A Monsanto GMO maize, called MON89034, caused kidney disease and bladder stones in rats
This is a newly edited version of an article previously published on GMWatch:
http://gmwatch.org/en/news/latest-news/18120
---
EU’s GMO regulator ignored human health warnings over a Monsanto insecticidal corn
by Claire Robinson
Independent Science News, 5 March 2018
https://www.independentsciencenews.org/health/eus-gmo-regulator-ignored-human-health-warnings-over-a-monsanto-insecticidal-corn/
[Find references at above URL]
A Monsanto genetically modified (GMO) maize, called MON89034, caused kidney disease and bladder stones in rats in industry tests performed in 2007. Several EU member states, including Germany, Belgium, Austria, and France, independently raised concerns about these results during the EU’s standard three-month regulatory consultation process. But the central GMO regulator of the EU, the European Food Safety Authority (EFSA), issued a favourable opinion on MON89034 regardless.[1] With the usual lack of agreement from EU member states on whether to authorize the maize, the EU Commission subsequently approved MON89034 for human consumption in 2011.[2]
MON89034 has since been crossed with other GM maize varieties to form “stacked” GM crops containing multiple GM traits. As each newly stacked GMO trait involving MON89034 has come up for approval, member states have continued to draw attention to the original adverse health impacts in the rats fed MON89034.
France in particular has repeatedly raised concerns about the kidney and bladder effects in rats fed MON89034. But EFSA has always disregarded them and issued favourable opinions, allowing the EU leadership (the Commission) to so far approve nine stacked maize varieties containing MON89034.[3]
What’s in MON89034 maize?
MON89034, marketed as YieldGard™ VT Pro™, is a Monsanto GM maize that contains its own Bt toxin insecticides (also known as Cry toxins). MON89034 maize plants produce a synthetic Bt toxin, Cry1A.105 – a combination of Bt toxins called Cry1Ac/Cry1Ab and Cry1F. This synthetic toxin is combined with another Bt toxin called Cry2Ab2 [4]. Neither protein has a natural equivalent, so safety cannot be concluded by comparison with Bt toxins used previously in agriculture (Latham et al., 2017).
Kidney and bladder adverse effects
EFSA asserted that this GM maize was as safe as non-GMO maize even though in Monsanto’s own studies two out of 20 female rats receiving the high dose of GM maize (33% of the total diet) developed kidney damage and bladder stones. One of the two rats died after just two weeks on the GM diet.
EFSA reported that the changes in the two rats included “minimal” chronic progressive kidney disease or damage, minimal to moderate transitional cell hyperplasia (cell proliferation that can be a precursor to cancer of the urinary system), inflammation, and hydronephrosis (presence of water in the kidneys due to obstruction). EFSA added that both rats had “urinary bladder calculi” – bladder stones. The study pathologist concluded that the tissue abnormalities observed were probably linked to the stones.
EFSA’s response
Nevertheless, EFSA concluded that the kidney damage and bladder stones in the GM maize-fed rats were “spontaneous” and had nothing to do with the GM diet. This was because, according to EFSA, “a low incidence of urinary bladder calculi [stones] is known to occur in this rat strain”.
EFSA added, “According to historical control data supplied in the application, the incidence of urinary bladder calculi in high dose females in this study was also found in female control rats in previous studies conducted with CD rats in the same testing laboratory. The [GMO] Panel therefore considers the urinary bladder calculi as well as the associated kidney alterations as incidental findings which were not related to administration of maize MON89034.”
Member state concerns
EFSA issued its favourable opinion on MON89034 in 2008, concluding that it was as safe as non-GMO maize.[1] Some EU member states strongly disagreed. This is clear from their comments from the three month consultation period leading up to the publication of EFSA’s opinion.[5]
Germany commented on the kidney and bladder results: “While the applicant suggests that these findings are unrelated to consumption of the test diet, possible adverse effects of MON89034 maize on the health of the test animals cannot be excluded from this result and from other significantly different nephrological [kidney] and haematological [blood] findings in MON89034 maize fed female rats.”[5]
The German experts, from the German Federal Agency for Nature Conservation (BfN), recommended that Monsanto be required to carry out an additional two-generation study with the maize to test for long-term health effects. But EFSA responded that it saw “no reason to request additional feeding studies”.[5]
Austria also voiced concerns about the kidney and bladder findings, as did the experts from Belgium’s Biosafety Advisory Council. The Belgian experts focused on an additional worrying finding: a low thyroid/parathyroid weight relative to final body weight was found in this same group of female rats fed a 33% GM maize diet. Referring to the whole roster of effects in the GM-fed rats, Belgium recommended having “a closer look” to see “whether these findings are solely due to chance. In case any doubt remains, further testing is recommended.”[5]
Historical control data
Much of the disagreement around MON89034 surrounded the interpretation and reliability of data from historical controls. Thus EFSA repeatedly dismissed member states’ concerns about the bladder stones in the GM maize-fed female rats by referring to historical data that Monsanto had submitted from control group rats in other experiments. These data are unpublished and so cannot be checked by independent scientists. EFSA claimed that the data show that in this strain of rat, bladder stones or urinary calculi “sometimes appear”.[5] The implication was that MON89034 did not cause the problems.
