Volumetric Manganese Enhanced Magnetic Resonance Imaging in mice (mus musculus)

The present doctoral thesis introduces a method for semi-automatic volumetric analysis of the hippocampus and other distinct brain regions in laboratory mice. The method of volumetric manganese enhanced magnetic resonance imaging (vMEMRI) makes use of the paramagnetic property of the manganese ion, Mn2+, which results in a positive contrast enhancement of specific brain areas on the MR image and enables a more detailed image of brain morphology. The chemical similarity of Mn2+ to Calcium leads to an accumulation of Mn2+ in excited cells and consequentially an enhanced signal in certain brain regions in an activity dependent manner. However, one major drawback for vMEMRI is the toxicity of Mn2+. Therefore, the aims of the thesis have been: (1) Establishment of a MEMRI protocol in mice (2) Optimization of a Mn2+ application procedure to reduce toxic side effects (3) Development of an automatized method to determine hippocampal volume (4) Validation of vMEMRI analysis (5) Application of volumetric analysis in mouse models of psychopathology This thesis splits into 3 studies. Study 1 deals with Mn2+ toxicity and introduces an application method that considerably reduces the toxic side effects of Mn2+. Study 2 validates vMEMRI as a method to reliably determine hippocampal volume and explores its utilization it in animals with genetically and chemically modified hippocampi. Study 3 displays the application vMEMRI in a mouse model of a psychiatric disorder. Study 1 shows that a single application of Mn2+ in dosages used in current MEMRI studies leads to considerable toxic side effects measurable with physiological, behavioral and endocrine markers. In contrast, a fractionated application of a low dose of Mn2+ is proposed as an alternative to a single injection of a high dose. Repeated application of low dosages of 30 mg/kg Mn2+ showed less toxic side effects compared to the application schemes with higher dosages of 60 mg/kg. Additionally, the best vMEMRI signal contrast was seen for an injection protocol of 30 mg/kg 8 times with an inter-injection interval of 24 h (8x30/24 protocol). The impact of the 8x30/24 application protocol on longitudinal studies was tested by determining whether learning processes are disturbed. Mice were injected with the 8x30/24 protocol 2 weeks prior to receiving a single footshock. Manganese injected mice showed less contextual freezing to the shock context and a shock context reminder one month after shock application. Furthermore, mice showed increased hyperarousal and no avoidance of shock context related odors. This impairment in fear conditioning indicates a disturbed associative learning of Mn2+ injected mice. Therefore, it was investigated whether Mn2+ application shows a specific disturbance of hippocampus dependent learning. Mice were subjected to habitual and spatial learning protocols 12 h after each injection in a water cross-maze. There was no impairment in learning protocols which allowed for hippocampus-independent habitual learning. However, Mn2+ injected mice were specifically impaired in the hippocampus-dependent spatial learning protocol. Furthermore, it was shown that only mice with higher Mn2+ accumulation showed this impairment. Altogether, the results of this chapter argue for a fractionated application scheme such as 30 mg/kg every 24 h for 8 days to provide sufficient MEMRI signal contrast while minimizing toxic side effects. However, the treatment procedure has to be further improved to allow for an analysis of hippocampus-dependent learning processes as well. Because of the potential side effects, the vMEMRI method was applied as a final experiment in study 2 and 3. Study 2 introduces the method of vMEMRI, which allows, for the first time, an in vivo semi-automatic detection of hippocampal volume. Hippocampal volume of mice with genetically altered adult neurogenesis and those with chemically lesioned hippocampi could be analyzed with vMEMRI. Even the highly variable differences in hippocampal volume of these animals could be detected with vMEMRI. vMEMRI data correlated with manually obtained volumes and are in agreement with previously reported histological findings, indicating the high reliability of this method. Study 3 investigates the ability of vMEMRI to detect even small differences in brain morphology by examining volumetric changes of the hippocampus and other brain structures in a mouse model of PTSD supplemented with enriched housing conditions. It was shown, that exposure to a brief inescapable foot shock led to a volume reduction in both the left hippocampus and right central amygdala two months later. Enriched housing decreased the intensity of trauma-associated contextual fear independently of whether it was provided before or after the shock. vMEMRI analysis revealed that enriched housing led to an increase in whole brain volume, including the lateral ventricles and the hippocampus. Furthermore, the enhancement of hippocampal volume through enriched housing was accompanied by the amelioration of trauma-associated PTSD-like symptoms. Hippocampal volume gain and loss was mirrored by ex vivo ultramicroscopic measurements of the hippocampus. Together, these data demonstrate that vMEMRI is able to detect small changes in hippocampal and central amygdalar volumes induced by a traumatic experience in mice. In conclusion, vMEMRI proves to be very reliable and able to detect small volumetric differences in various brain regions in living mice. vMEMRI opens up a great number possibilities for future research determining neuroanatomical structure, volumes and activity in vivo as well as the ability to repeatedly determine such characteristics within each subject, given an improvement of the Mn2+ treatment protocols to minimize potential toxic side effects

