Your search keyword '"Lateral Ventricles"' showing total 69 results

1. Function of Oncogene Mycn in Adult Neurogenesis and Oligodendrogenesis.

Author

Chen, Jiao, Chen, Jiao, Guan, Zhonghui, Chen, Jiao, Chen, Jiao, and Guan, Zhonghui

Abstract

Human MYCN is an oncogene amplified in neuroblastoma and many other tumors. Both human MYCN and mouse Mycn genes are important in embryonic brain development, but their functions in adult healthy nerve system are completely unknown. Here, with Mycn-eGFP mice and quantitative RT-PCR, we found that Mycn was expressed in specific brain regions of young adult mice, including subventricular zone (SVZ), subgranular zone (SGZ), olfactory bulb (OB), subcallosal zone (SCZ), and corpus callosum (CC). With immunohistochemistry (IHC), we found that many Mycn-expressing cells expressed neuroblast marker doublecortin (DCX) and proliferation marker Ki67. With Dcx-creER and Mki67-creER mouse lines, we fate mapped Dcx-expressing neuroblasts and Mki67-expressing proliferation cells, along with deleting Mycn from these cells in adult mice. We found that knocking out Mycn from adult neuroblasts or proliferating cells significantly reduced cells in proliferation in SVZ, SGZ, OB, SCZ, and CC. We also demonstrated that the Mycn-deficient neuroblasts in SGZ matured quicker than wild-type neuroblasts, and that Mycn-deficient proliferating cells were more likely to survive in SVZ, SGZ, OB, SCZ, and CC compared to wild type. Thus, our results demonstrate that, in addition to causing tumors in the nervous system, oncogene Mycn has a crucial function in neurogenesis and oligodendrogenesis in adult healthy brain.

Published

2022

2. GLI3 Is Required for OLIG2+ Progeny Production in Adult Dorsal Neural Stem Cells.

Author

Embalabala, Rebecca J, Embalabala, Rebecca J, Brockman, Asa A, Jurewicz, Amanda R, Kong, Jennifer A, Ryan, Kaitlyn, Guinto, Cristina D, Álvarez-Buylla, Arturo, Chiang, Chin, Ihrie, Rebecca A, Embalabala, Rebecca J, Embalabala, Rebecca J, Brockman, Asa A, Jurewicz, Amanda R, Kong, Jennifer A, Ryan, Kaitlyn, Guinto, Cristina D, Álvarez-Buylla, Arturo, Chiang, Chin, and Ihrie, Rebecca A

Abstract

The ventricular-subventricular zone (V-SVZ) is a postnatal germinal niche. It holds a large population of neural stem cells (NSCs) that generate neurons and oligodendrocytes for the olfactory bulb and (primarily) the corpus callosum, respectively. These NSCs are heterogeneous and generate different types of neurons depending on their location. Positional identity among NSCs is thought to be controlled in part by intrinsic pathways. However, extrinsic cell signaling through the secreted ligand Sonic hedgehog (Shh) is essential for neurogenesis in both the dorsal and ventral V-SVZ. Here we used a genetic approach to investigate the role of the transcription factors GLI2 and GLI3 in the proliferation and cell fate of dorsal and ventral V-SVZ NSCs. We find that while GLI3 is expressed in stem cell cultures from both dorsal and ventral V-SVZ, the repressor form of GLI3 is more abundant in dorsal V-SVZ. Despite this high dorsal expression and the requirement for other Shh pathway members, GLI3 loss affects the generation of ventrally-, but not dorsally-derived olfactory interneurons in vivo and does not affect trilineage differentiation in vitro. However, loss of GLI3 in the adult dorsal V-SVZ in vivo results in decreased numbers of OLIG2-expressing progeny, indicating a role in gliogenesis.

Published

2022

3. Subventricular zone/white matter microglia reconstitute the empty adult microglial niche in a dynamic wave.

Author

Hohsfield, Lindsay A, Hohsfield, Lindsay A, Najafi, Allison R, Ghorbanian, Yasamine, Soni, Neelakshi, Crapser, Joshua, Figueroa Velez, Dario X, Jiang, Shan, Royer, Sarah E, Kim, Sung Jin, Henningfield, Caden M, Anderson, Aileen, Gandhi, Sunil P, Mortazavi, Ali, Inlay, Matthew A, Green, Kim N, Hohsfield, Lindsay A, Hohsfield, Lindsay A, Najafi, Allison R, Ghorbanian, Yasamine, Soni, Neelakshi, Crapser, Joshua, Figueroa Velez, Dario X, Jiang, Shan, Royer, Sarah E, Kim, Sung Jin, Henningfield, Caden M, Anderson, Aileen, Gandhi, Sunil P, Mortazavi, Ali, Inlay, Matthew A, and Green, Kim N

Abstract

Microglia, the brain's resident myeloid cells, play central roles in brain defense, homeostasis, and disease. Using a prolonged colony-stimulating factor 1 receptor inhibitor (CSF1Ri) approach, we report an unprecedented level of microglial depletion and establish a model system that achieves an empty microglial niche in the adult brain. We identify a myeloid cell that migrates from the subventricular zone and associated white matter areas. Following CSF1Ri, these amoeboid cells migrate radially and tangentially in a dynamic wave filling the brain in a distinct pattern, to replace the microglial-depleted brain. These repopulating cells are enriched in disease-associated microglia genes and exhibit similar phenotypic and transcriptional profiles to white-matter-associated microglia. Our findings shed light on the overlapping and distinct functional complexity and diversity of myeloid cells of the CNS and provide new insight into repopulating microglia function and dynamics in the mouse brain.

Published

2021

4. Single-cell analysis of the ventricular-subventricular zone reveals signatures of dorsal and ventral adult neurogenesis.

Author

Cebrian-Silla, Arantxa, Cebrian-Silla, Arantxa, Nascimento, Marcos Assis, Redmond, Stephanie A, Mansky, Benjamin, Wu, David, Obernier, Kirsten, Romero Rodriguez, Ricardo, Gonzalez-Granero, Susana, García-Verdugo, Jose Manuel, Lim, Daniel A, Álvarez-Buylla, Arturo, Cebrian-Silla, Arantxa, Cebrian-Silla, Arantxa, Nascimento, Marcos Assis, Redmond, Stephanie A, Mansky, Benjamin, Wu, David, Obernier, Kirsten, Romero Rodriguez, Ricardo, Gonzalez-Granero, Susana, García-Verdugo, Jose Manuel, Lim, Daniel A, and Álvarez-Buylla, Arturo

Abstract

The ventricular-subventricular zone (V-SVZ), on the walls of the lateral ventricles, harbors the largest neurogenic niche in the adult mouse brain. Previous work has shown that neural stem/progenitor cells (NSPCs) in different locations within the V-SVZ produce different subtypes of new neurons for the olfactory bulb. The molecular signatures that underlie this regional heterogeneity remain largely unknown. Here, we present a single-cell RNA-sequencing dataset of the adult mouse V-SVZ revealing two populations of NSPCs that reside in largely non-overlapping domains in either the dorsal or ventral V-SVZ. These regional differences in gene expression were further validated using a single-nucleus RNA-sequencing reference dataset of regionally microdissected domains of the V-SVZ and by immunocytochemistry and RNAscope localization. We also identify two subpopulations of young neurons that have gene expression profiles consistent with a dorsal or ventral origin. Interestingly, a subset of genes are dynamically expressed, but maintained, in the ventral or dorsal lineages. The study provides novel markers and territories to understand the region-specific regulation of adult neurogenesis.

Published

2021

5. Subventricular zone/white matter microglia reconstitute the empty adult microglial niche in a dynamic wave.

Author

Hohsfield, Lindsay A, Hohsfield, Lindsay A, Najafi, Allison R, Ghorbanian, Yasamine, Soni, Neelakshi, Crapser, Joshua, Figueroa Velez, Dario X, Jiang, Shan, Royer, Sarah E, Kim, Sung Jin, Henningfield, Caden M, Anderson, Aileen, Gandhi, Sunil P, Mortazavi, Ali, Inlay, Matthew A, Green, Kim N, Hohsfield, Lindsay A, Hohsfield, Lindsay A, Najafi, Allison R, Ghorbanian, Yasamine, Soni, Neelakshi, Crapser, Joshua, Figueroa Velez, Dario X, Jiang, Shan, Royer, Sarah E, Kim, Sung Jin, Henningfield, Caden M, Anderson, Aileen, Gandhi, Sunil P, Mortazavi, Ali, Inlay, Matthew A, and Green, Kim N

Abstract

Microglia, the brain's resident myeloid cells, play central roles in brain defense, homeostasis, and disease. Using a prolonged colony-stimulating factor 1 receptor inhibitor (CSF1Ri) approach, we report an unprecedented level of microglial depletion and establish a model system that achieves an empty microglial niche in the adult brain. We identify a myeloid cell that migrates from the subventricular zone and associated white matter areas. Following CSF1Ri, these amoeboid cells migrate radially and tangentially in a dynamic wave filling the brain in a distinct pattern, to replace the microglial-depleted brain. These repopulating cells are enriched in disease-associated microglia genes and exhibit similar phenotypic and transcriptional profiles to white-matter-associated microglia. Our findings shed light on the overlapping and distinct functional complexity and diversity of myeloid cells of the CNS and provide new insight into repopulating microglia function and dynamics in the mouse brain.

Published

2021

6. Estimation of the time of death by measuring the variation of lateral cerebral ventricle volume and cerebrospinal fluid radiodensity using postmortem computed tomography

Author

De-Giorgio, F., Ciasca, Gabriele, Fecondo, Gennaro, Mazzini, A., De Spirito, Marco, Pascali, Vincenzo Lorenzo, Ciasca G. (ORCID:0000-0002-3694-8229), Fecondo G., De Spirito M. (ORCID:0000-0003-4260-5107), Pascali V. L. (ORCID:0000-0001-6520-5224), De-Giorgio, F., Ciasca, Gabriele, Fecondo, Gennaro, Mazzini, A., De Spirito, Marco, Pascali, Vincenzo Lorenzo, Ciasca G. (ORCID:0000-0002-3694-8229), Fecondo G., De Spirito M. (ORCID:0000-0003-4260-5107), and Pascali V. L. (ORCID:0000-0001-6520-5224)

Abstract

Using postmortem CT (PMCT), changes in the volume of the lateral cerebral ventricles (LCVs) and modifications of the radiodensity of cerebrospinal fluid (CSF) have been examined to identify a possible relationship between these changes and the time of death. Subsequent periodical CT scans termed “sequential scans” for ten corpses at known time of death were obtained, and a 3D segmentation of the entire LCV was carried out to measure its volume and radiodensity over time from ~ 5.5- h up to 273-h postmortem. A linear decrease of the LCV volume for all the cases was observed in the investigated time range, together with an overall logarithmic increase of radiodensity. Although a larger sampling should be performed to improve the result reliability, our finding suggests that the postmortem variation of CSF radiodensity can be a potentially useful tool in determining postmortem interval, a finding that is worthy of further investigation.

