widely used in earthworm studies (e.g., refs (12−14)). Kogler et al. (2025) (1) also state that it is not plausible for a substance to be toxic at low concentration, but not at the higher concentrations in an acute test. Such thinking is derived from solute chemistry and does not consider the bioaccessibility, bioavailability, or the behavior of the material in the exposure media. Microplastic particles, and other forms of particulate pollutants (e.g., nanoparticles, soot particles, sparingly soluble metal oxides), are colloids in water and do not behave like solutes (see Handy et al., 2008 (15) on colloid theory and ecotoxicity). For example, at lower concentrations, particulates may be more dispersed and therefore have a greater total surface area for bioavailability than at higher concentrations. At high particle number concentrations, aggregation behavior could greatly reduce bioaccessibility and therefore bioavailability and toxicity. For these reasons, the dose–response curve is not necessarily going to be like that for a solute, and the metrics used for dosimetry in particle toxicology have been extensively discussed (e.g., Hull et al. 2012 (16)). It is, therefore, by no means implied that higher exposure automatically translates to greater harmful effects. In recognition of those uncertainties in the dose metric, the toxicity data presented in our study were reported as both particle number concentration and mass concentration. In their comment, Kogler et al. (2025) (1) suggest that for biodegradable materials, toxicity testing should be performed on the degradation products rather than the parent material. For historical reasons, polymers, including those made of plastics, are regulated in a different way than other chemicals. In the EU, polymers have been mostly classified as so-called “polymers of low concern” on the assumption of low toxicity and therefore not usually subject to the Registration, Evaluation, Authorisation, and Restriction of Chemicals (REACH) regulations, EC 1907/2006, unless they contain 2% or more of monomers that might behave as a solute and the polymer production exceed one tonne per annum. This view is being challenged by the scientific community (e.g., Groh et al. 2023 (17)). The REACH regulations have recently been amended to include polymers from (micro)plastics (regulation EU 2023/2055), and this reporting will likely become mandatory during 2025. Regardless of historic regulatory requirements, it remains of key environmental relevance to determine the hazard of a product in the form in which it is released into the environment. In the case of fibers, and polymers used in this study, the application of sewage-derived biosolids directly introduces substantial quantities into terrestrial systems each year. (18,19) Further, colored fibers, including those of biobased origins, are widely documented in the environment including in regions far from input sources, such as in deep-sea sediments (20) and Arctic ice cores, (21) indicating their persistence and the precedence for testing the particles themselves. Moreover, one must perform a study before the degradation products can be determined. Any degradation products emitted from the materials during our 56-days of chronic exposure (28 days adult exposure, with a further 28 days for fecundity assessments) would have been contained within the soil experimental system, with earthworms subsequently exposed to these. Due to the technical barriers of conducting such analytical chemistry of potentially multiple breakdown products and/or metabolites in complex environmental matrices, there are no requirements to measure these in OECD ecotoxicity test guidelines in the exposed organisms, and this was not practical in our study for the same reasons; nonetheless, the biological end points in a controlled laboratory experiment can confirm if exposure to a hazardous substance(s) has occurred. The evidence of tissue repair in the histology presented in our original article, the absence of glutathione depletion, and normal concentrations for most of the electrolytes measured, indicate that the animals were meeting the bioenergetic cost of toxicity. (2) As stated in our original article, the aim was not to determine the detailed mechanisms of toxicity but to perform ecologically relevant experiments examining the individual and likely population level effects of the fibers. Inevitably, full mechanistic understanding will come after more experiments, with additional end points and approaches, beyond the scope of a single paper. It is also important to recognize that effects vary between species, and more complete understanding on toxicity of biobased materials such as these will require further testing with other species and in other environmental settings. Finally, with respect to the appropriateness of the data analysis, our original article (2) applied internationally validated, routine methods (i.e., OECD protocols), with levels of replication (n = 10 for filter paper contact experiment, n = 4 replicate vessels for chronic exposure) which are aligned with, or exceed, those recommended by the OECD and the scientific community. (22,23) The level of replication and data assumptions (e.g., checked for abnormality, skewness) were appropriate for the statistical tests performed (24) and are widely used in peer-reviewed studies, (13,25) with results reported as statistically significant or not significant as in the paper. This research was funded by the Natural Environment Research Council through the grants NE/V007556/1 and NE/V007246/1 This article references 25 other publications. This article has not yet been cited by other publications.
