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Increasing Brain Acidity May Reduce Anxiety


Animal study highlights potential new target for treating anxiety disorders

Increasing acidity in the brain’s emotional control center reduces anxiety, according to an animal study published February 26 in The Journal of Neuroscience. The findings suggest a new mechanism for the body’s control of fear and anxiety, and point to a new target for the treatment of anxiety disorders.

Anxiety disorders, which are characterized by an inability to control feelings of fear and uncertainty, are the most prevalent group of psychiatric diseases. At the cellular level, these disorders are associated with heightened activity in the basolateral amygdala (BLA), which is known to play a central role in emotional behavior.

Many cells in the BLA possess acid-sensing ion channels called ASIC1a, which respond to pH changes in the environment outside of the cell. Maria Braga, DDS, PhD, and colleagues at the Uniformed Services University of the Health Sciences, F. Edward Hébert School of Medicine, found that activating ASIC1a decreased the activity of nearby cells and reduced anxiety-like behavior in animals. These findings add to previous evidence implicating the role of ASIC1a in anxiety.

“These findings suggest that activating these channels, specifically in fear-related areas such as the amygdala, may be a key to regulating anxiety,” explained Anantha Shekhar, MD, PhD, who studies panic disorders at Indiana University and was not involved in this study. “Developing specific drugs that can stimulate these channels could provide a new way to treat anxiety and fear disorders such a post-traumatic stress and panic disorders.”

To determine the effect ASIC1a activation has on neighboring cells, Braga’s group bathed BLA cells in an acidic solution in the laboratory and measured the signals sent to nearby cells. Lowering the pH of the solution decreased the activity of cells in the BLA.

Activating ASIC1a also affected animal behavior. When the researchers administered a drug that blocks ASIC1a directly into the BLA of rats, the rats displayed more anxiety-like behavior than animals that did not receive the drug. In contrast, when rats received a drug designed to increase the activity of ASIC1a channels in the BLA, the animals displayed less anxiety-like behavior.

“Our study emphasizes the importance of identifying and elucidating mechanisms involved in the regulation of brain function for the development of more efficacious therapies for treating psychiatric and neurological illnesses,” Braga said. While the findings suggest that drugs targeting ASICs may one day lead to novel therapies for anxiety disorders, Braga noted that “more research is needed to understand the roles that ASIC1a channels play in the brain.”

Link to the article:

The Journal of Neuroscience

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Dorsoventral vs. Septotemporal hippocampus

April 29, 2011 Leave a comment

Everybody knows what the hippocampus is for: memory. And…maybe something about anxiety or depression? Yes – over the last 10 years or so many studies have been published showing that the hippocampus has these two roles and that the mnemonic and emotional functions of the hippocampus are associated with its septal (dorsal) and temporal (ventral) ends, respectively. This new knowledge means that we’ve had to reorient our perspective. What we see when we consider the septal hippocampus may not be the same if we only consider its temporal end. My goal here is not to provide a review of the memory vs. emotional functions of the hippocampus (btw this dichotomy is a vast oversimplification). Instead, I’d like to talk about how people have differentiated these two ends of the hippocampus in their analyses. I’m also happy to showcase a bunch of pretty anatomical images that will probably never be published in a traditional journal article.

Some studies showing different functions of septal and temporal hippocampus

  • Some of the best reviews of the topic are by Bannerman et al from 2004 and 2011.
  • A recent and free review article by Fanselow and Dong.
  • Classic Moser papers showing spatial memory is more dependent on dorsal hippocampus and anxiety/fear behavior on ventral hippocampus
  • recent paper suggesting that spatial processing in the septal hippocampus meets the behavioral-control functions of the temporal hippocampus to enable rapid spatial learning

History of neurogenesis quantification. So, back in the day, before I even knew what a neuron was, and before it was well-established that there was functional differentiation along the hippocampal axis, people would pick a few sections from the dorsal hippocampus (it’s much more photogenic, gets all the glory), count new neurons, and make it a density measurement. Then the stereology police arrived (seriously, that’s what they’re called) and pointed out that changes in tissue volume or cell packing could change density measurements without there being any differences in numbers of cells. Stereological analyses also prevent any biases that might arise from creating arbitrary boundaries when examining only part of the hippocampus. And so people started doing stereological counts, which require a systematic quantification throughout the entire hippocampus. My guess is that this probably delayed the appreciation that neurogenesis could vary in magnitude and function along the hippocampal axis. Now that we know that stereology is pointless we can get back to business (this is a joke – please don’t arrest me).