Published

2021

7. Single-cell RNA-seq analysis revealed long-lasting adverse effects of tamoxifen on neurogenesis in prenatal and adult brains.

Author

Lee, Chia-Ming, Lee, Chia-Ming, Zhou, Liqiang, Liu, Jiping, Shi, Jiayu, Geng, Yanan, Liu, Min, Wang, Jiaruo, Su, Xinjie, Barad, Nicholas, Wang, Junbang, Sun, Yi Eve, Lin, Quan, Lee, Chia-Ming, Lee, Chia-Ming, Zhou, Liqiang, Liu, Jiping, Shi, Jiayu, Geng, Yanan, Liu, Min, Wang, Jiaruo, Su, Xinjie, Barad, Nicholas, Wang, Junbang, Sun, Yi Eve, and Lin, Quan

Abstract

The CreER/LoxP system is widely accepted to track neural lineages and study gene functions upon tamoxifen (TAM) administration. We have observed that prenatal TAM treatment caused high rates of delayed delivery and fetal mortality. This substance could produce undesired results, leading to data misinterpretation. Here, we report that administration of TAM during early stages of cortical neurogenesis promoted precocious neural differentiation, while it inhibited neural progenitor cell (NPC) proliferation. The TAM-induced inhibition of NPC proliferation led to deficits in cortical neurogenesis, dendritic morphogenesis, synaptic formation, and cortical patterning in neonatal and postnatal offspring. Mechanistically, by employing single-cell RNA-sequencing (scRNA-seq) analysis combined with in vivo and in vitro assays, we show TAM could exert these drastic effects mainly through dysregulating the Wnt-Dmrta2 signaling pathway. In adult mice, administration of TAM significantly attenuated NPC proliferation in both the subventricular zone and the dentate gyrus. This study revealed the cellular and molecular mechanisms for the adverse effects of TAM on corticogenesis, suggesting that care must be taken when using the TAM-induced CreER/LoxP system for neural lineage tracing and genetic manipulation studies in both embryonic and adult brains.

Published

2020

8. Myxoid glioneuronal tumor, PDGFRA p.K385-mutant: clinical, radiologic, and histopathologic features.

Author

Lucas, Calixto-Hope G, Lucas, Calixto-Hope G, Villanueva-Meyer, Javier E, Whipple, Nicholas, Oberheim Bush, Nancy Ann, Cooney, Tabitha, Chang, Susan, McDermott, Michael, Berger, Mitchel, Cham, Elaine, Sun, Peter P, Putnam, Angelica, Zhou, Hong, Bollo, Robert, Cheshier, Samuel, Poppe, Matthew M, Fung, Kar-Ming, Sung, Sarah, Glenn, Chad, Fan, Xuemo, Bannykh, Serguei, Hu, Jethro, Danielpour, Moise, Li, Rong, Alva, Elizabeth, Johnston, James, Van Ziffle, Jessica, Onodera, Courtney, Devine, Patrick, Grenert, James P, Lee, Julieann C, Pekmezci, Melike, Tihan, Tarik, Bollen, Andrew W, Perry, Arie, Solomon, David A, Lucas, Calixto-Hope G, Lucas, Calixto-Hope G, Villanueva-Meyer, Javier E, Whipple, Nicholas, Oberheim Bush, Nancy Ann, Cooney, Tabitha, Chang, Susan, McDermott, Michael, Berger, Mitchel, Cham, Elaine, Sun, Peter P, Putnam, Angelica, Zhou, Hong, Bollo, Robert, Cheshier, Samuel, Poppe, Matthew M, Fung, Kar-Ming, Sung, Sarah, Glenn, Chad, Fan, Xuemo, Bannykh, Serguei, Hu, Jethro, Danielpour, Moise, Li, Rong, Alva, Elizabeth, Johnston, James, Van Ziffle, Jessica, Onodera, Courtney, Devine, Patrick, Grenert, James P, Lee, Julieann C, Pekmezci, Melike, Tihan, Tarik, Bollen, Andrew W, Perry, Arie, and Solomon, David A

Abstract

"Myxoid glioneuronal tumor, PDGFRA p.K385-mutant" is a recently described tumor entity of the central nervous system with a predilection for origin in the septum pellucidum and a defining dinucleotide mutation at codon 385 of the PDGFRA oncogene replacing lysine with either leucine or isoleucine (p.K385L/I). Clinical outcomes and optimal treatment for this new tumor entity have yet to be defined. Here, we report a comprehensive clinical, radiologic, and histopathologic assessment of eight cases. In addition to its stereotypic location in the septum pellucidum, we identify that this tumor can also occur in the corpus callosum and periventricular white matter of the lateral ventricle. Tumors centered in the septum pellucidum uniformly were associated with obstructive hydrocephalus, whereas tumors centered in the corpus callosum and periventricular white matter did not demonstrate hydrocephalus. While multiple patients were found to have ventricular dissemination or local recurrence/progression, all patients in this series remain alive at last clinical follow-up despite only biopsy or subtotal resection without adjuvant therapy in most cases. Our study further supports "myxoid glioneuronal tumor, PDGFRA p.K385-mutant" as a distinct CNS tumor entity and expands the spectrum of clinicopathologic and radiologic features of this neoplasm.

Published

2020

9. Region-specific and activity-dependent regulation of SVZ neurogenesis and recovery after stroke.

Author

Liang, Huixuan, Liang, Huixuan, Zhao, Handi, Gleichman, Amy, Machnicki, Michal, Telang, Sagar, Tang, Sydney, Rshtouni, Mary, Ruddell, Jack, Carmichael, S Thomas, Liang, Huixuan, Liang, Huixuan, Zhao, Handi, Gleichman, Amy, Machnicki, Michal, Telang, Sagar, Tang, Sydney, Rshtouni, Mary, Ruddell, Jack, and Carmichael, S Thomas

Abstract

Stroke is the leading cause of adult disability. Neurogenesis after stroke is associated with repair; however, the mechanisms regulating poststroke neurogenesis and its functional effect remain unclear. Here, we investigate multiple mechanistic routes of induced neurogenesis in the poststroke brain, using both a forelimb overuse manipulation that models a clinical neurorehabilitation paradigm, as well as local manipulation of cellular activity in the peri-infarct cortex. Increased activity in the forelimb peri-infarct cortex via either modulation drives increased subventricular zone (SVZ) progenitor proliferation, migration, and neuronal maturation in peri-infarct cortex. This effect is sensitive to competition from neighboring brain regions. By using orthogonal tract tracing and rabies virus approaches in transgenic SVZ-lineage-tracing mice, SVZ-derived neurons synaptically integrate into the peri-infarct cortex; these effects are enhanced with forelimb overuse. Synaptic transmission from these newborn SVZ-derived neurons is critical for spontaneous recovery after stroke, as tetanus neurotoxin silencing specifically of the SVZ-derived neurons disrupts the formation of these synaptic connections and hinders functional recovery after stroke. SVZ-derived neurogenesis after stroke is activity-dependent, region-specific, and sensitive to modulation, and the synaptic connections formed by these newborn cells are functionally critical for poststroke recovery.

Published

2019

10. Region-specific and activity-dependent regulation of SVZ neurogenesis and recovery after stroke.

Author

Liang, Huixuan, Liang, Huixuan, Zhao, Handi, Gleichman, Amy, Machnicki, Michal, Telang, Sagar, Tang, Sydney, Rshtouni, Mary, Ruddell, Jack, Carmichael, S Thomas, Liang, Huixuan, Liang, Huixuan, Zhao, Handi, Gleichman, Amy, Machnicki, Michal, Telang, Sagar, Tang, Sydney, Rshtouni, Mary, Ruddell, Jack, and Carmichael, S Thomas

Abstract

Stroke is the leading cause of adult disability. Neurogenesis after stroke is associated with repair; however, the mechanisms regulating poststroke neurogenesis and its functional effect remain unclear. Here, we investigate multiple mechanistic routes of induced neurogenesis in the poststroke brain, using both a forelimb overuse manipulation that models a clinical neurorehabilitation paradigm, as well as local manipulation of cellular activity in the peri-infarct cortex. Increased activity in the forelimb peri-infarct cortex via either modulation drives increased subventricular zone (SVZ) progenitor proliferation, migration, and neuronal maturation in peri-infarct cortex. This effect is sensitive to competition from neighboring brain regions. By using orthogonal tract tracing and rabies virus approaches in transgenic SVZ-lineage-tracing mice, SVZ-derived neurons synaptically integrate into the peri-infarct cortex; these effects are enhanced with forelimb overuse. Synaptic transmission from these newborn SVZ-derived neurons is critical for spontaneous recovery after stroke, as tetanus neurotoxin silencing specifically of the SVZ-derived neurons disrupts the formation of these synaptic connections and hinders functional recovery after stroke. SVZ-derived neurogenesis after stroke is activity-dependent, region-specific, and sensitive to modulation, and the synaptic connections formed by these newborn cells are functionally critical for poststroke recovery.

Published

2019

11. Quantification of glioblastoma mass effect by lateral ventricle displacement.

Author

Steed, Tyler C, Steed, Tyler C, Treiber, Jeffrey M, Brandel, Michael G, Patel, Kunal S, Dale, Anders M, Carter, Bob S, Chen, Clark C, Steed, Tyler C, Steed, Tyler C, Treiber, Jeffrey M, Brandel, Michael G, Patel, Kunal S, Dale, Anders M, Carter, Bob S, and Chen, Clark C

Abstract

Mass effect has demonstrated prognostic significance for glioblastoma, but is poorly quantified. Here we define and characterize a novel neuroimaging parameter, lateral ventricle displacement (LVd), which quantifies mass effect in glioblastoma patients. LVd is defined as the magnitude of displacement from the center of mass of the lateral ventricle volume in glioblastoma patients relative to that a normal reference brain. Pre-operative MR images from 214 glioblastoma patients from The Cancer Imaging Archive (TCIA) were segmented using iterative probabilistic voxel labeling (IPVL). LVd, contrast enhancing volumes (CEV) and FLAIR hyper-intensity volumes (FHV) were determined. Associations with patient survival and tumor genomics were investigated using data from The Cancer Genome Atlas (TCGA). Glioblastoma patients had significantly higher LVd relative to patients without brain tumors. The variance of LVd was not explained by tumor volume, as defined by CEV or FLAIR. LVd was robustly associated with glioblastoma survival in Cox models which accounted for both age and Karnofsky's Performance Scale (KPS) (p = 0.006). Glioblastomas with higher LVd demonstrated increased expression of genes associated with tumor proliferation and decreased expression of genes associated with tumor invasion. Our results suggest LVd is a quantitative measure of glioblastoma mass effect and a prognostic imaging biomarker.