Manganese-Enhanced Magnetic Resonance Imaging: Overview and Central Nervous System Applications With a Focus on Neurodegeneration

Manganese-enhanced magnetic resonance imaging (MEMRI) rose to prominence in the 1990s as a sensitive approach to high contrast imaging. Following the discovery of manganese conductance through calcium-permeable channels, MEMRI applications expanded to include functional imaging in the central nervous system (CNS) and other body systems. MEMRI has since been employed in the investigation of physiology in many animal models and in humans. Here, we review historical perspectives that follow the evolution of applied MRI research into MEMRI with particular focus on its potential toxicity. Furthermore, we discuss the more current in vivo investigative uses of MEMRI in CNS investigations and the brief but decorated clinical usage of chelated manganese compound mangafodipir in humans

Manganese-Enhanced Magnetic Resonance Imaging of the Spinal Cord in Rats

Manganese-enhanced magnetic resonance imaging (MEMRI) offers a novel neuroimaging method in visualizing the activity patterns of neural circuits. MEMRI is using the divalent manganese ion, which has been used as a cellular contrast agent. The present study was conducted to determine the contrast-enhancing effects of manganese ion administered into the spinal cord of rats. Manganese ion was administered into the spinal cord by lumbar puncture. Ex vivo magnetic resonance images were obtained at 6, 12, 24, and 48 hours after manganese ion injection. Although the highly contrasted images were not observed 6 or 12 hr after manganese injection, the distinctive manganese-enhanced images began to appear at 24 hours after manganese ion injection. These results suggest that the gray matter is the foci of intense paramagnetic signals and MEMRI may provide an effective technique to visualize the activity-dependent patterns in the spinal cordope

Monitoring dynamic calcium homeostasis alterations by T₁-weighted and T₁-mapping cardiac manganese enhanced MRI (MEMRI) in a murine myocardial infarction model

Manganese has been used as a T₁-weighted MRI contrast agent in a variety of applications. Because manganese ions (Mn²) enter viable myocardial cells via voltage gated calcium channels, manganese-enhanced MRI (MEMRI) is sensitive to the viability and the inotropic state of the heart. In spite of the established importance of calcium regulation in the heart both prior to, and following, myocardial injury, monitoring strategies to assess calcium homeostasis in affected cardiac tissues are limited. This study implements a T₁-mapping method to obtain quantitative information both dynamically and over a range of MnCl₂ infusion doses. In order to optimize the current manganese infusion protocols, both dose dependent and temporal washout studies were performed. A non-linear relationship between infused MnCl₂ solution dose and increase in left ventricular free wall relaxation rate (∆R₁) was observed. Control mice also exhibited significant manganese clearance over time, with approximately 50% decrease of ∆R₁ occurring in just 2.5 hours. The complicated efflux time dependence possibly suggests multiple efflux mechanisms. Using the measured relationship between infused MnCl₂ and ∆R₁, absolute Mn concentration ICP-MS data analysis provided a means to estimate the absolute heart Mn concentration in vivo. We have shown that this technique has the sensitivity to observe or monitor potential Ca²+ handling alterations in vivo due to the physiological remodeling following myocardial infarction. Left ventricular free wall ∆R₁ values were significantly lower (P = 0.005) in the adjacent zone, surrounding the injured myocardial tissue, than healthy left ventricular free wall tissue. This inferred reduction in Mn concentration can be used to estimate potentially salvageable myocardium in vivo for future therapeutic treatment or evaluation of disease progression.M.S.Committee Chair: Hu, Tom; Committee Co-Chair: Rahnema, Farzad; Committee Member: Wang, Chris; Committee Member: Yanasak, Natha