Difficulty of quantifying subregions due to curvature of the hippocampus. One of the reasons the hippocampus is such a popular neurobiological model is its anatomy – the dentate gyrus, CA3 and CA1 subfields are all composed of tightly packed cells that are easy to identify. Thinking of the hippocampus along its long axis, one end projects to the septum and the other abuts the temporal lobe, hence “septotemporal” is technically the most accurate way to refer to the different ends of the hippocamus. The hippocampus is curved in such a way that you can actually cut it along any of the 3 spatial planes (X, Y, Z aka coronal, horizontal, saggital) and hit the hippocampus perpendicular to the septotemporal axis somewhere, giving rise to the classic the trisynaptic circuit. However, because of this same curvature, sectioning the brain in only one of the three planes means that some portion of the hippocampus is not going to be cut perpendicular to the long axis, producing sections in which septotemporal coordinates are hard to define.

The 3D nature of the hippocampus using images from the Allen Brain Explorer:

Figure 1: The dentate gyrus subfield of the hippocampus (i.e. green banana), from its septal pole, extends caudally and laterally and then ventrally. Green axis=dorsoventral, red=rostrocaudal, yellow=mediolateral.

Figure 2: A relatively caudal coronal section with the 3D dentate gyrus shown in the left panel, for comparison. This section contains ventral dentate gyrus (at the bottom, by “temporal”) but, at the top of the section, it also contains a portion of the dentate gyrus that is very dorsal, despite being far from the septal pole.

Figure 3: This section is more caudal than the previous example, yet the dentate granule cells (white patches within the bright green region) do not extend as far in the ventral direction. So, more caudal ≠ more ventral.

Others on the curvature problem:

Schlessinger et al., 1975: Since the dentate gyrus follows the general curvature of the hippocampal formation, it is difficult to apply the usual topographical terms to its various parts. The rostral third or half of the gyrus is more-or-less horizontally disposed within the cerebral hemisphere…At about the junction of its rostral and caudal halves the gyrus is sharply flexed upon itself, and comes to be vertically disposed….Again, because of the flexure of the hippocampal formation, it is inappropriate to refer to the dentate gyrus as having a dorsal (or rostral) and a ventral (or caudal) part. Following Gottlieb and Cowan (’73) we shall refer to the long axis of the gyrus, extending from the temporal pole of the hemisphere to just behind the septal region, as its temporalseptal axis.

Amaral & Witter, 1989: Because of its complex three-dimensional shape, normal sections of the hippocampus, i.e. those oriented perpendicular to the long axis, are obtained for only a small part of its septotemporal extent in standard coronal or horizontal sections. This situation severely complicates the analysis of the connections within the hippocampal formation.

De Hoz et al., 2003: In discussing different regions of the hippocampus, we use the terms “septal” and “temporal” to refer to the rostralmost and the ventralmost poles of the longitudinal axis, respectively, because this terminology allows an even division of this axis into septal and temporal halves. The terms “dorsal” and “ventral” are sometimes used to refer to the same areas; the dorsal hippocampus is, however, more extensive than the ventral.

So how can we divide the hippocampus? Many people work with coronal sections. Can we delineate boundaries between different hippocampal subregions in coronal sections? Banasr et al. has described a reproducible method for separating dorsal from ventral hippocampus using coronal sections. Here, the dorsal regions would contain a fair bit of mid-septotemporal hippocampus but indeed, only the dorsal sections would contain septal hippocampus and only ventral sections would contain temporal hippocampus:

Figure 4: Separating dorsal and ventral hippocampus in coronal sections

Jayatissa et al. has horizontally sectioned the rat brain and then used anatomical coordinates to divide dorsal from ventral. This seems to be a good way to isolate pure, septal hippocampus but dorsal measures would again blur together the septal and mid-septal regions.