Published

2018

12. The systemic environment: at the interface of aging and adult neurogenesis.

Author

Smith, Lucas K, Smith, Lucas K, White, Charles W, Villeda, Saul A, Smith, Lucas K, Smith, Lucas K, White, Charles W, and Villeda, Saul A

Abstract

Aging results in impaired neurogenesis in the two neurogenic niches of the adult mammalian brain, the dentate gyrus of the hippocampus and the subventricular zone of the lateral ventricle. While significant work has characterized intrinsic cellular changes that contribute to this decline, it is increasingly apparent that the systemic environment also represents a critical driver of brain aging. Indeed, emerging studies utilizing the model of heterochronic parabiosis have revealed that immune-related molecular and cellular changes in the aging systemic environment negatively regulate adult neurogenesis. Interestingly, these studies have also demonstrated that age-related decline in neurogenesis can be ameliorated by exposure to the young systemic environment. While this burgeoning field of research is increasingly garnering interest, as yet, the precise mechanisms driving either the pro-aging effects of aged blood or the rejuvenating effects of young blood remain to be thoroughly defined. Here, we review how age-related changes in blood, blood-borne factors, and peripheral immune cells contribute to the age-related decline in adult neurogenesis in the mammalian brain, and posit both direct neural stem cell and indirect neurogenic niche-mediated mechanisms.

Published

2018

13. The systemic environment: at the interface of aging and adult neurogenesis.

Author

Smith, Lucas K, Smith, Lucas K, White, Charles W, Villeda, Saul A, Smith, Lucas K, Smith, Lucas K, White, Charles W, and Villeda, Saul A

Abstract

Aging results in impaired neurogenesis in the two neurogenic niches of the adult mammalian brain, the dentate gyrus of the hippocampus and the subventricular zone of the lateral ventricle. While significant work has characterized intrinsic cellular changes that contribute to this decline, it is increasingly apparent that the systemic environment also represents a critical driver of brain aging. Indeed, emerging studies utilizing the model of heterochronic parabiosis have revealed that immune-related molecular and cellular changes in the aging systemic environment negatively regulate adult neurogenesis. Interestingly, these studies have also demonstrated that age-related decline in neurogenesis can be ameliorated by exposure to the young systemic environment. While this burgeoning field of research is increasingly garnering interest, as yet, the precise mechanisms driving either the pro-aging effects of aged blood or the rejuvenating effects of young blood remain to be thoroughly defined. Here, we review how age-related changes in blood, blood-borne factors, and peripheral immune cells contribute to the age-related decline in adult neurogenesis in the mammalian brain, and posit both direct neural stem cell and indirect neurogenic niche-mediated mechanisms.

Published

2018

14. Quantification of glioblastoma mass effect by lateral ventricle displacement.

Author

Steed, Tyler C, Steed, Tyler C, Treiber, Jeffrey M, Brandel, Michael G, Patel, Kunal S, Dale, Anders M, Carter, Bob S, Chen, Clark C, Steed, Tyler C, Steed, Tyler C, Treiber, Jeffrey M, Brandel, Michael G, Patel, Kunal S, Dale, Anders M, Carter, Bob S, and Chen, Clark C

Abstract

Mass effect has demonstrated prognostic significance for glioblastoma, but is poorly quantified. Here we define and characterize a novel neuroimaging parameter, lateral ventricle displacement (LVd), which quantifies mass effect in glioblastoma patients. LVd is defined as the magnitude of displacement from the center of mass of the lateral ventricle volume in glioblastoma patients relative to that a normal reference brain. Pre-operative MR images from 214 glioblastoma patients from The Cancer Imaging Archive (TCIA) were segmented using iterative probabilistic voxel labeling (IPVL). LVd, contrast enhancing volumes (CEV) and FLAIR hyper-intensity volumes (FHV) were determined. Associations with patient survival and tumor genomics were investigated using data from The Cancer Genome Atlas (TCGA). Glioblastoma patients had significantly higher LVd relative to patients without brain tumors. The variance of LVd was not explained by tumor volume, as defined by CEV or FLAIR. LVd was robustly associated with glioblastoma survival in Cox models which accounted for both age and Karnofsky's Performance Scale (KPS) (p = 0.006). Glioblastomas with higher LVd demonstrated increased expression of genes associated with tumor proliferation and decreased expression of genes associated with tumor invasion. Our results suggest LVd is a quantitative measure of glioblastoma mass effect and a prognostic imaging biomarker.

Published

2018

15. In Vivo Selection of a Computationally Designed SCHEMA AAV Library Yields a Novel Variant for Infection of Adult Neural Stem Cells in the SVZ.

Author

Ojala, David S, Ojala, David S, Sun, Sabrina, Santiago-Ortiz, Jorge L, Shapiro, Mikhail G, Romero, Philip A, Schaffer, David V, Ojala, David S, Ojala, David S, Sun, Sabrina, Santiago-Ortiz, Jorge L, Shapiro, Mikhail G, Romero, Philip A, and Schaffer, David V

Abstract

Directed evolution continues to expand the capabilities of complex biomolecules for a range of applications, such as adeno-associated virus vectors for gene therapy; however, advances in library design and selection strategies are key to develop variants that overcome barriers to clinical translation. To address this need, we applied structure-guided SCHEMA recombination of the multimeric adeno-associated virus (AAV) capsid to generate a highly diversified chimeric library with minimal structural disruption. A stringent in vivo Cre-dependent selection strategy was implemented to identify variants that transduce adult neural stem cells (NSCs) in the subventricular zone. A novel variant, SCH9, infected 60% of NSCs and mediated 24-fold higher GFP expression and a 12-fold greater transduction volume than AAV9. SCH9 utilizes both galactose and heparan sulfate as cell surface receptors and exhibits increased resistance to neutralizing antibodies. These results establish the SCHEMA library as a valuable tool for directed evolution and SCH9 as an effective gene delivery vector to investigate subventricular NSCs.

Published

2018

16. Improved Cerebrospinal Fluid-Based Discrimination between Alzheimer's Disease Patients and Controls after Correction for Ventricular Volumes

Author

van Waalwijk van Doorn, Linda J. C., Freund-Levi, Yvonne, Verbeek, Marcel M., van Waalwijk van Doorn, Linda J. C., Freund-Levi, Yvonne, and Verbeek, Marcel M.

Abstract

Cerebrospinal fluid (CSF) biomarkers may support the diagnosis of Alzheimer's disease (AD). We studied if the diagnostic power of AD CSF biomarker concentrations, i.e., Aβ42, total tau (t-tau), and phosphorylated tau (p-tau), is affected by differences in lateral ventricular volume (VV), using CSF biomarker data and magnetic resonance imaging (MRI) scans of 730 subjects, from 13 European Memory Clinics. We developed a Matlab-algorithm for standardized automated segmentation analysis of T1 weighted MRI scans in SPM8 for determining VV, and computed its ratio with total intracranial volume (TIV) as proxy for total CSF volume. The diagnostic power of CSF biomarkers (and their combination), either corrected for VV/TIV ratio or not, was determined by ROC analysis. CSF Aβ42 levels inversely correlated to VV/TIV in the whole study population (Aβ42: r = -0.28; p < 0.0001). For CSF t-tau and p-tau, this association only reached statistical significance in the combined MCI and AD group (t-tau: r = -0.15; p-tau: r = -0.13; both p < 0.01). Correction for differences in VV/TIV improved the differentiation of AD versus controls based on CSF Aβ42 alone (AUC: 0.75 versus 0.81) or in combination with t-tau (AUC: 0.81 versus 0.91). In conclusion, differences in VV may be an important confounder in interpreting CSF Aβ42 levels., Funding Agencies:Aegis of JPND Netherlands Organisation for Health Research and Development (ZonMw), the Netherlands Instituto de Salud Carlos III (ISCIII), Spain PI11/3035 PI11/02425 PI14/01126 Italian Ministry of Health, Italy IG-2014-2354450 Health Research Council of the Academy of Finland, Finland 263193 TUBITAK, Turkey 112S360 Fundacaopara a Ciencia e a Tecnologia (FCT), Portugal PIC/IC/83206/2007 JPND/0005/2011 ZonMW CAVIA project to Verbeek 733050202 Alzheimer Nederland Alzheimer's drug discovery foundation ISAO CIBERNED program (Program 1, Alzheimer Disease) FondoEuropeo de Desarrollo Regional (FEDER) Union Europea Marato TV3 201412.10 Alzheimer's Association IMI Project "PharmaCog", FP7 AXA Research Fund Fondation Universite Pierre et Marie Curie Fondation pour la Recherche sur Alzheimer, Paris, France Ce travail a beneficie d'une aide de l'Etat, program "Investissements d'avenir" ANR-10-IAIHU-06 Swiss National Science Foundation Dutch national 'Deltaplan for Dementia' Una manera de hacer Europa

Published

2017

17. Unique Organization of the Nuclear Envelope in the Post-natal Quiescent Neural Stem Cells.

Author

Cebrián-Silla, Arantxa, Cebrián-Silla, Arantxa, Alfaro-Cervelló, Clara, Herranz-Pérez, Vicente, Kaneko, Naoko, Park, Dae, Sawamoto, Kazunobu, Alvarez-Buylla, Arturo, Lim, Daniel, García-Verdugo, José, Cebrián-Silla, Arantxa, Cebrián-Silla, Arantxa, Alfaro-Cervelló, Clara, Herranz-Pérez, Vicente, Kaneko, Naoko, Park, Dae, Sawamoto, Kazunobu, Alvarez-Buylla, Arturo, Lim, Daniel, and García-Verdugo, José

Abstract

Neural stem cells (B1 astrocytes; NSCs) in the adult ventricular-subventricular-zone (V-SVZ) originate in the embryo. Surprisingly, recent work has shown that B1 cells remain largely quiescent. They are reactivated postnatally to function as primary progenitors for neurons destined for the olfactory bulb and some corpus callosum oligodendrocytes. The cellular and molecular properties of quiescent B1 cells remain unknown. Here we found that a subpopulation of B1 cells has a unique nuclear envelope invagination specialization similar to envelope-limited chromatin sheets (ELCS), reported in certain lymphocytes and some cancer cells. Using molecular markers, [3H]thymidine birth-dating, and Ara-C, we found that B1 cells with ELCS correspond to quiescent NSCs. ELCS begin forming in embryonic radial glia cells and represent a specific nuclear compartment containing particular epigenetic modifications and telomeres. These results reveal a unique nuclear compartment in quiescent NSCs, which is useful for identifying these primary progenitors and study their gene regulation.

