Medical/biological study (experimental study)

A study of neurotoxic biomarkers, c-fos and GFAP after acute exposure to GSM radiation at 900MHz in the picrotoxin model of rat brains med./bio.

By: Carballo-Quintas M, Martinez-Silva I, Cadarso-Suarez C, Alvarez-Figueiras M, Ares-Pena FJ, Lopez-Martin E

Published in: Neurotoxicology 2011; 32 (4): 478-494

Aim of study (acc. to author)

To study a time-course description of effects after acute microwave exposure in the rat brain by measuring 1) the neuronal activation using the c-fos expression and 2) glial reactivity as an indicator of parallel neuronal damage in seizure-related rat model.

Background/further details

Rats were made seizure-prone by injection of a subconvulsive dose of the GABA antagonist picrotoxin.
72 adult male rats were divided into 12 groups: 1) picrotoxin treated (to induce seizure proneness), exposed for 2 h and investigated after 90 min., 2) picrotoxin treated, sham-exposed for 2 h and investigated after 90 min., 3) no picrotoxin administration, exposed for 2 h and investigated after 90 min., 4) no picrotoxin administration, sham-exposed for 2 h and investigated after 90 min., 5) picrotoxin treated, exposed for 2 h and investigated after 24 h, 6) picrotoxin treated, sham-exposed for 2 h and investigated after 24 h, 7) no picrotoxin administration, exposed for 2 h and investigated after 24 h, 8) no picrotoxin administration, sham-exposed for 2 h and investigated after 24 h, 9) picrotoxin treated, exposed for 2 h and investigated after three days, 10) picrotoxin treated, sham-exposed for 2 h and investigated after three days, 11) no picrotoxin administration, exposed for 2h and investigated after three days, 12) no picrotoxin administration, sham-exposed for 2 h and investigated after three days.

Endpoint

effects on the neurological system: clinical signs of seizure or jerks; c-fos and GFAP expression in the brain

Exposure

- 900 MHz
- microwaves
- PW pulsed wave
- mobile communications
- digital mobile phone
- GSM
- co-exposure

Exposure	Parameters
Exposure 1: 900 MHz Modulation type: pulsed Exposure duration: continuous for 2 h	power: 1 W (output power) power: 192.67 mW maximum (178.37 - 192.67 mW mean absorbed power with PT) power: 202.33 mW maximum (189.41 - 202.33 mW mean absorbed power without PT) SAR: 1.44 W/kg mean (brain) (1.32 - 1.44 W/kg with PT) SAR: 1.38 W/kg mean (brain) (1.35 - 1.38 W/kg without PT) SAR: 1.62 W/kg peak value (1 g) (1.48 - 1.62 W/kg in the brain with PT) SAR: 1.55 W/kg peak value (1 g) (1.52 - 1.55 W/kg in the brain without PT) SAR: 0.81 W/kg mean (whole body) (0.74 - 0.81 W/kg with PT) SAR: 0.78 W/kg mean (whole body) (0.76 - 0.78 W/kg without PT) SAR: 4.47 W/kg peak value (1 g) (4.09 - 4.47 W/kg in the body with PT) SAR: 4.28 W/kg peak value (1 g) (4.19 - 4.28 W/kg in the body without PT)

Exposure

Parameters

Exposure 1: 900 MHz

Modulation type: pulsed

Exposure duration: continuous for 2 h

power: 1 W (output power)
power: 192.67 mW maximum (178.37 - 192.67 mW mean absorbed power with PT)
power: 202.33 mW maximum (189.41 - 202.33 mW mean absorbed power without PT)
SAR: 1.44 W/kg mean (brain) (1.32 - 1.44 W/kg with PT)
SAR: 1.38 W/kg mean (brain) (1.35 - 1.38 W/kg without PT)
SAR: 1.62 W/kg peak value (1 g) (1.48 - 1.62 W/kg in the brain with PT)
SAR: 1.55 W/kg peak value (1 g) (1.52 - 1.55 W/kg in the brain without PT)
SAR: 0.81 W/kg mean (whole body) (0.74 - 0.81 W/kg with PT)
SAR: 0.78 W/kg mean (whole body) (0.76 - 0.78 W/kg without PT)
SAR: 4.47 W/kg peak value (1 g) (4.09 - 4.47 W/kg in the body with PT)
SAR: 4.28 W/kg peak value (1 g) (4.19 - 4.28 W/kg in the body without PT)

