Female reproductive toxicology of cadmium

Massányi, Péter; Lukáč, Norbert; Uhrín, V.; Toman, R.; Pivko, J.; Rafay, J.; Forgács, Zsolt; Somosy, Z.

doi:10.1556/abiol.58.2007.3.5

Cited by 66 publications

(30 citation statements)

References 14 publications

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“…Rather, Cd effects in mice were largely strain-dependent due to genetically determined expression of the Cd transporter ZIP-8, and not due to the MT phenotype (Taylor et al 1973;Liu et al 2001;Dalton et al 2005). In the female reproductive tract, however, Cd treatment in rats resulted in estrogen-like, proliferative effects (Johnson et al 2003), whereas in rabbits and mice, it caused degenerative changes in various parts of the reproductive tract and reduced pregnancy rate (Dalton et al 1996a;Massany et al 2007). The impaired reproduction was present also in Cd-treated TG, MT-1-overexpressing female mice (Dalton et al 1996a).…”

Section: Metallothionein In the Urinementioning

confidence: 99%

Role of metallothionein in cadmium traffic and toxicity in kidneys and other mammalian organs

et al. 2010

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Metallothioneins are cysteine-rich, small metal-binding proteins present in various mammalian tissues. Of the four common metallothioneins, MT-1 and MT-2 (MTs) are expressed in most tissues, MT-3 is predominantly present in brain, whereas MT-4 is restricted to the squamous epithelia. The expression of MT-1 and MT-2 in some organs exhibits sex, age, and strain differences, and inducibility with a variety of stimuli. In adult mammals, MTs have been localized largely in the cell cytoplasm, but also in lysosomes, mitochondria and nuclei. The major physiological functions of MTs include homeostasis of essential metals Zn and Cu, protection against cytotoxicity of Cd and other toxic metals, and scavenging free radicals generated in oxidative stress. The role of MTs in Cd-induced acute and chronic toxicity, particularly in liver and kidneys, is reviewed in more details. In acute toxicity, liver is the primary target, whereas in chronic toxicity, kidneys are major targets of Cd. The intracellular MTs bind Cd ions and form CdMT. In chronic intoxication, Cd stimulates de novo synthesis of MTs; it is assumed that toxicity in the cells starts when loading with Cd ions exceeds the buffering capacity of intracellular MTs. CdMT, released from the Cd-injured organs, or when applied parenterally for experimental purposes, reaches the kidneys via circulation, where it is filtered, endocytosed in the proximal tubule cells, and degraded in lysosomes. Liberated Cd can immediately affect the cell structures and functions. The resulting proteinuria and CdMT in the urine can be used as biomarkers of tubular injury.

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Section: Metallothionein In the Urinementioning

confidence: 99%

Role of metallothionein in cadmium traffic and toxicity in kidneys and other mammalian organs

et al. 2010

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“…In addition, the industrial emission particularly from metal refining industries [2] has resulted in increased accumulation of Cd in the environment. Cd commonly exists in +2 state and has a long biological half-life of 15-30 years [3], mainly due to its low rate of excretion from the body, and accumulates in blood, kidney, and liver as well as in the reproductive organs [4][5][6]. Hence, it has elicited diverse toxic effects and caused nephrotoxicity, carcinogenity, teratogenicity, endo-crine, and immune toxicities [6][7][8].…”

Section: Introductionmentioning

confidence: 99%

Gestational Cadmium Exposure-Induced Ovotoxicity Delays Puberty through Oxidative Stress and Impaired Steroid Hormone Levels

Samuel¹,

Stanley

Princess³

et al. 2011

J. Med. Toxicol.

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Cadmium (Cd), an environmental pollutant, has been shown to be highly toxic to both humans and animals. Its widespread industrial use has led to its accumulation in the environment. Cd has been shown to target multiple organs following acute intoxication, causing nephrotoxicity, immunotoxicity, osteotoxicity, and reproductive toxicity. Cd can cross the placental barrier and cause a wide range of defects during fetal development. The current study was aimed to assess the effect of Cd on the female reproductive system. Female rats were exposed to Cd [50/200 ppm] from embryonic day 9 to 21 through drinking water. Serum steroid hormone concentrations, hematological parameters, antioxidant enzyme levels, and ovarian histopathology were described. Water consumption, gravid uterine/body weight decreased in both the doses of Cd-treated dams. The hematological parameters analyzed in rat pups showed a significant reduction in both doses of Cd studied, while hemoglobin showed a significant reduction in 200 ppm Cd treatment alone. MCHC levels did not show any variation in 50 ppm Cd treatment, while 200 ppm Cd treatment significantly increased. Specific activities of superoxide dismutase, catalase, glutathione peroxidase, glutathione reductase, glutathione-S-transferase, and serum testosterone, estradiol, and progesterone were significantly decreased. The levels of hydrogen peroxide and lipid peroxidation were increased in 50 and 200 ppm Cd-treated rats. These changes were accompanied with disrupted ovarian histoarchitecture, an extended estrous cycle, and delayed pubertal onset in Cd-treated rats. The data generated from the present study suggest that gestational Cd treatment induces ovarian toxicity and reproductive dysfunction through increased oxidative stress.

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“…Gestational exposure to Cd affects female reproductive health as a result of changes in ovarian function associated with altered ovarian histoarchitecture, oxidative stress, anemia, and delayed puberty with impaired steroid hormone levels (Thompson and Bannigan, 2008). ROS not only have effects on the male reproductive system but also have effects on the female reproductive system in terms of interfering with the implantation and fertilization of eggs, female infertility, and the unregulated synthesis of female sex hormones (Massányi et al, 2007a).…”

Section: Direct Effects On the Ovary And Ovarian Productionmentioning

confidence: 99%