In the US, the Environmental Protection Agency has an endocrine disruptor screening programme to validate methods for estrogenic, androgenic and thyroid hormone-like substances. Despite these initiatives, many open questions remain such as, i) defining ‘endocrine disrupter’ (ED), A closer look at each point of the above points followed. Navitoclax manufacturer i) The International Programme on Chemical Safety and Weybridge have proposed slightly
different definitions of an endocrine disrupter. It has been suggested by ECETOC to adopt the Weybridge definition and this appears likely. Current experience in the EFSA Pesticide Risk Assessment Peer Review (PRAPeR) show several current and pressing needs including a clear definition of endocrine disruption and guidelines to reduce uncertainties, scientific and practical tools, and harmonisation in interim measures. Research is needed to understand the basic science and mechanisms of action, and to develop TSA HDAC price measurement methods and risk assessment models. Screening and testing methodologies have to be developed to identify potential endocrine disrupters and to determine adverse effects and dose–response curves and to assess risk, taking into account the requirements of the current legislation. The presentation concluded with a review of the
next steps to be taken in order to reach a consensus on how to regulate endocrine-active pesticides. First the development and validation of appropriate screens and tests, to be followed by OSBPL9 development of procedures and policies and
finally development of standard evaluations and risk assessment guidelines. This is a big order, but progress has begun. At OECD, new guidelines were adopted in September 2009 which accepted two assays and validated a third. The Hershberger assay (Test Guideline 441) and the Human Estrogen Receptor Transcription Assay (Test Guideline 455) were adopted as standard tests and the Repeat Dose 28-day Oral Toxicity (Test Guideline 407) was updated and validated, although here some further fine tuning may be necessary. Finally an examination of validated Quantitative Structure-Activity Relationships could allow an automated look at numerous compounds without the use of animal studies. Decision Criteria in Human Health Risk Assessment for ED Substances. Dr. Karen Hirsch-Ernst, BfR, Germany. This talk was a summary of the meeting Establishment of assessment and decision criteria in human health risk assessment for substances with endocrine disrupting properties under the EU plant protection product regulation, hosted by the German Federal Institute for Risk Assessment (BfR) in Berlin from 11 to 13 November 2009. This was a preliminary report, reflecting the discussion and part of the results of the BfR workshop, but not necessarily detailing the opinion of all participants or of the institutions they work for.