However, the experts from the French food safety agency ANSES pointed out that the percentage of high-dose GM maize-fed rats developing bladder stones was 10%, whereas it was 0.49% in the historical control data.[5] EFSA never addressed this major discrepancy.
The French experts commented that “additional explanations” were required. Without them, ANSES “cannot conclude on the safety of products derived from maize varieties carrying the MON89034 transformation event”.[5]
The French were still not reassured by Monsanto’s historical control data in 2016,[6] when they reviewed Monsanto’s application for the approval of a GM maize containing the MON89034 trait, called MIR162 x MON87427 x MON89034 x NK603.
ANSES stated, “Although historical data from 70 studies conducted between 1999 and 2006 with rats of the same strain were provided by the petitioner, they did not appear sufficient to conclude that there was no link between the oral administration of MON89034 maize and the occurrence of bladder stones observed in female animals fed the high dose of MON89034.”[6]
ANSES repeated these concerns in a 2017 opinion on another stacked trait maize, MON89034 x 1507 x NK603 x DAS-40278-9.[7]
Risks stack up
As is clear from ANSES’s recent opinions, EU member states’ concerns over MON89034 have not gone away. Rather they have intensified as this GM Bt maize variety has been crossed with other GM Bt maize varieties to produce “stacked” multi-GM-trait crops. The database run by the industry body ISAAA lists a total of 10 GMO maize varieties containing the MON89034 trait that have been approved in Europe for food and feed use.[8]
With stacked trait GM crops, there is a risk that the multiple GMO components of the crop will interact with each other, with other elements in the plant, or with the agrochemicals applied during cultivation, and create new or enhanced toxins or allergens.
However, EFSA does not assess the combined effects of the different GM traits in a stacked variety, nor does it require a 90-day animal toxicity feeding study with the stacked GM crop, such as is required for single-trait GM varieties. Instead EFSA bases its safety assessment on the previous animal feeding studies with the single-trait GM varieties that were crossed to make the stacked-trait variety.[9,10]
Shaky foundation
In 2007 several member states expressed concerns about the safety of a stacked trait GM maize variety containing MON89034, known as MON89034 x MON88017.[11] But EFSA failed to respond to any of these concerns with hard evidence or substantive scientific argument and in 2011 MON89034 x MON88017 was approved for food and feed use.[12]
In a comment that questions whether a solid structure can be built on a shaky foundation, Austria stated that EFSA’s risk assessments of the single traits that went into MON89034 x MON88017 were “insufficient”, so considering an approval for the stacked crop before questions about the single traits had been clarified was not “appropriate”.[11]
Austria also challenged the need for this GM crop by stating that the rootworm pest targeted by the Bt toxins in the GM maize can be controlled by simple crop rotations. It also pointed out that many components of the GM maize were statistically significantly different from the controls and recommended molecular profiling “omics” analysis to detect unintended effects.[11]
France, Austria, and Belgium worried that no animal feeding toxicology studies with the complete stacked trait GM crop had been done, so the safety of the combined Bt toxins had not been tested.[11]
Austria stated, “Despite the new risk of interactions based on gene-stacking no toxicity feeding studies were conducted. The studies carried out on the single events are not regarded as sufficient for the risk assessment of novel constituents and proteins by stacking.”[11]
Belgium stated that a 13-week feeding study in rats should be performed with the stacked trait crop since “synergistic effects” of the combined proteins in the maize “cannot be excluded”.[11]
As GM crops become more complex, skeptical EU member states and the public are likely to grow more mistrustful of EFSA’s failures to address risk and of the Commission’s actions in approving these crops without a democratic mandate.
Claire Robinson is editor of GMWatch.org and the co-author, with two genetic engineers, of GMO Myths and Truths: A Citizen’s Guide to the Evidence on the Safety and Efficacy of Genetically Modified Crops and Foods, which is available from Amazon.
References to this article are available here:
https://www.independentsciencenews.org/health/eus-gmo-regulator-ignored-human-health-warnings-over-a-monsanto-insecticidal-corn/