Unveiling Variability and Uncertainty for Better Science and Decisions on Cancer Risks from Environmental Chemicals

Bogen, Kenneth T.

doi:10.1111/risa.12290

Cited by 5 publications

(3 citation statements)

References 35 publications

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“…38,39 Under this hypothesis, the implied J-shaped DR pattern for increased tumor risk would differ fundamentally from the linear-no-threshold DR pattern implied by the multistage somatic mutation (MSM) theory of tumorigenesis. 38 -43 Consistent with this hypothesis is evidence that potently anti-inflammatory synthetic oleanane triterpenes such as the acetylenic tricyclic bis -(cyano enone) TBE-31, 1-2-cyano-3-,12-dioxooleana-1,9(11)-dien-28-oyl (CDDO) ethyl amide (CDDO-EA), and CDDO-imidazole (CDDO-Im) activate the Nrf2-ARE cytoprotective pathway, induce phase II enzymes, and can suppress or completely block formation of enzyme-altered proliferative hepatocellular foci and liver tumors in rodents coadministered hepatotoxic liver carcinogens such as aflatoxin B 1 (also a potent mutagen) and carbon tetrachloride. 17,36,37,44,45 Although aflatoxin B 1 exposures induce macromolecular adducts with a linear DR pattern over a wide range of doses down to 0.16 ng/kg, coadministration of CDDO-Im before and during aflatoxin B 1 exposures that otherwise efficiently increase the occurrence of liver preneoplastic foci and tumors in male rats can nearly or completely eliminate these aflatoxin B 1 -induced lesions without proportionately reducing aflatoxin B 1 –DNA adducts, 36,34,37 which appears to be at odds with MSM theory.…”

Section: Discussionmentioning

confidence: 82%

Low-Dose Dose–Response for In Vitro Nrf2-ARE Activation in Human HepG2 Cells

Bogen

2017

Dose-Response

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Kelch-like ECH-associated protein 1 (Keap1), nuclear factor erythroid 2-like factor 2-related factor 2 (Nrf2), and the antioxidant response element (ARE) are interacting components of a master regulatory signaling pathway that coordinates redox homeostasis, cytoprotective responses, and shifts in stem cell state. This study reexamined detailed dose–response (DR) data reported for in vitro Nrf2-ARE activation in human hepatoblastoma HepG2 cell lines containing either a ARE-bla or ARE-luc reporter at 12 different concentrations of each of 15 chemicals. The normalized study data were combined among chemicals exhibiting a positive response, yielding n = 531 (179) DR data for 9 (7) chemicals using the ARE-bla (ARE-luc) assay. Three-parameter linear/kth-power regression fits obtained to each combined set of ARE-bla- or ARE-luc-assay response data provided good fits (R 2 = .99 or .91, respectively, P fit > .99) that each incorporate a highly significant negative initial linear slope (P = 4 × 10−5 or .00025) and an overall J-shaped DR pattern. Results from this reanalysis of high-resolution ARE response data support the hypothesis that nonlinear ARE-mediated adaptive cellular responses to oxidative stress are governed by an ultrasensitive molecular switch.

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Section: Discussionmentioning

confidence: 82%

Low-Dose Dose–Response for In Vitro Nrf2-ARE Activation in Human HepG2 Cells

Bogen

2017

Dose-Response

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“…However, regulatory-policy interest typically focuses not on a broad range of potency estimates for each chemical carcinogen, but rather on a conservatively defined upper confidence limit (UCL) on each such estimated potency. A recent comparison of UCLs on estimated human vs. rodent potencies for 24 chemical carcinogens showed that these UCLs exhibit a pattern consistent with the hypothesis that x = 0, and more specifically that UCL estimates of human and rodent potency for chemical carcinogens are, on average, equal to within a factor of <3 with 95% confidence (Bogen 2014).…”

Section: D2 Interspecies Extrapolation and Body-weight Adjustment Of Tumorigenic Potencymentioning

confidence: 72%

Reassessment of MTBE cancer potency considering modes of action for MTBE and its metabolites

