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- fMRI (5) (entfernen)
Studien zeigen, dass sowohl die genetische Prädisposition als auch Umweltfaktoren zu häufigen Erkrankungen - wie Schmerzerkrankungen oder psychiatrischen Störungen - beitragen. Molekulargenetische Studien legen nahe, dass ein Teil der Erblichkeit in häufigen genetischen Varianten zu finden ist. Die Untersuchung des Zusammenwirkens dieser Faktoren kann das Verständnis der Ätiologie dieser Erkrankungen erweitern, und neue Präventions- und Behandlungsansätze hervorbringen. In der vorliegenden Arbeit werden vier Studien präsentiert, in denen Umwelt- und genetische Risikofaktoren für psychische Erkrankungen und Schmerz untersucht wurden: In der ersten Studie (Kapitel II) wurden mögliche Wirkmechanismen von etablierten Risikofaktoren für psychiatrische Störungen " das Aufwachsen und Leben in städtischer Umgebung " mit bildgebenden Verfahren untersucht. Einen möglichen Mechanismus stellt der erhöhte soziale Stress in städtischer Umgebung dar. In dieser Studie unterliefen zwei Stichproben von gesunden Probanden zwei verschiedene soziale Stressparadigmen für die Anwendung im fMRT, wovon eines im Rahmen dieser Doktorarbeit entwickelt wurde (ScanSTRESS). Hierbei zeigte sich eine erhöhte Amygdalaaktivität bei Probanden, welche aktuell in der Stadt lebten, während die Aktivität des perigenualen anterioren Cingulums mit dem Aufwachsen in der Stadt assoziiert war. Diese Befunde legen nahe, dass die akute Stressverarbeitung durch Umweltfaktoren in sensiblen Phasen der Entwicklung des Nervensystems beeinflusst wird. In der zweiten Studie (Kapitel III), wurde die Modulierung des Einflusses der städtischen Umwelt auf die Stressverarbeitung durch eine Einzelnukleotid-Polymorphismus (SNP; rs324981) im Gen, welches für den Neuropeptid S (NPS) Rezeptor kodiert (NPSR1), untersucht. In einer Stichprobe, welche das ScanSTRESS-Paradigma absolvierte, konnte gezeigt werden, dass rs324981 " in Interaktion mit städtischem Aufwachsen " die Aktivität der rechten Amygdala beeinflusste. Diese Resultate legen nahe, dass das NPS-System in der menschlichen Stressreaktion involviert ist, und diese in Interaktion mit Umweltfaktoren beeinflusst. In der dritten Studie (Kapitel IV), wurde der Effekt der genetischen Variation von NPSR1 auf die zentralnervöse und endokrine Stressverarbeitung weitergehend untersucht. Da sowohl die Stressregulation, als auch psychiatrische Störungen stark geschlechtsspezifische Ausprägungen aufweisen, wurde die Interaktion von genetischer Variation in NPSR1 mit dem Geschlecht berücksichtigt. Hierfür wurde eine Stichprobe von 277 Probanden mit dem Trierer Sozialen Stresstest (TSST) und eine Stichprobe von 65 Probanden mit dem ScanSTRESS-Paradigma untersucht. Die Analyse zeigte die geschlechtsspezifische Assoziation einer Allel-Kombination (Haplotyp) von drei funktionalen SNPs (rs2530547, rs324981 und rs727162) mit der Cortisolantwort auf den TSST, und einen geschlechtsspezifischen Effekt von rs324981 auf die zentralnervösen Aktivierungsmuster. Diese Ergebnisse legen nahe, dass das Geschlecht die Effekte von genetischer Variation im NPS-System auf die Stressregulation moduliert. In der vierten Studie (Kapitel V), wurde der Einfluss der genetischen Prädisposition und Umweltfaktoren auf chronischen Schmerz nach einer Amputation untersucht. Hierfür wurde eine Studie an 122 Individuen durchgeführt, bei welchen zwei Gliedmaßen amputiert wurden. Das Auftreten und die Intensität von sowohl Phantom- als auch Stumpfschmerzen zeigten einen starken Zusammenhang mit der Ausprägung des selben Schmerztyps zwischen den beiden amputierten Körpergliedern, es waren aber nur moderate Zusammenhänge zwischen den beiden Schmerzarten zu beobachten. Dieses Ergebnis legt den Einfluss von sowohl spezifischen, als auch gemeinsamen (potentiell genetischen) Risikofaktoren für beide Schmerztypen nahe.