对“生物基微纤维是否比传统塑料微纤维危害小:来自蚯蚓的证据”函件的反驳
最近的一篇评论(Kogler et al. 2025)(1)对我们题为“生物基微纤维比传统塑料微纤维危害小吗:来自蚯蚓的证据”的论文(2)对我们的研究做出了断言,我们在这里澄清。他们的通信文章也显示了对使用与生物基/可生物降解塑料相关的标准化生态毒性测试的误解。Kolger等人(2025)(1)提出了一个担忧,即由于经济合作与发展组织(OECD)技术指南(TG) 207(2)是一种急性筛选试验,因此不适合在没有更详细的人工土壤测试的情况下得出“定量结论”。我们的方法在测试策略中有多个步骤:急性暴露以得出OECD TG 207后死亡率的剂量-反应曲线(3),然后在OECD TG 222蚯蚓繁殖试验(4)后在自然土壤中慢性暴露,并附加生化、组织病理学和行为终点,以检查个体和可能的群体水平对繁殖成功和动物健康的影响。经合组织TG 207与经合组织其他生态毒性测试一样,是由国际科学界编写、验证(例如通过实验室间测试)并批准的。因此,在相互接受数据原则下,(5)人们应该接受OECD TG 207的结果,当它正确进行时,就像我们所做的那样。在OECD计划的背景下,OECD TG 207蚯蚓急性毒性试验(3)中的滤纸接触法构成了一个可靠的初步评估,以确定关注的化学物质,然后进行进一步的测试。当然,对于研究而言,其范围往往超出了商业上用于提供危害数据以支持向监管机构提交环境安全报告的个别标准化测试。除了OECD TG 222(4)中规定的土壤暴露的生长、死亡率和繁殖分析外,我们还包括生化、组织病理学和行为终点,因为这些测量提供了污染物对生物体(例如细胞过程)影响的机制见解。同样重要的是要注意,在我们的实验中包括了阴性(不添加纤维)和阳性有机化学控制(用于确认测试系统的响应性)。阳性对照和额外终点的纳入超出了经合发组织指南的要求,强调了所实施的有力方法和所报告证据的重要性。同样,OECD TG 207和/或TG 222在已发表的研究中被广泛使用,并有额外的终点来理解生物机制,包括颗粒材料和纤维(例如,参考文献(6−9))。此外,我们对纳米材料蚯蚓试验议定书修正案的考虑(10)最近已扩展到塑料。(11)关于Kogler等人(2025)(1)提出的应该使用人工土壤的建议,我们更倾向于自然土壤的环境现实主义,特别是广泛用于蚯蚓研究的Lufa 2.2土壤(例如,参考文献(12 - 14))。Kogler等人(2025)(1)也指出,一种物质在低浓度下有毒是不合理的,但在急性试验中浓度较高时则不然。这种想法来源于溶质化学,没有考虑到材料在暴露介质中的生物可及性、生物利用度或行为。微塑料颗粒和其他形式的颗粒污染物(例如,纳米颗粒、烟灰颗粒、少量可溶的金属氧化物)在水中是胶体,不像溶质那样表现(见Handy等人,2008年(15)关于胶体理论和生态毒性)。例如,在较低浓度下,颗粒可能更分散,因此比在较高浓度下具有更大的生物利用度总表面积。在高颗粒数浓度下,聚集行为会大大降低生物可及性,从而降低生物利用度和毒性。由于这些原因,剂量-反应曲线不一定会像溶质的那样,颗粒毒理学中用于剂量测定的指标已经被广泛讨论(例如,Hull et al. 2012(16))。因此,这绝不意味着越高的接触会自动转化为更大的有害影响。考虑到剂量计量的不确定性,本研究中提出的毒性数据报告为粒子数浓度和质量浓度。Kogler等人(2025)(1)在评论中提出,对于生物可降解材料,应对降解产物进行毒性测试,而不是对母体材料进行毒性测试。由于历史原因,聚合物,包括由塑料制成的聚合物,受到的监管方式与其他化学品不同。 在欧盟,聚合物大多被归类为所谓的“低关注聚合物”,假设其毒性较低,因此通常不受化学品注册、评估、授权和限制(REACH)法规(EC 1907/2006)的约束,除非它们含有2%或更多的可能表现为溶质的单体,并且聚合物产量每年超过一吨。这一观点正受到科学界的挑战(例如,Groh等人,2023(17))。REACH法规最近进行了修订,包括(微)塑料聚合物(法规EU 2023/2055),该报告可能在2025年成为强制性的。