In vivo identification of brain structures functionally involved in spatial learning and strategy switch

Spatial learning is a complex behavior which includes, among others, encoding of space, sensory and motivational processes, arousal and locomotor performance. Today, our view on spatial navigation is largely hippocampus-centrist. Less is known about the involvement of brain structures up- and downstream, or out of this circuit. Here, I provide the first in vivo assessment of the neural matrix underlying spatial learning, using functional manganese-enhanced MRI (MEMRI) and voxel-wise whole brain analysis. Mice underwent place-learning (PL) vs. response-learning (RL) in the water cross maze (WCM) and its readout was correlated to the Mn2+ contrasts. Thus, I identified structures involved in spatial learning largely overlooked in the past, due to methods focused on region of interest (ROI) analyses. These structures include several sensory-related structures and differ between place-learners and response-learners, with the former (PL) comprising mostly structures involved in different properties of visual processing, such as horizontal gaze (e.g. nucleus prepositus) and saccade (e.g. fastigial nucleus), or provide vision-input and eye movement information from parahippocampal (e.g. presubiculum, perirhinal, postrhinal and ectorhinal areas) and other regions (e.g. orbital area, superior colliculus and vestibular ocular-reflex from the vestibular nucleus) likely to head-direction, grid- and place-cells; and the latter (RL) presenting structures related to more basic rodent sensory computations, like odor (e.g main and accessory olfactory bulb, cortical amygdala, piriform, endopiriform and postpiriform areas) and acoustic stimuli representation (e.g. auditory area, nucleus of the lateral lemniscus and superior olivary complex), or sensory-motor properties, such as body representation (e.g. somatosensory area – upper limbs) and head-direction signal. Add-on experiments pointed to preferential Mn2+ accumulation towards projection terminals, suggesting that our mapping was mostly formed by projection sites of the originally activated structures. This is corroborated by in-depth analysis of MEMRI data after WCM learning showing mostly downstream targets of the hippocampus. These differ between fornical afferences from vCA1 and direct innervation from dCA1/iCA1 (for PL), and structures along the longitudinal association bundle originating in vCA1 (for RL). To elucidate the pattern of Mn2+ accumulation seen on the scans, I performed c-fos expression analyses following learning in the WCM. This helped me identify the structures initially activated during spatial learning and its underlying connectivity to establish the matrix. Finally, to test the causal involvement of selected structures from our previous findings I inhibited them (through DREADDs) while mice performed the WCM task. I also focused on the causal involvement of the vHPC-mPFC circuit on strategy switch during WCM learning. I believe that this study might shed light into new brain structures involved in spatial learning and strategy switch and complement the current knowledge on these circuits’ connectivity. Moreover, I elucidated some functional mechanisms of MEMRI, clarifying the interpretation of data obtained with this method and its possible future applications

In vivo identification of brain structures functionally involved in spatial learning and strategy switch

