| Literature DB >> 22754462 |
Susana Alfaro-Lira1, María Pizarro-Ortiz, Gloria M Calaf.
Abstract
The use of organophosphorous insecticides in agricultural environments and in urban settings has increased significantly. The aim of the present study was to analyze morphological alterations induced by malathion and 17β-estradiol (estrogen) in rat kidney tissues. There were four groups of animals: control, malathion, estrogen and combination of both substances. The animals were injected for five days and sacrificed 30, 124 and 240 days after treatments. Kidney tissues were analyzed for histomorphological and immunocytochemical alterations. Morphometric analysis indicated that malathion plus estrogen-treated animals showed a significantly (p < 0.05) higher grade of glomerular hypertrophy, signs of tubular damage, atypical proliferation in cortical and hilium zone than malathion or estrogen alone-treated and control animals after 240 days. Results indicated that MFG, ER-α, ER-β, PgR, CYP1A1, Neu/ErbB2, PCNA, vimentin and Thrombospondin 1 (THB) protein expression was increased in convoluted tubules of animals treated with combination of malathion and estrogen after 240 days of 5 day treatment. Malignant proliferation was observed in the hilium zone. In summary, the combination of malathion and estrogen induced pathological lesions in glomeruli, convoluted tubules, atypical cell proliferation and malignant proliferation in hilium zone and immunocytochemical alterations in comparison to control animals or animals treated with either substance alone. It can be concluded that an increased risk of kidney malignant transformation can be induced by exposure to environmental and endogenous substances.Entities:
Keywords: CYP1A1; ER-α; ER-β; MFG; Neu/ErbB2; PCNA; PgR; THBS; atypical cell proliferation; estrogen; kidney; malathion; vimentin
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Year: 2012 PMID: 22754462 PMCID: PMC3386577 DOI: 10.3390/ijerph9051630
Source DB: PubMed Journal: Int J Environ Res Public Health ISSN: 1660-4601 Impact factor: 3.390
Figure 1The graphs show the degree of (A) Glomerular hypertrophy, (B) Signs of tubular damage, Atypical proliferation in (C) Cortical area and (D) hilium zone. The error bars correspond to 5% error. (*) Significant difference (p < 0.05) between treatment and control group. (C) control, (M) malathion, (E) estrogen, (M + E) malathion in combination with estrogen.
Figure 2Representative images of glomerular hypertrophy graded from 1 a 4 points (A–D) and normal (E) and damaged tubular structures (F–H).
Figure 3(A–B) Representative images of tubules stained with H & E (HE). Immunochemical staining of control and combination of malathion and estrogen-treated rats after 240 days of 5 days treatment. Protein expression of (C–D) MGF, (E–F) ERα, (G–H) ERß and (I–J) PgR.
Figure 4Representative images of immunochemical staining of control and combination of malathion and estroegen-treated rats after 240 days of 5 days treatment: Protein expression of (A–B) Neu/ErbB2, (C–D) CYP1A1, (E–F) PCNA, (G–H) vimentin and (I–J) thrombospondin 1.