The human brain is characterised by two apparently symmetrical cerebral hemispheres. However, the functions attributed to each half of the brain are very distinct with a relative specialisation of the left hemisphere for language processing. Most laterality research has been performed on a behavioural level, using techniques such as visual half-field presentation. The visual half-field technique involves the presentation of stimuli in the left or right visual field for a very short time (about 200 ms). During the presentation of lateralized stimuli, the gaze of the participants is fixated on a centrally presented fixation cross. This technique takes advantage of the anatomy of the visual pathway as the temporal hemiretinae project ipsilateral, while the nasal hemiretinae project contralateral. Thus, stimuli presented in the left or right visual field are initially processed in the contralateral hemisphere. Language organisation can also be directly investigated using functional magnetic resonance imaging (fMRI). Both behavioural and neuroimaging studies showed that about 95% of right-handed men have a left hemispheric specialisation for language. In contrast, data on language organisation in women are ambiguous. It is supposed that this ambivalent picture might be associated with changes in gonadal steroid levels in blood during the menstrual cycle. However, gonadal steroid effects are complex and their role in functional cerebral lateralization is still open to discussion. The aim of this PhD project was to investigate, using fMRI: (1) the processing of linguistic information initially received in the specialised, non-specialised or both hemispheres; (2) linking the associated brain activation pattern with progesterone levels during the menstrual cycle. Firstly, brain activation was measured in 16 right-handed, healthy males during processing of different components of language (orthography, phonology and semantics) after reception in the left, right or both hemispheres. Secondly, to investigate changes in language organisation during the menstrual cycle, we conducted an event-related fMRI study during semantic and phonological processing also using visual half-field and central presentation of linguistic stimuli. Our results revealed higher BOLD signal intensity change in the visual cortex contralateral to the visual field of stimulus presentation compared to the ipsilateral visual cortex reflecting the crossing of visual pathways. We also found support for the hypothesis that the superiority of word recognition in the left VWFA is the result of a reduced activity in the right VWFA under left hemispheric control. Further, linguistic information received in the subdominant RH, is interhemispheric transferred to the left hemisphere for phonological processing. Semantic processing in contrast occurs in the specialised and in the non-specialised hemisphere. For the group of women, data analysis revealed that during semantic processing, salivary progesterone levels correlated positively with brain activity of the left superior frontal gyrus, left middle and inferior occipital gyri and bilateral fusiform gyrus. In contrast, the brain activation pattern for phonological processing did not change significantly across the menstrual cycle. In conclusion, the effect of serum progesterone levels on brain activity is task and region specific.