Published

2017

18. Comparative analyses identify molecular signature of MRI-classified SVZ-associated glioblastoma.

Author

Lin, Chin-Hsing Annie, Lin, Chin-Hsing Annie, Rhodes, Christopher T, Lin, ChenWei, Phillips, Joanna J, Berger, Mitchel S, Lin, Chin-Hsing Annie, Lin, Chin-Hsing Annie, Rhodes, Christopher T, Lin, ChenWei, Phillips, Joanna J, and Berger, Mitchel S

Abstract

Glioblastoma (GBM) is a highly aggressive brain cancer with limited therapeutic options. While efforts to identify genes responsible for GBM have revealed mutations and aberrant gene expression associated with distinct types of GBM, patients with GBM are often diagnosed and classified based on MRI features. Therefore, we seek to identify molecular representatives in parallel with MRI classification for group I and group II primary GBM associated with the subventricular zone (SVZ). As group I and II GBM contain stem-like signature, we compared gene expression profiles between these 2 groups of primary GBM and endogenous neural stem progenitor cells to reveal dysregulation of cell cycle, chromatin status, cellular morphogenesis, and signaling pathways in these 2 types of MRI-classified GBM. In the absence of IDH mutation, several genes associated with metabolism are differentially expressed in these subtypes of primary GBM, implicating metabolic reprogramming occurs in tumor microenvironment. Furthermore, histone lysine methyltransferase EZH2 was upregulated while histone lysine demethylases KDM2 and KDM4 were downregulated in both group I and II primary GBM. Lastly, we identified 9 common genes across large data sets of gene expression profiles among MRI-classified group I/II GBM, a large cohort of GBM subtypes from TCGA, and glioma stem cells by unsupervised clustering comparison. These commonly upregulated genes have known functions in cell cycle, centromere assembly, chromosome segregation, and mitotic progression. Our findings highlight altered expression of genes important in chromosome integrity across all GBM, suggesting a common mechanism of disrupted fidelity of chromosome structure in GBM.

Published

2017

19. Effect of skull type on the relative size of cerebral cortex and lateral ventricles in dogs

Author

Pilegaard, Anders M., Berendt, Mette, Holst, Pernille, Møller, Arne, McEvoy, Fintan J., Pilegaard, Anders M., Berendt, Mette, Holst, Pernille, Møller, Arne, and McEvoy, Fintan J.

Abstract

Volume measurements of the brain are of interest in the diagnosis of brain pathology. This is particularly so in the investigation hydrocephalus and canine cognitive dysfunction (CCD), both of which result in thinning of the cerebral cortex and enlarged ventricles. Volume assessment can be made using computed tomography or more usually magnetic resonance imaging (MRI). There is, however, some uncertainty in the interpretation of such volume data due to the great variation in skull size and shape seen in dog. In this retrospective study, we examined normal MRI images from 63 dogs < 6 years of age. We used a continuous variable, the cranial index (CrI) to indicate skull shape and compared it with MRI volume measurements derived using Cavalieri's principle. We found a negative correlation between CrI and the ratio of cortical to ventricular volume. Breeds with a high CrI (large laterolateral compared to rostrocaudal cranial cavity dimension) had a smaller ratio of cortical to ventricular volume (low C:V ratio) than breeds with lower CrI skull types. It is important to consider this effect of skull shape on the relative volume estimates of the cerebral cortex and ventricles when trying to establish if pathology is present.

Published

2017

20. Effect of skull type on the relative size of cerebral cortex and lateral ventricles in dogs

Author

Pilegaard, Anders M., Berendt, Mette, Holst, Pernille, Møller, Arne, McEvoy, Fintan J., Pilegaard, Anders M., Berendt, Mette, Holst, Pernille, Møller, Arne, and McEvoy, Fintan J.

Abstract

Volume measurements of the brain are of interest in the diagnosis of brain pathology. This is particularly so in the investigation hydrocephalus and canine cognitive dysfunction (CCD), both of which result in thinning of the cerebral cortex and enlarged ventricles. Volume assessment can be made using computed tomography or more usually magnetic resonance imaging (MRI). There is, however, some uncertainty in the interpretation of such volume data due to the great variation in skull size and shape seen in dog. In this retrospective study, we examined normal MRI images from 63 dogs < 6 years of age. We used a continuous variable, the cranial index (CrI) to indicate skull shape and compared it with MRI volume measurements derived using Cavalieri's principle. We found a negative correlation between CrI and the ratio of cortical to ventricular volume. Breeds with a high CrI (large laterolateral compared to rostrocaudal cranial cavity dimension) had a smaller ratio of cortical to ventricular volume (low C:V ratio) than breeds with lower CrI skull types. It is important to consider this effect of skull shape on the relative volume estimates of the cerebral cortex and ventricles when trying to establish if pathology is present.

Published

2017

21. Pallidum and lateral ventricle volume enlargement in autism spectrum disorder.

Author

Turner, Andia H, Turner, Andia H, Greenspan, Kiefer S, van Erp, Theo GM, Turner, Andia H, Turner, Andia H, Greenspan, Kiefer S, and van Erp, Theo GM

Abstract

Studies on structural brain abnormalities in individuals with autism spectrum disorders (ASD) have been of limited size and many findings have not been replicated. In the largest ASD brain morphology study to date, we compared subcortical, total brain (TBV), and intracranial (ICV) volumes between 472 subjects with DSM-IV ASD diagnoses and 538 healthy volunteers (age range: 6-64 years), obtained from high-resolution structural brain scans provided by the Autism Brain Imaging Data Exchange (ABIDE). Compared to healthy volunteers, we found significantly larger pallidum (Cohen's d=0.15) and lateral ventricle volumes (Cohen's d=0.18) in ASD. These enlargements were independent of total brain volume and IQ, passed FDR correction for multiple comparisons, and were observed in overall, male-only, and medication-free subjects. In addition, intracranial, hippocampal, and caudate volumes were enlarged in ASD at a nominal statistical threshold of p<0.05. This study provides the first robust evidence for pallidum enlargement in ASD independent from TBV and encourages further study of the functional role of the pallidum in individuals with autism spectrum disorder.

Published

2016

22. A Primate lncRNA Mediates Notch Signaling during Neuronal Development by Sequestering miRNA.

Author

Rani, Neha, Rani, Neha, Nowakowski, Tomasz J, Zhou, Hongjun, Godshalk, Sirie E, Lisi, Véronique, Kriegstein, Arnold R, Kosik, Kenneth S, Rani, Neha, Rani, Neha, Nowakowski, Tomasz J, Zhou, Hongjun, Godshalk, Sirie E, Lisi, Véronique, Kriegstein, Arnold R, and Kosik, Kenneth S

Abstract

Long non-coding RNAs (lncRNAs) are a diverse and poorly conserved category of transcripts that have expanded greatly in primates, particularly in the brain. We identified an lncRNA, which has acquired 16 microRNA response elements for miR-143-3p in the Catarrhini branch of primates. This lncRNA, termed LncND (neurodevelopment), is expressed in neural progenitor cells and then declines in neurons. Binding and release of miR-143-3p by LncND control the expression of Notch receptors. LncND expression is enriched in radial glia cells (RGCs) in the ventricular and subventricular zones of developing human brain. Downregulation in neuroblastoma cells reduced cell proliferation and induced neuronal differentiation, an effect phenocopied by miR-143-3p overexpression. Gain of function of LncND in developing mouse cortex led to an expansion of PAX6+ RGCs. These findings support a role for LncND in miRNA-mediated regulation of Notch signaling within the neural progenitor pool in primates that may have contributed to the expansion of cerebral cortex.

Published

2016

23. Extensive migration of young neurons into the infant human frontal lobe.

Author

Paredes, Mercedes F, Paredes, Mercedes F, James, David, Gil-Perotin, Sara, Kim, Hosung, Cotter, Jennifer A, Ng, Carissa, Sandoval, Kadellyn, Rowitch, David H, Xu, Duan, McQuillen, Patrick S, Garcia-Verdugo, Jose-Manuel, Huang, Eric J, Alvarez-Buylla, Arturo, Paredes, Mercedes F, Paredes, Mercedes F, James, David, Gil-Perotin, Sara, Kim, Hosung, Cotter, Jennifer A, Ng, Carissa, Sandoval, Kadellyn, Rowitch, David H, Xu, Duan, McQuillen, Patrick S, Garcia-Verdugo, Jose-Manuel, Huang, Eric J, and Alvarez-Buylla, Arturo

Abstract

The first few months after birth, when a child begins to interact with the environment, are critical to human brain development. The human frontal lobe is important for social behavior and executive function; it has increased in size and complexity relative to other species, but the processes that have contributed to this expansion are unknown. Our studies of postmortem infant human brains revealed a collection of neurons that migrate and integrate widely into the frontal lobe during infancy. Chains of young neurons move tangentially close to the walls of the lateral ventricles and along blood vessels. These cells then individually disperse long distances to reach cortical tissue, where they differentiate and contribute to inhibitory circuits. Late-arriving interneurons could contribute to developmental plasticity, and the disruption of their postnatal migration or differentiation may underlie neurodevelopmental disorders.

Published

2016

24. Evolutionary origin of Tbr2-expressing precursor cells and the subventricular zone in the developing cortex.

Author

Martínez-Cerdeño, Verónica, Martínez-Cerdeño, Verónica, Cunningham, Christopher L, Camacho, Jasmin, Keiter, Janet A, Ariza, Jeanelle, Lovern, Matthew, Noctor, Stephen C, Martínez-Cerdeño, Verónica, Martínez-Cerdeño, Verónica, Cunningham, Christopher L, Camacho, Jasmin, Keiter, Janet A, Ariza, Jeanelle, Lovern, Matthew, and Noctor, Stephen C

Abstract

The subventricular zone (SVZ) is greatly expanded in primates with gyrencephalic cortices and is thought to be absent from vertebrates with three-layered, lissencephalic cortices, such as the turtle. Recent work in rodents has shown that Tbr2-expressing neural precursor cells in the SVZ produce excitatory neurons for each cortical layer in the neocortex. Many excitatory neurons are generated through a two-step process in which Pax6-expressing radial glial cells divide in the VZ to produce Tbr2-expressing intermediate progenitor cells, which divide in the SVZ to produce cortical neurons. We investigated the evolutionary origin of SVZ neural precursor cells in the prenatal cerebral cortex by testing for the presence and distribution of Tbr2-expressing cells in the prenatal cortex of reptilian and avian species. We found that mitotic Tbr2(+) cells are present in the prenatal cortex of lizard, turtle, chicken, and dove. Furthermore, Tbr2(+) cells are organized into a distinct SVZ in the dorsal ventricular ridge (DVR) of turtle forebrain and in the cortices of chicken and dove. Our results are consistent with the concept that Tbr2(+) neural precursor cells were present in the common ancestor of mammals and reptiles. Our data also suggest that the organizing principle guiding the assembly of Tbr2(+) cells into an anatomically distinct SVZ, both developmentally and evolutionarily, may be shared across vertebrates. Finally, our results indicate that Tbr2 expression can be used to test for the presence of a distinct SVZ and to define the boundaries of the SVZ in developing cortices.

