Medical/biological study (experimental study)

50-Hz magnetic field exposure influences DNA repair and mitochondrial DNA synthesis of distinct cell types in brain and kidney of adult mice med./bio.

By: Schmitz C, Keller E, Freuding T, Silny J, Korr H

Published in: Acta Neuropathol 2004; 107 (3): 257-264

Aim of study (acc. to author)

To investigate the extent of nuclear DNA repair and the relative amount of nuclear DNA single-strand breaks for different cell types in brain and kidney of adult mice after a 50 Hz magnetic field exposure. The question should be answered whether or not DNA damage occurs.

Background/further details

Five minutes after ending exposure, the animals received [³H]thymidine (for autoradiographs) and were killed 2 h later. Autoradiographs were prepared from paraffin sections of brains and kidneys.

Endpoint

genotoxicity/mutation: DNA repair, single-strand breaks, and mitochondrial DNA synthesis

Exposure

- 50/60 Hz
- magnetic field

Exposure	Parameters
Exposure 1: 50 Hz Exposure duration: continuous for 8 weeks	magnetic flux density: 1.8 mT mean

Exposure 1

Main characteristics

Frequency	50 Hz
Type	magnetic field
Waveform	sinusoidal
Exposure duration	continuous for 8 weeks

Exposure setup

Exposure source	Helmholtz coils
Setup	Four cages containing 5 mice each were placed within the inner space of the coils.

Parameters

Measurand	Value	Type	Method	Mass	Remarks
magnetic flux density	1.8 mT	mean	measured	-	-

Exposed system:

animal
mouse/Han:NMRI
whole body

Methods Endpoint/measurement parameters/methodology

genotoxicity/mutation: extent of nuclear DNA repair (unscheduled DNA synthesis (nuclear grain numbers)); amount of nuclear DNA single-strand breaks (in situ nick translation (nuclear grain numbers)); mitochondrial DNA synthesis (cytoplasmic grain densities) (autoradiographs)

Investigated system:

tissue slices

Investigated organ system:

brain/CNS
kidney

Time of investigation:

after exposure

Main outcome of study (acc. to author)

A significant increase in both unscheduled DNA synthesis and in situ nick translation was only found for epithelial cells of the choroid plexus. Thus, these two independent methods indicate that nuclear DNA damage is produced by long-lasting and strong magnetic field irradiation. The fact that only plexus epithelial cells were affected might point to possible effects of magnetic fields on iron transport across the blood-cerebrospinal fluid (Liquor cerebrospinalis) barrier, but the mechanisms are currently not understood.
Mitochondrial DNA synthesis was exclusively increased in renal epithelial cells of distal convoluted tubules (Tubuli renalis) and collecting ducts, i.e., cells with a very high content of mitochondria, possibly indicating increased metabolic activity of these cells.
In summary, the pilot study has shown that a long-lasting and strong 50 Hz magnetic field exposure with a flux density above 1 mT appears to be able to produce nuclear DNA damage within at least one distinct cell population in the brain.

Study character:

medical/biological study
experimental study
pilot/exploratory/preliminary study

Study funded by

RWTH Aachen University, Germany

Woodbine L et al. (2015): The rate of X-ray induced DNA double strand break repair in the embryonic mouse brain is unaffected by exposure to 50 Hz magnetic fields
Saha S et al. (2014): Increased apoptosis and DNA double-strand breaks in the embryonic mouse brain in response to very low-dose X-rays but not 50 Hz magnetic fields
Korr H et al. (2014): No evidence of persisting unrepaired nuclear DNA single strand breaks in distinct types of cells in the brain, kidney, and liver of adult mice after continuous eight-week 50 Hz magnetic field exposure with flux density of 0.1 mT or 1.0 mT
Villarini M et al. (2013): Brain hsp70 expression and DNA damage in mice exposed to extremely low frequency magnetic fields: a dose-response study
Gholampour F et al. (2011): Chronic Exposure to Extremely Low Frequency Electromagnetic Field Induces Mild Renal Damages in Rats
Koyama S et al. (2008): Extremely low frequency (ELF) magnetic fields enhance chemically induced formation of apurinic/apyrimidinic (AP) sites in A172 cells