Spatial learning is a complex behavior which includes, among others, encoding of space, sensory and motivational processes, arousal and locomotor performance. Today, our view on spatial navigation is largely hippocampus-centrist. Less is known about the involvement of brain structures up- and downstream, or out of this circuit. Here, I provide the first in vivo assessment of the neural matrix underlying spatial learning, using functional manganese-enhanced MRI (MEMRI) and voxel-wise whole brain analysis. Mice underwent place-learning (PL) vs. response-learning (RL) in the water cross maze (WCM) and its readout was correlated to the Mn2+ contrasts. Thus, I identified structures involved in spatial learning largely overlooked in the past, due to methods focused on region of interest (ROI) analyses. These structures include several sensory-related structures and differ between place-learners and response-learners, with the former (PL) comprising mostly structures involved in different properties of visual processing, such as horizontal gaze (e.g. nucleus prepositus) and saccade (e.g. fastigial nucleus), or provide vision-input and eye movement information from parahippocampal (e.g. presubiculum, perirhinal, postrhinal and ectorhinal areas) and other regions (e.g. orbital area, superior colliculus and vestibular ocular-reflex from the vestibular nucleus) likely to head-direction, grid- and place-cells; and the latter (RL) presenting structures related to more basic rodent sensory computations, like odor (e.g main and accessory olfactory bulb, cortical amygdala, piriform, endopiriform and postpiriform areas) and acoustic stimuli representation (e.g. auditory area, nucleus of the lateral lemniscus and superior olivary complex), or sensory-motor properties, such as body representation (e.g. somatosensory area ? upper limbs) and head-direction signal. Add-on experiments pointed to preferential Mn2+ accumulation towards projection terminals, suggesting that our mapping was mostly formed by projection sites of the originally activated structures. This is corroborated by in-depth analysis of MEMRI data after WCM learning showing mostly downstream targets of the hippocampus. These differ between fornical afferences from vCA1 and direct innervation from dCA1/iCA1 (for PL), and structures along the longitudinal association bundle originating in vCA1 (for RL). To elucidate the pattern of Mn2+ accumulation seen on the scans, I performed c-fos expression analyses following learning in the WCM. This helped me identify the structures initially activated during spatial learning and its underlying connectivity to establish the matrix. Finally, to test the causal involvement of selected structures from our previous findings I inhibited them (through DREADDs) while mice performed the WCM task. I also focused on the causal involvement of the vHPC-mPFC circuit on strategy switch during WCM learning. I believe that this study might shed light into new brain structures involved in spatial learning and strategy switch and complement the current knowledge on these circuits? connectivity. Moreover, I elucidated some functional mechanisms of MEMRI, clarifying the interpretation of data obtained with this method and its possible future applications

Applications of manganese-enhanced magnetic resonance imaging in neuroscience

xi, 84 leaves ; 29 cmManganese-Enhanced Magnetic Resonance Imaging (MEMRI) has proven itself to be a beneficial technique in the field of Neuroscience. This thesis applies MEMRI to studies in neuroscience by first establishing the limitations concerning the use of MEMRI in live rats. Experiment 1 used an osmotic pump for manganese (Mn) delivery to the lateral ventricles for acquisition of anatomical images using MEMRI. From my knowledge, this was the first method demonstrating slow infusion of Mn to the lateral ventricles. In Experiment 2, MEMRI was used for volumetric analysis the whole brain and hippocampus of prenatally stressed rats. To my knowledge, this study was the first to investigate the effect of generational prenatal stress on the structure of a rat’s brain using MEMRI and histology. Additionally, Experiment 2 investigated the use of a subcutaneous osmotic pump to deliver Mn for MEMRI. A summary on the use of MEMRI in Neuroscience concludes this thesis, with a discussion on the methods used and related technical considerations

Manganese-Enhanced Magnetic Resonance Imaging: Overview and Central Nervous System Applications With a Focus on Neurodegeneration

Manganese-enhanced magnetic resonance imaging (MEMRI) rose to prominence in the 1990s as a sensitive approach to high contrast imaging. Following the discovery of manganese conductance through calcium-permeable channels, MEMRI applications expanded to include functional imaging in the central nervous system (CNS) and other body systems. MEMRI has since been employed in the investigation of physiology in many animal models and in humans. Here, we review historical perspectives that follow the evolution of applied MRI research into MEMRI with particular focus on its potential toxicity. Furthermore, we discuss the more current in vivo investigative uses of MEMRI in CNS investigations and the brief but decorated clinical usage of chelated manganese compound mangafodipir in humans

Neurons in the primate medial basal forebrain signal combined information about reward uncertainty, value, and punishment anticipation

It has been suggested that the basal forebrain (BF) exerts strong influences on the formation of memory and behavior. However, what information is used for the memory-behavior formation is unclear. We found that a population of neurons in the medial BF (medial septum and diagonal band of Broca) of macaque monkeys encodes a unique combination of information: reward uncertainty, expected reward value, anticipation of punishment, and unexpected reward and punishment. The results were obtained while the monkeys were expecting (often with uncertainty) a rewarding or punishing outcome during a Pavlovian procedure, or unexpectedly received an outcome outside the procedure. In vivo anterograde tracing using manganese-enhanced MRI suggested that the major recipient of these signals is the intermediate hippocampal formation. Based on these findings, we hypothesize that the medial BF identifies various contexts and outcomes that are critical for memory processing in the hippocampal formation