This thesis presents a study of the visual change detection mechanism. This mechanism is thought to be responsible for the detection of sudden and unexpected changes in our visual environment. As the brain is a capacity limited system and has to deal with a continuous stream of information from its surroundings only a part of the vast amount of information can be completely processed and be brought to conscious awareness. This information, which passes through attentional filters, is used for goal-directed behaviour. Therefore, the change detection mechanism is a very useful aid to cope with important information which is outside the focus of our attention. rnIt is thought that a neural memory trace of repetitive visual information is stored. Each new information input is compared to this existing memory trace by a so-called change or mismatch detection system. Following a sudden change, the comparison process leads to a mismatch and the detection system elicits a warning signal, to which an orienting response can follow. This involves a change in the focus of attention towards this sudden environmental change which can then be evaluated for potential danger and allows for a behavioural adaptation to the new situation. rnTo this purpose a paradigm was developed combining a 2-choice response time task with in the background a mismatch detection task of which the subjects were not aware. This paradigm was implemented in an ERP and an fMRI study and was used to study the the change detection mechanism and its relationship with impulsivity.rnIn previous studies a change detection system for auditory information had already been established. As the brain is a very efficient system it was thought to be unlikely that this change detection system is only available for the processing of auditory information. rnIndeed, a modality specific mismatch response at the sensory specific occipital cortex and a more general response at the frontocentral midline, both resembling the components shown in auditory research, were found in the ERP study.rnAdditionally, magnetic resonance imaging revealed a possible functional network of regions, which responded specifically to the processing of a deviant. These regions included the occipital gyrus, premotor cortex, inferior frontal cortex, thalamas, insula, and parts of the cingular cortex. rnThe relationship between impulsivity measures and visual change detection was established in an additional study. More impulsive subjects showed less detection of deviant stimuli, which was most likely due to too fast and imprecise information processing.rnIn summary it can be said, that the work presented in this thesis demonstrates that visual mismatch negativity was established, a number of regions could be associated with change detection and additionally the relevance of change detection in information processing was shown.rn
Although it has been demonstrated that nociceptive processing can be modulated by heterotopically and concurrently applied noxious stimuli, the nature of brain processes involved in this percept modulation in healthy subjects remains elusive. Using functional magnetic resonance imaging (fMRI) we investigated the effect of noxious counter-stimulation on pain processing. FMRI scans (1.5 T; block-design) were performed in 34 healthy subjects (median age: 23.5 years; range: 20-31 yrs.) during combined and single application (duration: 15 s; ISI=36 s incl. 6 s rating time) of noxious interdigital-web pinching (intensity range: 6-15 N) and contact-heat (45-49 -°C) presented in pseudo-randomized order during two runs separated by approx. 15 min with individually adjusted equi-intense stimuli. In order to control for attention artifacts, subjects were instructed to maintain their focus either on the mechanical or on the thermal pain stimulus. Changes in subjective pain intensity were computed as percent differences (∆%) in pain ratings between single and heterotopic stimulation for both fMRI runs, resulting in two subgroups showing a relative pain increase (subgroup P-IN, N=10) vs. decrease (subgroup P-DE, N=12). Second level and Region of Interest analysis conducted for both subgroups separately revealed that during heterotopic noxious counter-stimulation, subjects with relative pain decrease showed stronger and more widespread brain activations compared to subjects with relative pain increase in pain processing regions as well as a fronto-parietal network. Median-split regression analyses revealed a modulatory effect of prefrontal activation on connectivity between the thalamus and midbrain/pons, supporting the proposed involvement of prefrontal cortex regions in pain modulation. Furthermore, the mid-sagittal size of the total corpus callosum and five of its subareas were measured from the in vivo magnetic resonance imaging (MRI) recordings. A significantly larger relative truncus size (P=.04) was identified in participants reporting a relative decrease of subjective pain intensity during counter-stimulation, when compared to subjects experiencing a relative pain increase. The above subgroup differences observed in functional and structural imaging data are discussed with consideration of potential differences in cognitive and emotional aspects of pain modulation.
Magnet Resonance Imaging (MRI) and Electroencephalography (EEG) are tools used to investigate the functioning of the working brain in both humans and animal studies. Both methods are increasingly combined in separate or simultaneous measurements under the assumption to benefit from their individual strength while compensating their particular weaknesses. However, little attention has been paid to how statistical analyses strategies can influence the information that can be retrieved from a combined EEG fMRI study. Two independent studies in healthy student volunteers were conducted in the context of emotion research to demonstrate two approaches of combining MRI and EEG data of the same participants. The first study (N = 20) applied a visual search paradigm and found that in both measurements the assumed effects were absent by not statistically combining their results. The second study (N = 12) applied a novelty P300 paradigm and found that only the statistical combination of MRI and EEG measurements was able to disentangle the functional effects of brain areas involved in emotion processing. In conclusion, the observed results demonstrate that there are added benefits of statistically combining EEG-fMRI data acquisitions by assessing both the inferential statistical structure and the intra-individual correlations of the EEG and fMRI signal.