What if we wanted to separate the septal and temporal ends of the hippocampus? One method, described in Amaral & Witter, 1989 offers a solution:

We have adopted a strategy first described by Gaarskjaer that obviates this problem. In short…the fixed hippocampal formation is dissected from the brain and gently extended before histological processing. In this way the extended hippocampus can be positioned such that normal sections are obtained from much of the septotemporal extent of the structure.

A similar approach had been used (see here and here). One drawback is that you ruin much of the rest of the brain during the dissection process (insert but-who-cares-about-the-rest-of-the-brain joke here). Here’s a figure from thesis that illustrates the similar-shaped hippocampal slices obtained with this method:

Figure 5: DAPI counterstained sections, evenly spaced across the septotemporal axis. Sampling scheme illustrated at the top. Shaded regions indicate how different septotemporal regions could be binned. S=suprapyramidal blade of the dentate gyrus, I=infrapyramidal blade, DG=dentate gyrus.

Another strategy isn’t too different from the method of Banasr, above. To get at the septal hippocampus you’re just being a bit more selective and only examining portions of the dorsal hippocampus that extend quite far rostrally. For the caudal sections that contain both dorsal and ventral hippocampus the rhinal fissure seems like a good guide – anything falling on the ventral side I’m counting as ventral.

But if you’re lazy…

A fast, revolutionary new method for examining the hippocampus along its full septotemporal axis in a single section! It almost sounds too good to be true. In fact, it is. But it provides some interesting pictures for those of you who have stuck with me this far.

Recently, a lot of rats has been irradiated to eliminate adult neurogenesis. Before coming to any conclusions about the behavioral data it was needed to know whether neurogenesis was completely blocked AND whether it was blocked throughout the entire dentate gyrus. Due to laziness to cut hundreds of sections for each rat, the hippocampus was extracted but instead of sectioning perpendicular to its septotemporal axis, it was sectioned parallel to, or along, its septotemporal axis by flattening and freezing it on a microtome stage. With this approach the entire dentate gyrus could be cut in about 30 sections and sections that had the entire septotemporal length of the dentate gyrus became present. Then they were stained for NeuN and DCX to visualize neurons and immature neurons, respectively. I think every other section was stained; one example is shown below.

Figure 6: Hippocampal sections stained for NeuN and DCX. The dentate gyrus can be identified as the layer of tightly-packed orange cells on the left, that are bordered by green DCX+ cells. Sections were cut from the side of the infrapyramidal blade towards the suprapyramidal blade (direction of cutting = section 1→9). Images were taken with a 20x objective and subsequently stitched together.

Is it really necessary to divide septotemporally? I guess it depends. Many studies that have focussed more on dorsal vs. ventral have made significant findings. If the anatomical method is well-described and reproducible, what more could you ask for? It’s possible, however, that combining different septotemporal regions into the same analysis could obscure a result. For example, when the activation of new neurons was examined after water maze training, it was found a steadily-increasing amount of activation as going from septal to temporal (see Figure 7). Had the 2 septal quartiles been pooled together and the 2 temporal quartiles pooled together, the observed difference would have been much smaller than when comparing the septalmost quartile with the temporalmost quartile.

Figure 7: The density of ‘activated’ new neurons (i.e. PSA-NCAM+ and Fos+) increased from septal to temporal. Note the mid-septal and mid-temporal regions were similar. Also note that I used D and V nomenclature, for ‘dorsal’ and ‘ventral’, despite repeatedly emphasizing in this post that ’septal’ and ‘temporal’ is more accurate.

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and now…

Pretty pictures from these sections!

Messy.

Just a nice example of some DCX dendrites.

DCX labeling outside of the dentate gyrus. I think this was in the subiculum but who can say for sure with these weird sections.

Septotemporal sample #1

Septotemporal sample #2

Septotemporal sample #3

Septotemporal sample #4

CRAB

ALLIGATOR

PUPPY / BIRDIE

Special thanks and credit to http://www.functionalneurogenesis.com and to Sarah Ferrante for sectioning, staining and imaging the tissue.