无论历史法规要求如何,确定产品以其释放到环境中的形式的危害仍然是关键的环境相关性。在本研究中使用的纤维和聚合物的情况下,来自污水的生物固体的应用每年直接向陆地系统引入大量的生物固体。(18,19)此外,有色纤维,包括生物基纤维,在环境中被广泛记录,包括在远离输入源的地区,如深海沉积物(20)和北极冰芯(21)中,表明它们的持久性和对颗粒本身进行测试的优先性。此外,在确定降解产物之前必须进行研究。在我们56天的慢性暴露(28天成人暴露,另外28天用于繁殖力评估)期间,材料释放的任何降解产物都将包含在土壤实验系统中,蚯蚓随后暴露于这些降解产物中。由于在复杂的环境基质中对潜在的多种分解产物和/或代谢物进行这种分析化学的技术障碍,在经合组织的生态毒性测试指南中没有要求对暴露的生物体进行测量,出于同样的原因,这在我们的研究中是不切实际的;尽管如此,受控实验室实验中的生物终点可以确认是否发生了接触有害物质的情况。在我们最初的文章中提出的组织学组织修复的证据,没有谷胱甘肽耗竭,以及大多数电解质测量的正常浓度,表明动物正在满足毒性的生物能量成本。(2)正如我们在原文章中所述,目的不是确定毒性的详细机制,而是进行生态学相关的实验,检查纤维对个体和可能的群体水平的影响。不可避免的是,完整的机制理解将在更多的实验之后出现,有更多的终点和方法,超出了一篇论文的范围。同样重要的是要认识到,不同物种的影响是不同的,更全面地了解这些生物基材料的毒性将需要在其他物种和其他环境条件下进行进一步的测试。最后,关于数据分析的适当性,我们的原始文章(2)应用了国际验证的常规方法(即经合组织协议),其复制水平(滤纸接触实验n = 10,慢性暴露n = 4)与经合组织和科学界推荐的水平一致或超过。(22,23)复制水平和数据假设(例如,检查异常、偏度)适用于所进行的统计检验(24),并广泛用于同行评议研究(13,25),报告的结果如论文所述具有统计学意义或不具有统计学意义。本研究由自然环境研究委员会资助,项目编号为NE/V007556/1和NE/V007246/1。本文引用了25篇其他出版物。这篇文章尚未被其他出版物引用。
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来源期刊
环境科学与技术
环境科学与技术 环境科学-工程:环境
CiteScore
17.50
自引率
9.60%
发文量
12359
审稿时长
2.8 months
期刊介绍: Environmental Science & Technology (ES&T) is a co-sponsored academic and technical magazine by the Hubei Provincial Environmental Protection Bureau and the Hubei Provincial Academy of Environmental Sciences. Environmental Science & Technology (ES&T) holds the status of Chinese core journals, scientific papers source journals of China, Chinese Science Citation Database source journals, and Chinese Academic Journal Comprehensive Evaluation Database source journals. This publication focuses on the academic field of environmental protection, featuring articles related to environmental protection and technical advancements.
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