Published

2016

25. Pbx1 is required for adult subventricular zone neurogenesis.

Author

Grebbin, Britta Moyo, Grebbin, Britta Moyo, Hau, Ann-Christin, Groß, Anja, Anders-Maurer, Marie, Schramm, Jasmine, Koss, Matthew, Wille, Christoph, Mittelbronn, Michel, Selleri, Licia, Schulte, Dorothea, Grebbin, Britta Moyo, Grebbin, Britta Moyo, Hau, Ann-Christin, Groß, Anja, Anders-Maurer, Marie, Schramm, Jasmine, Koss, Matthew, Wille, Christoph, Mittelbronn, Michel, Selleri, Licia, and Schulte, Dorothea

Abstract

TALE-homeodomain proteins function as components of heteromeric complexes that contain one member each of the PBC and MEIS/PREP subclasses. We recently showed that MEIS2 cooperates with the neurogenic transcription factor PAX6 in the control of adult subventricular zone (SVZ) neurogenesis in rodents. Expression of the PBC protein PBX1 in the SVZ has been reported, but its functional role(s) has not been investigated. Using a genetic loss-of-function mouse model, we now show that Pbx1 is an early regulator of SVZ neurogenesis. Targeted deletion of Pbx1 by retroviral transduction of Cre recombinase into Pbx2-deficient SVZ stem and progenitor cells carrying floxed alleles of Pbx1 significantly reduced the production of neurons and increased the generation of oligodendrocytes. Loss of Pbx1 expression in neuronally committed neuroblasts in the rostral migratory stream in a Pbx2 null background, by contrast, severely compromised cell survival. By chromatin immunoprecipitation from endogenous tissues or isolated cells, we further detected PBX1 binding to known regulatory regions of the neuron-specific genes Dcx and Th days or even weeks before the respective genes are expressed during the normal program of SVZ neurogenesis, suggesting that PBX1 might act as a priming factor to mark these genes for subsequent activation. Collectively, our results establish that PBX1 regulates adult neural cell fate determination in a manner beyond that of its heterodimerization partner MEIS2.

Published

2016

26. Differential localization of glioblastoma subtype: implications on glioblastoma pathogenesis.

Author

Steed, Tyler C, Steed, Tyler C, Treiber, Jeffrey M, Patel, Kunal, Ramakrishnan, Valya, Merk, Alexander, Smith, Amanda R, Carter, Bob S, Dale, Anders M, Chow, Lionel ML, Chen, Clark C, Steed, Tyler C, Steed, Tyler C, Treiber, Jeffrey M, Patel, Kunal, Ramakrishnan, Valya, Merk, Alexander, Smith, Amanda R, Carter, Bob S, Dale, Anders M, Chow, Lionel ML, and Chen, Clark C

Abstract

IntroductionThe subventricular zone (SVZ) has been implicated in the pathogenesis of glioblastoma. Whether molecular subtypes of glioblastoma arise from unique niches of the brain relative to the SVZ remains largely unknown. Here, we tested whether these subtypes of glioblastoma occupy distinct regions of the cerebrum and examined glioblastoma localization in relation to the SVZ.MethodsPre-operative MR images from 217 glioblastoma patients from The Cancer Imaging Archive were segmented automatically into contrast enhancing (CE) tumor volumes using Iterative Probabilistic Voxel Labeling (IPVL). Probabilistic maps of tumor location were generated for each subtype and distances were calculated from the centroid of CE tumor volumes to the SVZ. Glioblastomas that arose in a Genetically Modified Murine Model (GEMM) model were also analyzed with regard to SVZ distance and molecular subtype.ResultsClassical and mesenchymal glioblastomas were more diffusely distributed and located farther from the SVZ. In contrast, proneural and neural glioblastomas were more likely to be located in closer proximity to the SVZ. Moreover, in a GFAP-CreER; PtenloxP/loxP; Trp53loxP/loxP; Rb1loxP/loxP; Rbl1-/- GEMM model of glioblastoma where tumor can spontaneously arise in different regions of the cerebrum, tumors that arose near the SVZ were more likely to be of proneural subtype (p < 0.0001).ConclusionsGlioblastoma subtypes occupy different regions of the brain and vary in proximity to the SVZ. These findings harbor implications pertaining to the pathogenesis of glioblastoma subtypes.

Published

2016

27. A Primate lncRNA Mediates Notch Signaling during Neuronal Development by Sequestering miRNA.

Author

Rani, Neha, Rani, Neha, Nowakowski, Tomasz J, Zhou, Hongjun, Godshalk, Sirie E, Lisi, Véronique, Kriegstein, Arnold R, Kosik, Kenneth S, Rani, Neha, Rani, Neha, Nowakowski, Tomasz J, Zhou, Hongjun, Godshalk, Sirie E, Lisi, Véronique, Kriegstein, Arnold R, and Kosik, Kenneth S

Abstract

Long non-coding RNAs (lncRNAs) are a diverse and poorly conserved category of transcripts that have expanded greatly in primates, particularly in the brain. We identified an lncRNA, which has acquired 16 microRNA response elements for miR-143-3p in the Catarrhini branch of primates. This lncRNA, termed LncND (neurodevelopment), is expressed in neural progenitor cells and then declines in neurons. Binding and release of miR-143-3p by LncND control the expression of Notch receptors. LncND expression is enriched in radial glia cells (RGCs) in the ventricular and subventricular zones of developing human brain. Downregulation in neuroblastoma cells reduced cell proliferation and induced neuronal differentiation, an effect phenocopied by miR-143-3p overexpression. Gain of function of LncND in developing mouse cortex led to an expansion of PAX6+ RGCs. These findings support a role for LncND in miRNA-mediated regulation of Notch signaling within the neural progenitor pool in primates that may have contributed to the expansion of cerebral cortex.

Published

2016

28. Pallidum and lateral ventricle volume enlargement in autism spectrum disorder.

Author

Turner, Andia H, Turner, Andia H, Greenspan, Kiefer S, van Erp, Theo GM, Turner, Andia H, Turner, Andia H, Greenspan, Kiefer S, and van Erp, Theo GM

Abstract

Studies on structural brain abnormalities in individuals with autism spectrum disorders (ASD) have been of limited size and many findings have not been replicated. In the largest ASD brain morphology study to date, we compared subcortical, total brain (TBV), and intracranial (ICV) volumes between 472 subjects with DSM-IV ASD diagnoses and 538 healthy volunteers (age range: 6-64 years), obtained from high-resolution structural brain scans provided by the Autism Brain Imaging Data Exchange (ABIDE). Compared to healthy volunteers, we found significantly larger pallidum (Cohen's d=0.15) and lateral ventricle volumes (Cohen's d=0.18) in ASD. These enlargements were independent of total brain volume and IQ, passed FDR correction for multiple comparisons, and were observed in overall, male-only, and medication-free subjects. In addition, intracranial, hippocampal, and caudate volumes were enlarged in ASD at a nominal statistical threshold of p<0.05. This study provides the first robust evidence for pallidum enlargement in ASD independent from TBV and encourages further study of the functional role of the pallidum in individuals with autism spectrum disorder.

Published

2016

29. Evolutionary origin of Tbr2-expressing precursor cells and the subventricular zone in the developing cortex.

Author

Martínez-Cerdeño, Verónica, Martínez-Cerdeño, Verónica, Cunningham, Christopher L, Camacho, Jasmin, Keiter, Janet A, Ariza, Jeanelle, Lovern, Matthew, Noctor, Stephen C, Martínez-Cerdeño, Verónica, Martínez-Cerdeño, Verónica, Cunningham, Christopher L, Camacho, Jasmin, Keiter, Janet A, Ariza, Jeanelle, Lovern, Matthew, and Noctor, Stephen C

Abstract

The subventricular zone (SVZ) is greatly expanded in primates with gyrencephalic cortices and is thought to be absent from vertebrates with three-layered, lissencephalic cortices, such as the turtle. Recent work in rodents has shown that Tbr2-expressing neural precursor cells in the SVZ produce excitatory neurons for each cortical layer in the neocortex. Many excitatory neurons are generated through a two-step process in which Pax6-expressing radial glial cells divide in the VZ to produce Tbr2-expressing intermediate progenitor cells, which divide in the SVZ to produce cortical neurons. We investigated the evolutionary origin of SVZ neural precursor cells in the prenatal cerebral cortex by testing for the presence and distribution of Tbr2-expressing cells in the prenatal cortex of reptilian and avian species. We found that mitotic Tbr2(+) cells are present in the prenatal cortex of lizard, turtle, chicken, and dove. Furthermore, Tbr2(+) cells are organized into a distinct SVZ in the dorsal ventricular ridge (DVR) of turtle forebrain and in the cortices of chicken and dove. Our results are consistent with the concept that Tbr2(+) neural precursor cells were present in the common ancestor of mammals and reptiles. Our data also suggest that the organizing principle guiding the assembly of Tbr2(+) cells into an anatomically distinct SVZ, both developmentally and evolutionarily, may be shared across vertebrates. Finally, our results indicate that Tbr2 expression can be used to test for the presence of a distinct SVZ and to define the boundaries of the SVZ in developing cortices.

Published

2016

30. Differential localization of glioblastoma subtype: implications on glioblastoma pathogenesis.

Author

Steed, Tyler C, Steed, Tyler C, Treiber, Jeffrey M, Patel, Kunal, Ramakrishnan, Valya, Merk, Alexander, Smith, Amanda R, Carter, Bob S, Dale, Anders M, Chow, Lionel ML, Chen, Clark C, Steed, Tyler C, Steed, Tyler C, Treiber, Jeffrey M, Patel, Kunal, Ramakrishnan, Valya, Merk, Alexander, Smith, Amanda R, Carter, Bob S, Dale, Anders M, Chow, Lionel ML, and Chen, Clark C

Abstract

IntroductionThe subventricular zone (SVZ) has been implicated in the pathogenesis of glioblastoma. Whether molecular subtypes of glioblastoma arise from unique niches of the brain relative to the SVZ remains largely unknown. Here, we tested whether these subtypes of glioblastoma occupy distinct regions of the cerebrum and examined glioblastoma localization in relation to the SVZ.MethodsPre-operative MR images from 217 glioblastoma patients from The Cancer Imaging Archive were segmented automatically into contrast enhancing (CE) tumor volumes using Iterative Probabilistic Voxel Labeling (IPVL). Probabilistic maps of tumor location were generated for each subtype and distances were calculated from the centroid of CE tumor volumes to the SVZ. Glioblastomas that arose in a Genetically Modified Murine Model (GEMM) model were also analyzed with regard to SVZ distance and molecular subtype.ResultsClassical and mesenchymal glioblastomas were more diffusely distributed and located farther from the SVZ. In contrast, proneural and neural glioblastomas were more likely to be located in closer proximity to the SVZ. Moreover, in a GFAP-CreER; PtenloxP/loxP; Trp53loxP/loxP; Rb1loxP/loxP; Rbl1-/- GEMM model of glioblastoma where tumor can spontaneously arise in different regions of the cerebrum, tumors that arose near the SVZ were more likely to be of proneural subtype (p < 0.0001).ConclusionsGlioblastoma subtypes occupy different regions of the brain and vary in proximity to the SVZ. These findings harbor implications pertaining to the pathogenesis of glioblastoma subtypes.