Bogen¹,

Heilman²

2015

Critical Reviews in Toxicology

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A 1999 California state agency cancer potency (CP) evaluation of methyl tert-butyl ether (MTBE) assumed linear risk extrapolations from tumor data were plausible because of limited evidence that MTBE or its metabolites could damage DNA, and based such extrapolations on data from rat gavage and rat and mouse inhalation studies indicating elevated tumor rates in male rat kidney, male rat Leydig interstitial cells, and female rat leukemia/lymphomas. More recent data bearing on MTBE cancer potency include a rodent cancer bioassay of MTBE in drinking water; several new studies of MTBE genotoxicity; several similar evaluations of MTBE metabolites, formaldehyde, and tert-butyl alcohol or TBA; and updated evaluations of carcinogenic mode(s) of action (MOAs) of MTBE and MTBE metabolite's. The lymphoma/leukemia data used in the California assessment were recently declared unreliable by the U.S. Environmental Protection Agency (EPA). Updated characterizations of MTBE CP, and its uncertainty, are currently needed to address a variety of decision goals concerning historical and current MTBE contamination. To this end, an extensive review of data sets bearing on MTBE and metabolite genotoxicity, cytotoxicity, and tumorigenicity was applied to reassess MTBE CP and related uncertainty in view of MOA considerations. Adopting the traditional approach that cytotoxicity-driven cancer MOAs are inoperative at very low, non-cytotoxic dose levels, it was determined that MTBE most likely does not increase cancer risk unless chronic exposures induce target-tissue toxicity, including in sensitive individuals. However, the corresponding expected (or plausible upper bound) CP for MTBE conditional on a hypothetical linear (e.g., genotoxic) MOA was estimated to be ∼2 × 10(-5) (or 0.003) per mg MTBE per kg body weight per day for adults exposed chronically over a lifetime. Based on this conservative estimate of CP, if MTBE is carcinogenic to humans, it is among the weakest 10% of chemical carcinogens evaluated by EPA.

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“…Linear-no-threshold (LNT) risk extrapolation has long been applied to estimate risks posed by low-level environmental (particularly by default for mutagenic) carcinogen exposures, based on the 60-year-old multistage somatic mutation/clonal expansion (MSM) theory of cancer. 1 First proposed and represented mathematically by Armitage and Doll in 1957, 2 the MSM theory overlaps most other current competing theories of cancer because the critical events it posits (namely, 2 or more critical oncogene mutations in a somatic stem cell, coupled if/as applicable with intrinsic and/or exposureinduced "promotion" by net proliferation of intermediate/premalignant cells) can also be induced or augmented by events posited as critical by those theories (eg, theories focusing on: 3 oxidative stress, infection, an inflammatory microenvironment, defective wound healing, chromosome damage, genomic instability, and epigenetic dysregulation). Generalizing MSM theory and Knudsen's related 2-mutation tumor suppressor inactivation model describing inherited susceptibility to retinobalstoma, [4][5][6] Moolgavkar, Venzon, Knudson (MVK) and colleagues represented the MSM model mathematically as a 2-stage doubly stochastic Poisson process (Figure 1, left) and fit this model well to many sets of experimental cancer bioassay and human cancer incidence data.…”

Section: Introductionmentioning

confidence: 99%

Inflammation as a Cancer Co-Initiator: New Mechanistic Model Predicts Low/Negligible Risk at Noninflammatory Carcinogen Doses

Bogen¹

2019

Dose-Response

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Linear-no-threshold (LNT) risk extrapolation has long been applied to estimate risks posed by low-level environmental carcinogen exposures, based on the 60-year-old multistage somatic mutation/clonal expansion (MSM) cancer theory. Recent evidence supports an alternative theory: Malignant tumors arise most efficiently from a stem cell that incurs requisite mutations and also is activated by inflammation to an epigenetically mediated and maintained state of adaptive hyperplasia (AH). This new inflammation-MSM (ISM) theory posits that inflammation-activated stem cells normally restricted to sites of injury-induced inflammation and tissue repair become uniquely susceptible to efficient carcinogenesis if normal post-inflammation AH termination is blocked by mutation. This theory posits that inflammation generally thus co-initiates cancer and transiently amplifies activated stem cells, implying that MSM theory (eg, the 2-stage stochastic “Moolgavkar, Venzon, Knudson [MVK]” model) is incomplete. Because inflammation dose–response typically is not LNT, the ISM theory predicts this is also true for most (perhaps all) carcinogens. The ISM (but not the MVK) model is shown to be consistent with recent data showing ∼100% carcinoma incidence (but not DNA adducts) in livers of rats exposed to aflatoxin B 1 and was eliminated when that dose was co-administered with a highly potent anti-inflammatory agent. Experimental approaches to test ISM theory more robustly are discussed.

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Unveiling Variability and Uncertainty for Better Science and Decisions on Cancer Risks from Environmental Chemicals

Cited by 5 publications

References 35 publications

Low-Dose Dose–Response for In Vitro Nrf2-ARE Activation in Human HepG2 Cells

Low-Dose Dose–Response for In Vitro Nrf2-ARE Activation in Human HepG2 Cells

Reassessment of MTBE cancer potency considering modes of action for MTBE and its metabolites

Inflammation as a Cancer Co-Initiator: New Mechanistic Model Predicts Low/Negligible Risk at Noninflammatory Carcinogen Doses

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