ELECTROMAGNETIC ENVIRONMENT GENERATED IN A TEM CELL FOR BIOLOGICAL DOSIMETRY APPLICATIONS

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ISEF 2007 XIII International Symposium on Electromagnetic Fields in Mechatronics, Electrical and Electronic Engineering Prague, Czech Republic, September 13-15, 2007 ELECTROMAGNETIC ENVIRONMENT GENERATED IN A TEM CELL FOR BIOLOGICAL DOSIMETRY APPLICATIONS Mihaela Morega 1, Simona Miclaus 2 1 POLITEHNICA University of Bucharest, Romania, mihaela@iem.pub.ro 2 Nicolae Balcescu Land Forces Academy, Sibiu, Romania, simo.miclaus@gmail.com Abstract - The study of biological material exposure to nonionizing electromagnetic field requires the existence and monitoring of a controlled testing environment. Far field exposure assessments in the frequency domain of microwaves are usually performed in rectangular enclosures that act as coaxial transmission lines and provide inside Transversal Electromagnetic (TEM) field distribution assimilated to planar waves, the so called TEM cells. A numerical analysis of the electromagnetic field (EMF) distribution based on the finite element method (FEM) is presented in the paper, with the aim of providing a useful research tool, complementary to experimental tests, for microwave dosimetry in biological media. Introduction Experimental work on biological effects due to radiofrequency (RF) and microwave (MW) field exposures needs a high quality dosimetric assessment. A relevant statistics of a quantified effect is strictly connected to the same exposure conditions throughout the whole volume of the biological sample. One of the commonly used plane wave exposure devices is the TEM-mode chamber or TEM cell, which offers the advantages of being versatile in size, relatively inexpensive, and relatively broad-banded. The TEM cell consists of a main rectangular waveguide (section used for the experimental dosimetry) continued with adjacent tapered transition sections that adapt the dimensions of the cell to the end ports; usually, one port is connected to the MW source through a coaxial cable and the other connects a matched load impedance [1, 2]. The proper correlation among exposure parameters is based on several objectives: maximum test volume, maximum MW frequency limit, good quality of the electric field distribution (maximum uniformity, minimum standing waves, minimum reflections, minimum higher order modes) [3]. We use the TEM cell for small volume biological samples exposure, either plant seeds or plant and animal tissues. The TEM cell can be instrumented to measure the specific energy absorption rate (SAR) in a biological sample continuously, by using three power meters; the incident-power density and polarization effects can also be measured. A network analyzer will provide the scattering parameters (S-parameters) values if connected, so as the reflection and transmission information can be obtained, when the cell is unloaded or loaded by the biological sample. Special attention must be given to the tapered transitions of the TEM cell, to ensure good impedance matches. Impedance mismatches cause standing waves in the chamber that may not be detected by power meters at the input and output ports. One can detect mismatches either by measuring time-domain reflection or by determining the E- and H-fields inside the chamber. In every case, it is necessary to map the fields inside the chamber so as to ensure single-mode operation. The MWs (gigahertz range) penetration depth inside an exposed biological sample is in the order of centimeters, and the inner electric field distribution, required for the dosimetric analysis, is currently non-uniform. Direct measurements of electric field strength and SAR at any location inside the exposed biological sample are almost impossible to be performed with adequate accuracy. In parallel to the experimental approach, the dosimetric characterization of the TEM cell may be obtained by using a theoretical approach. Numerical modeling is the technique able to provide complementary information to the experiment. A preliminary phase of the dosimetric study should therefore be the design and validation of the numerical model, able to simulate the experimental conditions. The

computational model provides complementary data to the experiment; it could be used for a proper correlation among exposure parameters (test preparation) and for extending the processing of the results. Numerical model Our study focuses on the TEM cell numerical model description and validation, followed by the evaluation of the EMF parameters inside the cell. Most EMF models of TEM cells refer only to the central rectangular part, where a TEM modal structure or a static field distribution is currently assumed [1, 3]. However, numerical techniques are able to model the entire cell geometry and different time-variation working conditions (useful especially when the quality of the electric field is assessed) as, for example, in [2] and [4], where the finite-difference time-domain (FDTD) method is used, or in [5] where a finite element method (FEM) model is referred. The FEM implemented by the commercial COMSOL Multiphysics [6] is used in our work for the generation of the numerical model that simulates the TEM cell (model IFI CC 104 SEXX) available to us for experimental dosimetry tests. The TEM cell has the geometry and dimensions showed in fig. 1 and table 1 (middle column). Our 3D FEM model is able to represent either the whole construction, or half of it, when longitudinal symmetry is considered. Both the harmonic and the time-variable regime are analyzed. The left end introduces the source through a port boundary condition and the right end is modeled through an adapted impedance boundary condition. The metallic enclosure and the median conductive septum are considered perfect electric conductors. The biological sample is placed near the bottom of the cell or above the septum, in the median region. Table 1 TEM cell dimensions TEM cell TEM [mm] model cell IFI CC 104 model in SEXX paper [2] A 450 300 B 450 80 C 450 136 L 850 564 a 25 21 b 25 19 c 19 14 a1=a2 225 140 b1=b2 224 39.5 b3 380 100 d 2 1 d1=d2 200 132 g 35 18 Fig. 1 The geometry of the TEM cell The validation of the numerical model was performed against a set of theoretical results given by Popovic et al. [2]. The geometric characteristics of the model introduced in [2] are specified in table 1 (last column). The electric field strength distribution (fig. 2 in [2]) and the voltage standing wave ratio (VSWR 1.25, fig. 2 in [2]) in the un loaded cell, as well as the SAR distribution in a rectangular

