Developmental Toxicity of Mycotoxin Fumonisin B1 in Animal Embryogenesis: An Overview
Abstract
:1. General Features of Fumonisin B1
2. Toxicokinetic of FB1
3. Mechanisms through Which the FB1 Exerts Its Developmental Toxicity
4. Fumonisin B1 and Developmental Toxicity in Animals
4.1. Mammalian Models
4.1.1. Rats
4.1.2. Hamsters
4.1.3. Mice
4.1.4. Rabbits
4.1.5. Humans
4.1.6. Cattle
4.2. Avian Species
5. Concluding Remark
Author Contributions
Funding
Acknowledgments
Conflicts of Interest
References
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Species | FB1 Treatment and Doses | Developmental Toxicity | Reference |
---|---|---|---|
Rat (Sprague-Dawley) | Rat embryos cultured in 0.2 to 40.4 ppm FB1 for 45 h at embryonic day (E) 9.5 | Retarded development; increased abnormal embryos phenotype | [44] |
Rat (Sprague-Dawley) | Rat embryos cultured in 0, 2.17, 7.22, 21.7, 72.2 or 217 ppm hydrolized FB1 (HFB1) for 45 h at E9.5 | Increased percentage of NTDs and other abnormalities | [76] |
Rat (Sprague-Dawley) | Male and female rats fed 0, 1, 10, or 55 ppm FB1 9 or 2 wk prior to mating | No effect on the peformance of dam or embryos; maternal toxicity by altering sphingolipid metabolism in the livers of dam at the highest dose | [77] |
Syrian Hamster | Female hamsters fed 0, 6, 12, 18 mg/kg-BW by gavage on E8–E9 | Increased fetal death; malformation at the highest dose | [78] |
Syrian Hamster | Pregnant Syrian hamsters given 0, 8.7, 10.4, 12.5, 15, or 18 mg/kg-BW by gavage on E8–E12. | Reduced litter size; decreased fetal weight; reduced body length | [79] |
Mouse (ICR) | Mouse embryos cultured with 0, 0.72, 1.44, 2.16, 3.60, 5.05, 10.8, 18.0, 36.0 or 72.1 ppm for 26 h and 36 ppm for 2 h | Induced facial NTDs; growth retardation | [80] |
Mouse (LM/Bc) | Pregnant mice injected with 0, 5, 10, 15 and 20 mg/kg-BW/day via intraperitoneal on E7.5 and E8.5 | Increased exencephaly from 5% to 79% | [44] |
Mouse (LM/Bc) | Female mice treated with 0, 2.5 or 10 mg/kg by intraperitoneal on E7 and E8 | NTDs (36%) in 10 mg/kg treated group | [64] |
Mouse (CD1) | Female mice fed 0, 12.5, 25, 50 and 100 mg FB1/kg-BW by gavage from E7–E15 | Fetal toxicity; increased fetal death; decreased fetal weight | [74] |
Mouse (CD1) | Pregnant mice injected with 15, 30 or 45 mg FB1/kg-BW/day (1st trial); 10, 23, 45 or 100 mg/kg-BW/day (2nd trial) via intraperitoneal at E7 and E8 | Fetotoxicity; increased NTDs (8–55%) | [81] |
Mouse (CD1) | Pregnant mice fed 12.5 mg/kg FB1 at E7.5 and E8.5 | NTDs (7.4% exencephaly) | [82] |
Mouse (LM/Bc, CD1) | Female mice fed 0, 50 or 150 mg/kg diet at wk 5 before mating and after mating until E16 | 10% of exencephaly in LM/Bc mice (at 150 mg/kg); No NTDs but fetal death in CD1 mice | [83] |
Rabbits (New Zealand White) | Rabbits fed 0, 0.1, 0.5, and 1.0 mg/kg-BW by gavage during E3–E19 | Decreased body and organ weights of fetuses | [84] |
Rabbits (NewZealand White x Chinchilla) | Male rabbits fed 0.13, 5.0, 7.5 and 10 mg/kg for 28 wk then mated with female rabbits | Induced embryo mortality | [85] |
Human neural epithelial cells | Cells treated with 0.00072, 0.0072, 0.072, 0.72, 7.2, and 72 ppm FB1 for 48 h | Altered balance of Sphingosine 1-phosphate | [86] |
Bovine oocytes | Cumulus-oocyte complexes matured in 3.6, 7.2, 14.4, 21.6, or 36.0 ppm FB1-containing medium for 22 h | Decreased percentages and quality of matured oocytes and embryos | [87] |
Chicken (Columbia x New Hampshire) | Eggs inoculated with 0.72, 7.2 or 72 ppm of FB1 or 14.4 ppm FB1 + 2.82 ppm FB2, and 0.84 ppm moniliformin at the air sac on day 1 or day 10 of incubation | Increased mortality rates; altered brain, beak, and neck development; pathologic changes in livers, kidneys, heart, lungs, musculoskeletal system, intestines, testes, and brains | [88] |
Chicken embryos (White Leghorn) | Chicken embryos injected with 0, 0.017, 0.085, 0.17, 0.425, 0.85, 1.275 and 1.74 ppm FB1 at day 1 of incubation | Increased embryonic death | [89] |
Chicken embryos (Peterson-Arbor Acres) | Chicken embryos injected with 0 or 0.25 ppm FB1 at 72 h of incubation | Increased embryonic mortality on d 18 | [90] |
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Lumsangkul, C.; Chiang, H.-I.; Lo, N.-W.; Fan, Y.-K.; Ju, J.-C. Developmental Toxicity of Mycotoxin Fumonisin B1 in Animal Embryogenesis: An Overview. Toxins 2019, 11, 114. https://doi.org/10.3390/toxins11020114
Lumsangkul C, Chiang H-I, Lo N-W, Fan Y-K, Ju J-C. Developmental Toxicity of Mycotoxin Fumonisin B1 in Animal Embryogenesis: An Overview. Toxins. 2019; 11(2):114. https://doi.org/10.3390/toxins11020114
Chicago/Turabian StyleLumsangkul, Chompunut, Hsin-I Chiang, Neng-Wen Lo, Yang-Kwang Fan, and Jyh-Cherng Ju. 2019. "Developmental Toxicity of Mycotoxin Fumonisin B1 in Animal Embryogenesis: An Overview" Toxins 11, no. 2: 114. https://doi.org/10.3390/toxins11020114
APA StyleLumsangkul, C., Chiang, H. -I., Lo, N. -W., Fan, Y. -K., & Ju, J. -C. (2019). Developmental Toxicity of Mycotoxin Fumonisin B1 in Animal Embryogenesis: An Overview. Toxins, 11(2), 114. https://doi.org/10.3390/toxins11020114