General information

rats were treated in 12 groups: i) rats injected with picrotoxin (PT) 5 min before the experiment and immobilized in methacrylate tubes with exposure to GSM for 2 h; rats studied 90 min after end of immobilization ii) rats injected with picrotoxin (PT) 5 min before the experiment and immobilized in methacrylate tubes without GSM exposure for 2 h; rats studied 90 min after end of immobilization ii) rats injected with vehicle (no PT) 5 min before the experiment and immobilized in methacrylate tubes with exposure to GSM for 2 h; rats studied 90 min after end of immobilization iv) rats injected with vehicle (no PT) 5 min before the experiment and immobilized in methacrylate tubes without GSM exposure for 2 h; rats studied 90 min after end of immobilization v) as i) but rats studied 24 h after end of immobilization vi) as ii) but rats studied 24 h after end of immobilization vii) as iii) but rats studied 24 h after end of immobilization viii) as iv) but rats studied 24 h after end of immobilization ix) as i) but rats studied 3 days after end of immobilization x) as ii) but rats studied 3 days after end of immobilization xi) as iii) but rats studied 3 days after end of immobilization xii) as iv) but rats studied 3 days after end of immobilization

Exposure 1

Main characteristics

Frequency	900 MHz
Type	electromagnetic field
Exposure duration	continuous for 2 h

Modulation

Modulation type	pulsed
Additional info	GSM

Exposure setup

Exposure source	antenna
Setup	methacrylate tubes with immobilized rats placed in a 150 cm x 46 cm x 70 cm radiation cage with an incorporated transmission antenna
Sham exposure	A sham exposure was conducted.

Parameters

Measurand	Value	Type	Method	Mass	Remarks
power	1 W	-	-	-	output power
power	192.67 mW	maximum	-	-	178.37 - 192.67 mW mean absorbed power with PT
power	202.33 mW	maximum	-	-	189.41 - 202.33 mW mean absorbed power without PT
SAR	1.44 W/kg	mean	estimated	brain	1.32 - 1.44 W/kg with PT
SAR	1.38 W/kg	mean	estimated	brain	1.35 - 1.38 W/kg without PT
SAR	1.62 W/kg	peak value	estimated	1 g	1.48 - 1.62 W/kg in the brain with PT
SAR	1.55 W/kg	peak value	estimated	1 g	1.52 - 1.55 W/kg in the brain without PT
SAR	0.81 W/kg	mean	estimated	whole body	0.74 - 0.81 W/kg with PT
SAR	0.78 W/kg	mean	estimated	whole body	0.76 - 0.78 W/kg without PT
SAR	4.47 W/kg	peak value	estimated	1 g	4.09 - 4.47 W/kg in the body with PT
SAR	4.28 W/kg	peak value	estimated	1 g	4.19 - 4.28 W/kg in the body without PT

Reference articles

Lopez-Martin E et al. (2009): The action of pulse-modulated GSM radiation increases regional changes in brain activity and c-Fos expression in cortical and subcortical areas in a rat model of picrotoxin-induced seizure proneness
Lopez-Martin F et al. (2008): An experimental Set-Up for measurement of the power absorbed from 900 MHz GSM standing waves by small animals, illustrated by application to Picrotoxin-treated rats
Lopez-Martin E et al. (2006): GSM radiation triggers seizures and increases cerebral c-Fos positivity in rats pretreated with subconvulsive doses of picrotoxin
Huber R et al. (2003): Radio frequency electromagnetic field exposure in humans: Estimation of SAR distribution in the brain, effects on sleep and heart rate
Fritze K et al. (1997): Effect of global system for mobile communication microwave exposure on the genomic response of the rat brain

Exposed system:

Methods Endpoint/measurement parameters/methodology

molecular biosynthesis: c-fos expression (in cortical structures (neocortex including somatosensory areas such as motor cortex and parietal somatosensory cortex; paleocortex including olfactory areas such as piriform cortex and primary sensory and integrative entorhinal cortex) and subcortical structures (hippocampal areas: dentate gyrus, CA1, CA3)) and GFAP expression (only after three days) in the brain (immunohistochemistry; microscopy)
effects on the neurological system: clinical signs of seizure (videotape) or myoclonic jerks; c-fos and GFAP expression in the brain (see "molecular biosynthesis")