enclosure filled with biologic material, are the results referred in the cited work and verified by our 3D FEM model, giving a very good agreement. VSWR is computed by our 3D FEM model, as indicated in the referred paper, from the snapshots of the Ez-component of the electric field strength, taken one-quarter cycle apart in time (at 0.837 GHz), along the longitudinal axis of the cell and 4 mm distance above the septum. TEM cell parameters analysis The presented TEM cell (model IFI CC 104 SEXX, fig. 1 and table 1) was primarily evaluated from the perspective of impedance matching and inner electric field uniformity. A preliminary analysis, based on the expressions given in [1], determines the characteristic impedance of the cell Z 0 = 51.45 " and the cut-off frequency f c = 0.333 GHz for the first order propagating mode TE 10, which sets the superior limit for TEM wave-mode propagation. However, the dosimetric investigation that we need to perform with the TEM cell requires higher frequencies exposure of the biological samples. This is the reason for evaluation the cell characteristics in the frequency range of (0.8... 1.8) GHz. A set of measurements was made for the S-parameters determination by using a PNA-L network analyzer model N5230A-Agilent (10 MHz to 40 GHz) connected to the TEM cell feeding port, with the end port connected to a matched impedance of 50 ohm. We compared the VSWR experimental and numerical results for several working frequencies within the range (0.8... 1.8) GHz. Fig. 2 shows the measured and computed VSWR values; the percentage differences fall within a 25% interval, considered here as an acceptable tolerance limit. Fig. 2 VSWR in the modeled TEM cell - measured versus computed values Electric field uniformity assessment The technical specification of the cell recommends to virtually enclose the exposed sample in a rectangular test volume (RTV) located either on the septum or on the metallic bottom of the cell, in the central area; its dimensions should not exceed one third of the volume between the septum and the walls of the TEM cell; 1 3 A " 1 3 C " 1 3 b2 represent 150 "150 " 75 (in mm) in the x, y, z directions. Our study primarily investigates the uniformity of the time harmonic electric field in the RTV, at the working frequency of 0.9 GHz, which is important for a dosimetric analysis focused on the study of MWs bio-effects observed on several samples of cereal seeds, prepared for EMF exposure in the RTV.

The EMF solution shows that only the Ez component of the electric field (component of E along the z axis, perpendicular to the septum and to the propagation direction) is significant within the RTV. This assertion is based on the electric field spectrum-plot visualization and on a quantitative estimate of Ex, Ey and Ez components of the electric field strength in the RTV. Fig. 3 shows the Ez spectrum in two slices: a cross-section perpendicular to the longitudinal axis of the cell (left) and a longitudinal plane of symmetry (right); the spectrum displayed here is limited to values in the range ±100 V/m; consequently, the region surrounding the septum margins is eliminated due to the extreme values caused by the discontinuities at the edges. In such conditions, the area of quasiuniformity of the Ez field is better evidenced by the almost uniform color above the septum, in the central region of the cell. It coincides roughly with the RTV defined earlier. Fig. 3 Ez-field spectrum for the uniformity analysis (P in = 0.4 W, f = 0.9 GHz) The three E-field components were compared in the RTV region, and fig. 4 shows Ex, Ey and Ez along an axis parallel to the septum, at 25 mm height, in the transversal (left) and correspondingly longitudinal (right) slices, defined above; the Ex and Ey components become more important against Ez component as the distance from the septum grows. Fig. 4 Ex, Ey, Ez - components of the electric field strength at 25 mm above the septum in the slices displayed by fig. 3 (P in = 0.4 W, f = 0.9 GHz) For a quantitative assessment of the field uniformity, fig. 5 shows the distribution of Ez - component inside the RTV region, along a centered transversal y-axis (left) and along a centered longitudinal x-axis (right) at three heights (h1=20mm, h2=40mm, h3=60mm, measured from the surface of the septum). The uniformity of the electric field is evaluated here with regard to the