Published

2016

31. Pbx1 is required for adult subventricular zone neurogenesis.

Author

Grebbin, Britta Moyo, Grebbin, Britta Moyo, Hau, Ann-Christin, Groß, Anja, Anders-Maurer, Marie, Schramm, Jasmine, Koss, Matthew, Wille, Christoph, Mittelbronn, Michel, Selleri, Licia, Schulte, Dorothea, Grebbin, Britta Moyo, Grebbin, Britta Moyo, Hau, Ann-Christin, Groß, Anja, Anders-Maurer, Marie, Schramm, Jasmine, Koss, Matthew, Wille, Christoph, Mittelbronn, Michel, Selleri, Licia, and Schulte, Dorothea

Abstract

TALE-homeodomain proteins function as components of heteromeric complexes that contain one member each of the PBC and MEIS/PREP subclasses. We recently showed that MEIS2 cooperates with the neurogenic transcription factor PAX6 in the control of adult subventricular zone (SVZ) neurogenesis in rodents. Expression of the PBC protein PBX1 in the SVZ has been reported, but its functional role(s) has not been investigated. Using a genetic loss-of-function mouse model, we now show that Pbx1 is an early regulator of SVZ neurogenesis. Targeted deletion of Pbx1 by retroviral transduction of Cre recombinase into Pbx2-deficient SVZ stem and progenitor cells carrying floxed alleles of Pbx1 significantly reduced the production of neurons and increased the generation of oligodendrocytes. Loss of Pbx1 expression in neuronally committed neuroblasts in the rostral migratory stream in a Pbx2 null background, by contrast, severely compromised cell survival. By chromatin immunoprecipitation from endogenous tissues or isolated cells, we further detected PBX1 binding to known regulatory regions of the neuron-specific genes Dcx and Th days or even weeks before the respective genes are expressed during the normal program of SVZ neurogenesis, suggesting that PBX1 might act as a priming factor to mark these genes for subsequent activation. Collectively, our results establish that PBX1 regulates adult neural cell fate determination in a manner beyond that of its heterodimerization partner MEIS2.

Published

2016

32. Extensive migration of young neurons into the infant human frontal lobe.

Author

Paredes, Mercedes F, Paredes, Mercedes F, James, David, Gil-Perotin, Sara, Kim, Hosung, Cotter, Jennifer A, Ng, Carissa, Sandoval, Kadellyn, Rowitch, David H, Xu, Duan, McQuillen, Patrick S, Garcia-Verdugo, Jose-Manuel, Huang, Eric J, Alvarez-Buylla, Arturo, Paredes, Mercedes F, Paredes, Mercedes F, James, David, Gil-Perotin, Sara, Kim, Hosung, Cotter, Jennifer A, Ng, Carissa, Sandoval, Kadellyn, Rowitch, David H, Xu, Duan, McQuillen, Patrick S, Garcia-Verdugo, Jose-Manuel, Huang, Eric J, and Alvarez-Buylla, Arturo

Abstract

The first few months after birth, when a child begins to interact with the environment, are critical to human brain development. The human frontal lobe is important for social behavior and executive function; it has increased in size and complexity relative to other species, but the processes that have contributed to this expansion are unknown. Our studies of postmortem infant human brains revealed a collection of neurons that migrate and integrate widely into the frontal lobe during infancy. Chains of young neurons move tangentially close to the walls of the lateral ventricles and along blood vessels. These cells then individually disperse long distances to reach cortical tissue, where they differentiate and contribute to inhibitory circuits. Late-arriving interneurons could contribute to developmental plasticity, and the disruption of their postnatal migration or differentiation may underlie neurodevelopmental disorders.

Published

2016

33. Uncovering the roles of long noncoding RNAs in neural development and glioma progression.

Author

Ramos, Alexander D, Ramos, Alexander D, Attenello, Frank J, Lim, Daniel A, Ramos, Alexander D, Ramos, Alexander D, Attenello, Frank J, and Lim, Daniel A

Abstract

In the past decade, thousands of long noncoding RNAs (lncRNAs) have been identified, and emerging data indicate that lncRNAs can have important biological functions and roles in human diseases including cancer. Many lncRNAs appear to be expressed specifically in the brain, and the roles of lncRNAs in neural stem cells (NSCs) and brain development are now beginning to be discovered. Here we review recent advances in understanding the diversity of lncRNA structure and functions in NSCs and brain development. NSCs in the adult mouse ventricular-subventricular zone (V-SVZ) generate new neurons throughout life, and we discuss how key elements of this adult neurogenic system have facilitated the discovery and functional characterization of known and novel lncRNAs. A review of lncRNAs described in other NSC systems reveals a variety of molecular mechanisms, including binding and recruitment of transcription factors, epigenetic modifiers, and RNA-splicing factors. Finally, we review emerging evidence indicating that specific lncRNAs can be key drivers of glial tumors, and discuss next steps towards an in vivo understanding of lncRNA function in development and disease.

Published

2016

34. The outer subventricular zone and primate-specific cortical complexification.

Author

Dehay, Colette, Dehay, Colette, Kennedy, Henry, Kosik, Kenneth S, Dehay, Colette, Dehay, Colette, Kennedy, Henry, and Kosik, Kenneth S

Abstract

Evolutionary expansion and complexification of the primate cerebral cortex are largely linked to the emergence of the outer subventricular zone (OSVZ), a uniquely structured germinal zone that generates the expanded primate supragranular layers. The primate OSVZ departs from rodent germinal zones in that it includes a higher diversity of precursor types, inter-related in bidirectional non-hierarchical lineages. In addition, primate-specific regulatory mechanisms are operating in primate cortical precursors via the occurrence of novel miRNAs. Here, we propose that the origin and evolutionary importance of the OSVZ is related to genetic changes in multiple regulatory loops and that cell-cycle regulation is a favored target for evolutionary adaptation of the cortex.

Published

2015

35. Baseline shape diffeomorphometry patterns of subcortical and ventricular structures in predicting conversion of mild cognitive impairment to Alzheimer's disease.

Author

Tang, Xiaoying, Tang, Xiaoying, Holland, Dominic, Dale, Anders M, Younes, Laurent, Miller, Michael I, Tang, Xiaoying, Tang, Xiaoying, Holland, Dominic, Dale, Anders M, Younes, Laurent, and Miller, Michael I

Abstract

In this paper, we propose a novel predictor for the conversion from mild cognitive impairment (MCI) to Alzheimer's disease (AD). This predictor is based on the shape diffeomorphometry patterns of subcortical and ventricular structures (left and right amygdala, hippocampus, thalamus, caudate, putamen, globus pallidus, and lateral ventricle) of 607 baseline scans from the Alzheimer's Disease Neuroimaging Initiative database, including a total of 210 healthy control subjects, 222 MCI subjects, and 175 AD subjects. The optimal predictor is obtained via a feature selection procedure applied to all of the 14 sets of shape features via linear discriminant analysis, resulting in a combination of the shape diffeomorphometry patterns of the left hippocampus, the left lateral ventricle, the right thalamus, the right caudate, and the bilateral putamen. Via 10-fold cross-validation, we substantiate our method by successfully differentiating 77.04% (104/135) of the MCI subjects who converted to AD within 36 months and 71.26% (62/87) of the non-converters. To be specific, for the MCI-converters, we are capable of correctly predicting 82.35% (14/17) of subjects converting in 6 months, 77.5% (31/40) of subjects converting in 12 months, 74.07% (20/27) of subjects converting in 18 months, 78.13% (25/32) of subjects converting in 24 months, and 73.68% (14/19) of subject converting in 36 months. Statistically significant correlation maps were observed between the shape diffeomorphometry features of each of the 14 structures, especially the bilateral amygdala, hippocampus, lateral ventricle, and two neuropsychological test scores--the Alzheimer's Disease Assessment Scale-Cognitive Behavior Section and the Mini-Mental State Examination.

Published

2015

36. The outer subventricular zone and primate-specific cortical complexification.

Author

Dehay, Colette, Dehay, Colette, Kennedy, Henry, Kosik, Kenneth S, Dehay, Colette, Dehay, Colette, Kennedy, Henry, and Kosik, Kenneth S

Abstract

Evolutionary expansion and complexification of the primate cerebral cortex are largely linked to the emergence of the outer subventricular zone (OSVZ), a uniquely structured germinal zone that generates the expanded primate supragranular layers. The primate OSVZ departs from rodent germinal zones in that it includes a higher diversity of precursor types, inter-related in bidirectional non-hierarchical lineages. In addition, primate-specific regulatory mechanisms are operating in primate cortical precursors via the occurrence of novel miRNAs. Here, we propose that the origin and evolutionary importance of the OSVZ is related to genetic changes in multiple regulatory loops and that cell-cycle regulation is a favored target for evolutionary adaptation of the cortex.

Published

2015

37. Baseline shape diffeomorphometry patterns of subcortical and ventricular structures in predicting conversion of mild cognitive impairment to Alzheimer's disease.

Author

Tang, Xiaoying, Tang, Xiaoying, Holland, Dominic, Dale, Anders M, Younes, Laurent, Miller, Michael I, Tang, Xiaoying, Tang, Xiaoying, Holland, Dominic, Dale, Anders M, Younes, Laurent, and Miller, Michael I

Abstract

In this paper, we propose a novel predictor for the conversion from mild cognitive impairment (MCI) to Alzheimer's disease (AD). This predictor is based on the shape diffeomorphometry patterns of subcortical and ventricular structures (left and right amygdala, hippocampus, thalamus, caudate, putamen, globus pallidus, and lateral ventricle) of 607 baseline scans from the Alzheimer's Disease Neuroimaging Initiative database, including a total of 210 healthy control subjects, 222 MCI subjects, and 175 AD subjects. The optimal predictor is obtained via a feature selection procedure applied to all of the 14 sets of shape features via linear discriminant analysis, resulting in a combination of the shape diffeomorphometry patterns of the left hippocampus, the left lateral ventricle, the right thalamus, the right caudate, and the bilateral putamen. Via 10-fold cross-validation, we substantiate our method by successfully differentiating 77.04% (104/135) of the MCI subjects who converted to AD within 36 months and 71.26% (62/87) of the non-converters. To be specific, for the MCI-converters, we are capable of correctly predicting 82.35% (14/17) of subjects converting in 6 months, 77.5% (31/40) of subjects converting in 12 months, 74.07% (20/27) of subjects converting in 18 months, 78.13% (25/32) of subjects converting in 24 months, and 73.68% (14/19) of subject converting in 36 months. Statistically significant correlation maps were observed between the shape diffeomorphometry features of each of the 14 structures, especially the bilateral amygdala, hippocampus, lateral ventricle, and two neuropsychological test scores--the Alzheimer's Disease Assessment Scale-Cognitive Behavior Section and the Mini-Mental State Examination.

