Dr.-Ing. Matthias Gräser

Universitätsklinikum Hamburg-Eppendorf (UKE)
Sektion für Biomedizinische Bildgebung
Lottestraße 55
2ter Stock, Raum 212
22529 Hamburg

Technische Universität Hamburg (TUHH)
Institut für Biomedizinische Bildgebung
Gebäude E, Raum 4.044
Am Schwarzenberg-Campus 3
21073 Hamburg

Tel.: 040 / 7410 25812
E-Mail: matthias.graeser(at)tuhh.de
E-Mail: ma.graeser(at)uke.de

Research Interests

  • Magnetic Particle Imaging
  • Low Noise Electronics
  • Inductive Sensors
  • Passive Electrical Devices

Curriculum Vitae

Matthias Gräser submitted his Dr.-Ing. thesis in january 2016 at the institute of medical engineering (IMT) at the university of Lübeck and is now working as a Research Scientist at the institute for biomedical imaging (IBI) at the technical university in Hamburg, Germany.  Here he develops concepts for Magnetic-Particle-Imaging (MPI) devices. His main aim is to improve the sensitivity of the imageing devices and improve resolution and application possibilities of MPI technology.

In 2011 Matthias Gräser started to work at the IMT as a Research Associate in the Magnetic Particle Imaging Technology (MAPIT) project. In this project he devolped the analog signal chains for a rabbit sized field free line imager. Additionally he developed a two-dimensional Magnetic-Particle-Spectrometer. This device can apply various field sequences and measure the particle response with a very high signal-to-noise ratio (SNR).

The dynamic behaviour of magnetic nanoparticles is still not fully understood. Matthias Gräser investigated the particle behaviour by modeling the particle behaviour with stochastic differential equations. With this model it is possible to simulate the impact of several particle parameters and field sequences on the particle response .

In 2010 Matthias Gräser finished his diploma at the Karlsruhe Institue of Technology (KIT). His diploma thesis investigated the nerve stimulation of magnetic fields in the range from 4 kHz to 25 kHz.

Journal Publications

Journal Publications

[183661]
Title: Saline bolus for negative contrast perfusion imaging in magnetic particle imaging.
Written by: F. Mohn, M. Exner, P. Szwargulski, M. Möddel, T. Knopp, and M. Graeser
in: <em>Physics in Medicine & Biology</em>. aug (2023).
Volume: <strong>68</strong>. Number: (17),
on pages: 5026
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ISBN: 0031-9155, 1361-6560
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DOI: 10.1088/1361-6560/ace309
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[BibTex]

Note: article, openaccess

Abstract: Magnetic Particle Imaging is capable to measure the spatial distribution of magnetic nanoparticles with high temporal resolution. As a quantitative tracer based imaging method, the signal is linear in the tracer concentration for any location that contains nanoparticles and zero in the surrounding tissue which does not provide any intrinsic signal. After tracer injection, the concentration over time (positive contrast) can be utilized to calculate dynamic diagnostic parameters like perfusion parameters in vessels and organs, which are an important tool in medical diagnosis. Every acquired perfusion image thus requires a new bolus of tracer with a sufficiently large iron dose to be visible above the background. We propose a method, where a bolus of physiological saline solution without any particles (negative contrast) displaces the remaining steady state concentration which in turn contributes to the image contrast. Perfusion parameters are calculated based on the time response of this negative bolus and compared to a positive bolus. Results from phantom experiments show that normalized signals from positive and negative boli are concurrent and deviations of calculated perfusion maps are low. Our method opens up the possibility to increase the total monitoring time of a future patient by utilizing a positive-negative contrast sequence, while minimizing the iron dose per acquired image.

Conference Proceedings

Conference Proceedings

[183661]
Title: Saline bolus for negative contrast perfusion imaging in magnetic particle imaging.
Written by: F. Mohn, M. Exner, P. Szwargulski, M. Möddel, T. Knopp, and M. Graeser
in: <em>Physics in Medicine & Biology</em>. aug (2023).
Volume: <strong>68</strong>. Number: (17),
on pages: 5026
Chapter:
Editor:
Publisher:
Series:
Address:
Edition:
ISBN: 0031-9155, 1361-6560
how published:
Organization:
School:
Institution:
Type:
DOI: 10.1088/1361-6560/ace309
URL:
ARXIVID:
PMID:

[BibTex]

Note: article, openaccess

Abstract: Magnetic Particle Imaging is capable to measure the spatial distribution of magnetic nanoparticles with high temporal resolution. As a quantitative tracer based imaging method, the signal is linear in the tracer concentration for any location that contains nanoparticles and zero in the surrounding tissue which does not provide any intrinsic signal. After tracer injection, the concentration over time (positive contrast) can be utilized to calculate dynamic diagnostic parameters like perfusion parameters in vessels and organs, which are an important tool in medical diagnosis. Every acquired perfusion image thus requires a new bolus of tracer with a sufficiently large iron dose to be visible above the background. We propose a method, where a bolus of physiological saline solution without any particles (negative contrast) displaces the remaining steady state concentration which in turn contributes to the image contrast. Perfusion parameters are calculated based on the time response of this negative bolus and compared to a positive bolus. Results from phantom experiments show that normalized signals from positive and negative boli are concurrent and deviations of calculated perfusion maps are low. Our method opens up the possibility to increase the total monitoring time of a future patient by utilizing a positive-negative contrast sequence, while minimizing the iron dose per acquired image.