average value of Ez inside the RTV, Ez med = 51 V/m (all values are rated to Ez med ). A similar analysis is performed when the RTV is placed on the bottom of the cell (the TEM cell is reversed from its position in fig 1, as will probably be the setting in our testing program); fig. 6 shows similar Ez distributions as fig. 5, but the three heights are measured from the bottom (conductive wall) of the TEM cell. In this case, Ez med = 29 V/m, and one can observe that Ez distribution inside the RTV leads, for both settings, to values that may be different from Ez med with up to ± 40 %. Depending on the culture dish or biological sample dimensions and shape, one could choose the proper setting for the experiment. Fig. 5 Ez - component distribution inside the RTV, at three heights, along a transversal axis (left) and a longitudinal axis (right), when the RTV is placed on the septum (f = 0.9 GHz) Fig. 6 Ez - component distribution inside the RTV, at three heights, along a transversal axis (left) and a longitudinal axis (right), when the RTV is placed on the bottom of the cell (f = 0.9 GHz) We have further evaluated the Ez distribution when considering the presence of absorbing material on the interior conductive walls of the cell. Six rectangular thin ferrite plates, 100 "100 " 8 (in mm) are fixed on the conductive cell walls, as fig. 7a suggests. When taking into account this supplementary configuration in the computational 3D FEM model, the problem dimensions augment. For an estimate of the necessity of considering the ferrite plates, we compared the electric field configurations for the model with and without the absorbing plates. The ferrite plates are considered as homogeneous and isotropic sub-domains, and the properties adopted here (at the working frequency of 0.9 GHz) are as follows: 13 and 2.3 for the relative electric permittivity and magnetic permeability and 0.108 S/m for the electric conductivity. Fig. 7a shows the Ez-component of the electric field strength in a cross-sectional slice, for the cell with ferrite plates, when the cell

is fed at 0.4 W and 0.9 GHz. In fig. 7b the distribution of the Ez - field component is presented inside the RTV region, when placed on the bottom of the cell. Fig. 7a should be compared with fig. 3a, while fig. 7b should be compared with fig. 6 (left). Even though the presence of the ferrite absorbing plates reduces the amplitude of the electric field (Ez med = 21 V/m inside the RTV), it clearly improves the uniformity of the Ez-component. The dispersion of Ez values around Ez med inside the RTV is in the range ± 25%. a. Ez - spectrum in a cross-sectional slice b. Ez - distribution along a transversal axis, at three heights, inside the RTV placed on the bottom of the cell Fig. 7 Ez-component of the electric field strength for the cell with ferrite plates (P in = 0.4 W, f = 0.9 GHz) Conclusions We presented in this paper the results of an evaluation study performed with a numerical 3D FEM model of a TEM cell, available for dosimetric studies on biological samples exposed to MWs. The accuracy and completeness of the numerical model is evaluated through several tests that imply validation against data published in the literature and experimental results. The evaluation of scattering parameters and the assessment of electric field uniformity in the region used for testing provide data useful for the design of the dosimetric study. The research will continue for other frequencies and with a biological sample placed inside the cell. Acknowledgment. The work presented here is supported through the research CEEX projects code PC-D06- PT10-464/2005 and PC-D11-PT14-258/2005 funded by the Romanian Ministry of Education and Research. References [1] M. L. Crawford, J. L. Workman, C. L. Thomas, Expanding the Bandwidth of TEM Cells for EMC Measurements, IEEE Trans. on EMC, vol. 20, no. 3, pp 368-375, 1978 [2] M. Popovic, S. C. Hagness, A. Taflove, Finite-Difference Time-Domain Analysis of a Complete Transverse Electromagnetic Cell Loaded with Liquid Biological Media in Culture Dishes, IEEE Trans. on BME, vol. 45, no. 8, pp 1067-1076, 1998 [3] K. Malaric, J. Bartolic, Design of a TEM-Cell with Increased Usable Test Area, Turk. J. Elec. Engin., vol.11, NO.2, pp 143-154, 2003 [4] O. Franek, V. Navratil, Z. Raida, Analysis of Gigahertz TEM Cell using Finite-Difference Time-Domain (FDTD) Method, 13th International Conference Radioelektronika, Brno, Czech Republic, 2003 [5] M. M. G. D Amico, Loaded TEM Cell Versus Free Space: Comparison of the E-Fields Inside Dielectric Spherical Objects, IEEE Trans. on EMC, vol. 41, no. 2, pp 158-160, 1999 [6] COMSOL Multiphysics, trademark of COMSOL AB, is a modeling package for the simulation of physical processes described with PDEs