Published

2015

38. The subventricular zone continues to generate corpus callosum and rostral migratory stream astroglia in normal adult mice.

Author

Sohn, Jiho, Sohn, Jiho, Orosco, Lori, Guo, Fuzheng, Chung, Seung-Hyuk, Bannerman, Peter, Mills Ko, Emily, Zarbalis, Kostas, Deng, Wenbin, Pleasure, David, Sohn, Jiho, Sohn, Jiho, Orosco, Lori, Guo, Fuzheng, Chung, Seung-Hyuk, Bannerman, Peter, Mills Ko, Emily, Zarbalis, Kostas, Deng, Wenbin, and Pleasure, David

Abstract

Astrocytes are the most abundant cells in the CNS, and have many essential functions, including maintenance of blood-brain barrier integrity, and CNS water, ion, and glutamate homeostasis. Mammalian astrogliogenesis has generally been considered to be completed soon after birth, and to be reactivated in later life only under pathological circumstances. Here, by using genetic fate-mapping, we demonstrate that new corpus callosum astrocytes are continuously generated from nestin(+) subventricular zone (SVZ) neural progenitor cells (NPCs) in normal adult mice. These nestin fate-mapped corpus callosum astrocytes are uniformly postmitotic, express glutamate receptors, and form aquaporin-4(+) perivascular endfeet. The entry of new astrocytes from the SVZ into the corpus callosum appears to be balanced by astroglial apoptosis, because overall numbers of corpus callosum astrocytes remain constant during normal adulthood. Nestin fate-mapped astrocytes also flow anteriorly from the SVZ in association with the rostral migratory stream, but do not penetrate into the deeper layers of the olfactory bulb. Production of new astrocytes from nestin(+) NPCs is absent in the normal adult cortex, striatum, and spinal cord. Our study is the first to demonstrate ongoing SVZ astrogliogenesis in the normal adult mammalian forebrain.

Published

2015

39. Empowering imaging biomarkers of Alzheimer's disease.

Author

Gutman, Boris A, Gutman, Boris A, Wang, Yalin, Yanovsky, Igor, Hua, Xue, Toga, Arthur W, Jack, Clifford R, Weiner, Michael W, Thompson, Paul M, Alzheimer's Disease Neuroimaging Initiative, Gutman, Boris A, Gutman, Boris A, Wang, Yalin, Yanovsky, Igor, Hua, Xue, Toga, Arthur W, Jack, Clifford R, Weiner, Michael W, Thompson, Paul M, and Alzheimer's Disease Neuroimaging Initiative

Abstract

In a previous report, we proposed a method for combining multiple markers of atrophy caused by Alzheimer's disease into a single atrophy score that is more powerful than any one feature. We applied the method to expansion rates of the lateral ventricles, achieving the most powerful ventricular atrophy measure to date. Here, we expand our method's application to tensor-based morphometry measures. We also combine the volumetric tensor-based morphometry measures with previously computed ventricular surface measures into a combined atrophy score. We show that our atrophy scores are longitudinally unbiased with the intercept bias estimated at 2 orders of magnitude below the mean atrophy of control subjects at 1 year. Both approaches yield the most powerful biomarker of atrophy not only for ventricular measures but also for all published unbiased imaging measures to date. A 2-year trial using our measures requires only 31 (22, 43) Alzheimer's disease subjects or 56 (44, 64) subjects with mild cognitive impairment to detect 25% slowing in atrophy with 80% power and 95% confidence.

Published

2015

40. A Distinct Population of Microglia Supports Adult Neurogenesis in the Subventricular Zone

Author

Ribeiro Xavier, Anna L., Kress, Benjamin T., Goldman, Steven A., Lacerda de Menezes, João R., Nedergaard, Maiken, Ribeiro Xavier, Anna L., Kress, Benjamin T., Goldman, Steven A., Lacerda de Menezes, João R., and Nedergaard, Maiken

Abstract

Microglia are involved in synaptic pruning both in development and in the mature CNS. In this study, we investigated whether microglia might further contribute to circuit plasticity by modulating neuronal recruitment from the neurogenic subventricular zone (SVZ) of the adult mouse striatum. We found that microglia residing in the SVZ and adjacent rostral migratory stream (RMS) comprise a morphologically and antigenically distinct phenotype of immune effectors. Whereas exhibiting characteristics of alternatively activated microglia, the SVZ/RMS microglia were clearly distinguished by their low expression of purinoceptors and lack of ATP-elicitable chemotaxis. Furthermore, the in vivo depletion of these microglia hampered the survival and migration of newly generated neuroblasts through the RMS to the olfactory bulb. SVZ and RMS microglia thus appear to comprise a functionally distinct class that is selectively adapted to the support and direction of neuronal integration into the olfactory circuitry. Therefore, this unique microglial subpopulation may serve as a novel target with which to modulate cellular addition from endogenous neural stem and progenitor cells of the adult brain.SIGNIFICANCE STATEMENT: Microglial cells are a specialized population of macrophages in the CNS, playing key roles as immune mediators. As integral components in the CNS, the microglia stand out for using the same mechanisms, phagocytosis and cytochemokine release, to promote homeostasis, synaptic pruning, and neural circuitry sculpture. Here, we addressed microglial functions in the subventricular zone (SVZ), the major postnatal neurogenic niche. Our results depict microglia as a conspicuous component of SVZ and its anterior extension, the rostral migratory stream, a pathway used by neuroblasts during their transit toward olfactory bulb layers. In addition to other unique populations residing in the SVZ niche, microglia display distinct morphofunctional properties that boost neur

Published

2015

41. Tumors of the lateral ventricles: a clinico-pathological study

Author

Ojha, Sandeep, Fernandes, Gwendolyn, Shenoy, Asha, Ojha, Sandeep, Fernandes, Gwendolyn, and Shenoy, Asha

Abstract

Introduction: Brain tumors are rare compared to other fatal and life-diminishing diseases and its incidence is increasing. The objective is to study the lateral ventricular tumors with reference to age groups, gender, anatomical location, the histopathological features including the histological grades, and the clinico- radio- pathological correlation of the above cases. Methodology: Retrospective analysis of tumors of the lateral ventricle of the CNS diagnosed in the department of Neuropathology at a tertiary care and referral hospital, from January 2001 to June 2009. Results: Average Incidence of primary lateral ventricular tumor was 1.6%, that tumor involve the left lateral ventricle (46.3%) more commonly than the right lateral ventricle (29.9%). Commonest tumors in our study were the Neuronal and mixed glioneuronal tumors [31%]. 78.1% of the lateral ventricular tumors were correctly diagnosed on radiology. Conclusion: Commonest tumors were Neuronal and mixed glioneuronal tumors. Most of the tumors belonged to low WHO grade. Fairly good correlation was found between radiological and histopathological diagnosis.

Published

2015

42. Tumors of the lateral ventricles: a clinico-pathological study

Author

Ojha, Sandeep, Fernandes, Gwendolyn, Shenoy, Asha, Ojha, Sandeep, Fernandes, Gwendolyn, and Shenoy, Asha

Abstract

Introduction: Brain tumors are rare compared to other fatal and life-diminishing diseases and its incidence is increasing. The objective is to study the lateral ventricular tumors with reference to age groups, gender, anatomical location, the histopathological features including the histological grades, and the clinico- radio- pathological correlation of the above cases. Methodology: Retrospective analysis of tumors of the lateral ventricle of the CNS diagnosed in the department of Neuropathology at a tertiary care and referral hospital, from January 2001 to June 2009. Results: Average Incidence of primary lateral ventricular tumor was 1.6%, that tumor involve the left lateral ventricle (46.3%) more commonly than the right lateral ventricle (29.9%). Commonest tumors in our study were the Neuronal and mixed glioneuronal tumors [31%]. 78.1% of the lateral ventricular tumors were correctly diagnosed on radiology. Conclusion: Commonest tumors were Neuronal and mixed glioneuronal tumors. Most of the tumors belonged to low WHO grade. Fairly good correlation was found between radiological and histopathological diagnosis.

Published

2015

43. Shape abnormalities of subcortical and ventricular structures in mild cognitive impairment and Alzheimer's disease: detecting, quantifying, and predicting.

Author

Tang, Xiaoying, Tang, Xiaoying, Holland, Dominic, Dale, Anders M, Younes, Laurent, Miller, Michael I, Alzheimer's Disease Neuroimaging Initiative, Tang, Xiaoying, Tang, Xiaoying, Holland, Dominic, Dale, Anders M, Younes, Laurent, Miller, Michael I, and Alzheimer's Disease Neuroimaging Initiative

Abstract

This article assesses the feasibility of using shape information to detect and quantify the subcortical and ventricular structural changes in mild cognitive impairment (MCI) and Alzheimer's disease (AD) patients. We first demonstrate structural shape abnormalities in MCI and AD as compared with healthy controls (HC). Exploring the development to AD, we then divide the MCI participants into two subgroups based on longitudinal clinical information: (1) MCI patients who remained stable; (2) MCI patients who converted to AD over time. We focus on seven structures (amygdala, hippocampus, thalamus, caudate, putamen, globus pallidus, and lateral ventricles) in 754 MR scans (210 HC, 369 MCI of which 151 converted to AD over time, and 175 AD). The hippocampus and amygdala were further subsegmented based on high field 0.8 mm isotropic 7.0T scans for finer exploration. For MCI and AD, prominent ventricular expansions were detected and we found that these patients had strongest hippocampal atrophy occurring at CA1 and strongest amygdala atrophy at the basolateral complex. Mild atrophy in basal ganglia structures was also detected in MCI and AD. Stronger atrophy in the amygdala and hippocampus, and greater expansion in ventricles was observed in MCI converters, relative to those MCI who remained stable. Furthermore, we performed principal component analysis on a linear shape space of each structure. A subsequent linear discriminant analysis on the principal component values of hippocampus, amygdala, and ventricle leads to correct classification of 88% HC subjects and 86% AD subjects.