Investigated system:

tissue slices
investigation on living organism

Investigated organ system:

brain/CNS

Time of investigation:

during exposure
after exposure

Main outcome of study (acc. to author)

The data revealed that c-fos expression and glial markers were triggered by the combined stress of non-thermal mobile phone exposure and the toxic effect of picrotoxin on cerebral tissues:
90 minutes after exposure high levels of c-fos expression were recorded in the neocortex and paleocortex along with low hippocampus activation in picrotoxin treated animals. Most brain areas, except the piriform cortex, showed important increases in neuronal activation 24 h after exposure and picrotoxin administration. Three days after picrotoxin treatment, exposure effects were still apparent in the neocortex, and the hippocampal sturctures (dentate gyrus and CA3), but a significant decrease in activity was found in the palaeocortex structures (piriform cortex and entorhinal cortex). During this time, glial reactivity increased in brain regions of irradiated, picrotoxin-treated animals.
The findings suggest the need for further examination of the effects of mobile telephone exposure on epileptic patients.

Study character:

medical/biological study
experimental study
full/main study
blind study

Study funded by

Ministerio Espanol de Ciencia y Innovación (Ministry of Science and Innovation), Spain
Xunta de Galicia, Spain

Kouchaki E et al. (2016): Effect of mobile phone radiation on pentylenetetrazole-induced seizure threshold in mice
Bouji M et al. (2016): Neurobiological effects of repeated radiofrequency exposures in male senescent rats
Aboul Ezz HS et al. (2013): The effect of pulsed electromagnetic radiation from mobile phone on the levels of monoamine neurotransmitters in four different areas of rat brain
Jorge-Mora T et al. (2011): The Effects of Single and Repeated Exposure to 2.45 GHz Radiofrequency Fields on c-Fos Protein Expression in the Paraventricular Nucleus of Rat Hypothalamus
Noor NA et al. (2011): Variations in amino acid neurotransmitters in some brain areas of adult and young male albino rats due to exposure to mobile phone radiation
Ammari M et al. (2010): GFAP expression in the rat brain following sub-chronic exposure to a 900 MHz electromagnetic field signal
Finnie JW et al. (2010): Microglial activation as a measure of stress in mouse brains exposed acutely (60 minutes) and long-term (2 years) to mobile telephone radiofrequency fields
Lopez-Martin E et al. (2009): The action of pulse-modulated GSM radiation increases regional changes in brain activity and c-Fos expression in cortical and subcortical areas in a rat model of picrotoxin-induced seizure proneness
Ammari M et al. (2008): Effect of a chronic GSM 900 MHz exposure on glia in the rat brain
Finnie JW et al. (2007): Stress response in mouse brain after long-term (2 year) exposure to mobile telephone radiofrequency fields using the immediate early gene, c-fos
Brillaud E et al. (2007): Effect of an acute 900MHz GSM exposure on glia in the rat brain: a time-dependent study
Lopez-Martin E et al. (2006): GSM radiation triggers seizures and increases cerebral c-Fos positivity in rats pretreated with subconvulsive doses of picrotoxin
Mausset-Bonnefont AL et al. (2004): Acute exposure to GSM 900-MHz electromagnetic fields induces glial reactivity and biochemical modifications in the rat brain
Sung JH et al. (2003): The influences of extremely low frequency magnetic fields on drug-induced convulsion in mouse
Erdinc OO et al. (2003): Electromagnetic waves of 900 MHz in acute pentylenetetrazole model in ontogenesis in mice
Hossmann KA et al. (2003): Effects of electromagnetic radiation of mobile phones on the central nervous system
Persinger MA et al. (1999): Facilitation of seizures in limbic epileptic rats by complex 1 microTesla magnetic fields
Miller SA et al. (1999): Ultrawideband radiation and pentylenetetrazol-induced convulsions in rats
Pappas BA et al. (1983): Acute exposure to pulsed microwaves affects neither pentylenetetrazol seizures in the rat nor chlordiazepoxide protection against such seizures

A study of neurotoxic biomarkers, c-fos and GFAP after acute exposure to GSM radiation at 900MHz in the picrotoxin model of rat brains med./bio.

Aim of study (acc. to author)

Background/further details

Endpoint

Exposure

General information

Exposure 1

Main characteristics

Modulation

Exposure setup

Parameters

Reference articles

Methods Endpoint/measurement parameters/methodology

Main outcome of study (acc. to author)

Study funded by

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