Published

2014

44. Structural growth trajectories and rates of change in the first 3 months of infant brain development.

Author

Holland, Dominic, Holland, Dominic, Chang, Linda, Ernst, Thomas M, Curran, Megan, Buchthal, Steven D, Alicata, Daniel, Skranes, Jon, Johansen, Heather, Hernandez, Antonette, Yamakawa, Robyn, Kuperman, Joshua M, Dale, Anders M, Holland, Dominic, Holland, Dominic, Chang, Linda, Ernst, Thomas M, Curran, Megan, Buchthal, Steven D, Alicata, Daniel, Skranes, Jon, Johansen, Heather, Hernandez, Antonette, Yamakawa, Robyn, Kuperman, Joshua M, and Dale, Anders M

Abstract

ImportanceThe very early postnatal period witnesses extraordinary rates of growth, but structural brain development in this period has largely not been explored longitudinally. Such assessment may be key in detecting and treating the earliest signs of neurodevelopmental disorders.ObjectiveTo assess structural growth trajectories and rates of change in the whole brain and regions of interest in infants during the first 3 months after birth.Design, setting, and participantsSerial structural T1-weighted and/or T2-weighted magnetic resonance images were obtained for 211 time points from 87 healthy term-born or term-equivalent preterm-born infants, aged 2 to 90 days, between October 5, 2007, and June 12, 2013.Main outcomes and measuresWe segmented whole-brain and multiple subcortical regions of interest using a novel application of Bayesian-based methods. We modeled growth and rate of growth trajectories nonparametrically and assessed left-right asymmetries and sexual dimorphisms.ResultsWhole-brain volume at birth was approximately one-third of healthy elderly brain volume, and did not differ significantly between male and female infants (347 388 mm3 and 335 509 mm3, respectively, P = .12). The growth rate was approximately 1%/d, slowing to 0.4%/d by the end of the first 3 months, when the brain reached just more than half of elderly adult brain volume. Overall growth in the first 90 days was 64%. There was a significant age-by-sex effect leading to widening separation in brain sizes with age between male and female infants (with male infants growing faster than females by 200.4 mm3/d, SE = 67.2, P = .003). Longer gestation was associated with larger brain size (2215 mm3/d, SE = 284, P = 4×10-13). The expected brain size of an infant born one week earlier than average was 5% smaller than average; at 90 days it will not have caught up, being 2% smaller than average. The cerebellum grew at the highest rate, more than doubling in 90 days, and the hippocampus grew at the slo

Published

2014

45. Shape abnormalities of subcortical and ventricular structures in mild cognitive impairment and Alzheimer's disease: detecting, quantifying, and predicting.

Author

Tang, Xiaoying, Tang, Xiaoying, Holland, Dominic, Dale, Anders M, Younes, Laurent, Miller, Michael I, Alzheimer's Disease Neuroimaging Initiative, Tang, Xiaoying, Tang, Xiaoying, Holland, Dominic, Dale, Anders M, Younes, Laurent, Miller, Michael I, and Alzheimer's Disease Neuroimaging Initiative

Abstract

This article assesses the feasibility of using shape information to detect and quantify the subcortical and ventricular structural changes in mild cognitive impairment (MCI) and Alzheimer's disease (AD) patients. We first demonstrate structural shape abnormalities in MCI and AD as compared with healthy controls (HC). Exploring the development to AD, we then divide the MCI participants into two subgroups based on longitudinal clinical information: (1) MCI patients who remained stable; (2) MCI patients who converted to AD over time. We focus on seven structures (amygdala, hippocampus, thalamus, caudate, putamen, globus pallidus, and lateral ventricles) in 754 MR scans (210 HC, 369 MCI of which 151 converted to AD over time, and 175 AD). The hippocampus and amygdala were further subsegmented based on high field 0.8 mm isotropic 7.0T scans for finer exploration. For MCI and AD, prominent ventricular expansions were detected and we found that these patients had strongest hippocampal atrophy occurring at CA1 and strongest amygdala atrophy at the basolateral complex. Mild atrophy in basal ganglia structures was also detected in MCI and AD. Stronger atrophy in the amygdala and hippocampus, and greater expansion in ventricles was observed in MCI converters, relative to those MCI who remained stable. Furthermore, we performed principal component analysis on a linear shape space of each structure. A subsequent linear discriminant analysis on the principal component values of hippocampus, amygdala, and ventricle leads to correct classification of 88% HC subjects and 86% AD subjects.

Published

2014

46. Traumatic brain injury reveals novel cell lineage relationships within the subventricular zone.

Author

Thomsen, Gretchen M, Thomsen, Gretchen M, Le Belle, Janel E, Harnisch, Jessica A, Mc Donald, Whitney S, Hovda, David A, Sofroniew, Michael V, Kornblum, Harley I, Harris, Neil G, Thomsen, Gretchen M, Thomsen, Gretchen M, Le Belle, Janel E, Harnisch, Jessica A, Mc Donald, Whitney S, Hovda, David A, Sofroniew, Michael V, Kornblum, Harley I, and Harris, Neil G

Abstract

The acute response of the rodent subventricular zone (SVZ) to traumatic brain injury (TBI) involves a physical expansion through increased cell proliferation. However, the cellular underpinnings of these changes are not well understood. Our analyses have revealed that there are two distinct transit-amplifying cell populations that respond in opposite ways to injury. Mash1+ transit-amplifying cells are the primary SVZ cell type that is stimulated to divide following TBI. In contrast, the EGFR+ population, which has been considered to be a functionally equivalent progenitor population to Mash1+ cells in the uninjured brain, becomes significantly less proliferative after injury. Although normally quiescent GFAP+ stem cells are stimulated to divide in SVZ ablation models, we found that the GFAP+ stem cells do not divide more after TBI. We found, instead, that TBI results in increased numbers of GFAP+/EGFR+ stem cells via non-proliferative means-potentially through the dedifferentiation of progenitor cells. EGFR+ progenitors from injured brains only were competent to revert to a stem cell state following brief exposure to growth factors. Thus, our results demonstrate previously unknown changes in lineage relationships that differ from conventional models and likely reflect an adaptive response of the SVZ to maintain endogenous brain repair after TBI.

Published

2014

47. Structural growth trajectories and rates of change in the first 3 months of infant brain development.

Author

Holland, Dominic, Holland, Dominic, Chang, Linda, Ernst, Thomas M, Curran, Megan, Buchthal, Steven D, Alicata, Daniel, Skranes, Jon, Johansen, Heather, Hernandez, Antonette, Yamakawa, Robyn, Kuperman, Joshua M, Dale, Anders M, Holland, Dominic, Holland, Dominic, Chang, Linda, Ernst, Thomas M, Curran, Megan, Buchthal, Steven D, Alicata, Daniel, Skranes, Jon, Johansen, Heather, Hernandez, Antonette, Yamakawa, Robyn, Kuperman, Joshua M, and Dale, Anders M

Abstract

ImportanceThe very early postnatal period witnesses extraordinary rates of growth, but structural brain development in this period has largely not been explored longitudinally. Such assessment may be key in detecting and treating the earliest signs of neurodevelopmental disorders.ObjectiveTo assess structural growth trajectories and rates of change in the whole brain and regions of interest in infants during the first 3 months after birth.Design, setting, and participantsSerial structural T1-weighted and/or T2-weighted magnetic resonance images were obtained for 211 time points from 87 healthy term-born or term-equivalent preterm-born infants, aged 2 to 90 days, between October 5, 2007, and June 12, 2013.Main outcomes and measuresWe segmented whole-brain and multiple subcortical regions of interest using a novel application of Bayesian-based methods. We modeled growth and rate of growth trajectories nonparametrically and assessed left-right asymmetries and sexual dimorphisms.ResultsWhole-brain volume at birth was approximately one-third of healthy elderly brain volume, and did not differ significantly between male and female infants (347 388 mm3 and 335 509 mm3, respectively, P = .12). The growth rate was approximately 1%/d, slowing to 0.4%/d by the end of the first 3 months, when the brain reached just more than half of elderly adult brain volume. Overall growth in the first 90 days was 64%. There was a significant age-by-sex effect leading to widening separation in brain sizes with age between male and female infants (with male infants growing faster than females by 200.4 mm3/d, SE = 67.2, P = .003). Longer gestation was associated with larger brain size (2215 mm3/d, SE = 284, P = 4×10-13). The expected brain size of an infant born one week earlier than average was 5% smaller than average; at 90 days it will not have caught up, being 2% smaller than average. The cerebellum grew at the highest rate, more than doubling in 90 days, and the hippocampus grew at the slo

Published

2014

48. A novel method for long-term monitoring of intracranial pressure in rats

Author

Uldall, Maria, Juhler, Marianne, Skjolding, Anders Daehli, Kruuse, Christina, Jansen-Olesen, Inger, Jensen, Rigmor, Uldall, Maria, Juhler, Marianne, Skjolding, Anders Daehli, Kruuse, Christina, Jansen-Olesen, Inger, and Jensen, Rigmor

Abstract

BACKGROUND: In preclinical neurological studies, monitoring intracranial pressure (ICP) in animal models especially in rodents is challenging. Further, the lack of methods for long-term ICP monitoring has limited the possibilities to conduct prolonged studies on ICP fluctuations in parallel to disease progression or therapeutic interventions. For these reasons we aimed to set up a simple and valid method for long-term ICP recordings in rats.NEW METHOD: A novel ICP method employing epidural probes was developed and validated by simultaneously ICP recordings in the lateral ventricle and in the epidural space. The two pressures were recorded twice a week for 59 days and the correlation was studied.RESULTS: The two pressure recordings correlated exceptionally well and the R(2) values on each recording day ranged between 0.99 and 1.00. However, the ventricular probes caused a number of complications including loss of patency and tissue damage probably due to cerebral infection, whereas the epidural probes were safe and reliable throughout the entire study.COMPARISON WITH EXISTING METHODS: Epidural probes are much easier to implant than ventricular probes. In addition, these new probes are far less invasive and induce no apparent mechanical tissue damage and highly decrease the infection risk associated with ICP recordings.CONCLUSION: Epidural ICP recorded with this new method is identical to the ventricular ICP for at least 59 days but is far less complicated and safer for the animals. The long-term method described is reliable, valid, inexpensive, and may be used in multiple disease models to study ICP.

Published

2014

49. A novel method for long-term monitoring of intracranial pressure in rats

Author

Uldall, Maria, Juhler, Marianne, Skjolding, Anders Daehli, Kruuse, Christina, Jansen-Olesen, Inger, Jensen, Rigmor, Uldall, Maria, Juhler, Marianne, Skjolding, Anders Daehli, Kruuse, Christina, Jansen-Olesen, Inger, and Jensen, Rigmor

Abstract

BACKGROUND: In preclinical neurological studies, monitoring intracranial pressure (ICP) in animal models especially in rodents is challenging. Further, the lack of methods for long-term ICP monitoring has limited the possibilities to conduct prolonged studies on ICP fluctuations in parallel to disease progression or therapeutic interventions. For these reasons we aimed to set up a simple and valid method for long-term ICP recordings in rats.NEW METHOD: A novel ICP method employing epidural probes was developed and validated by simultaneously ICP recordings in the lateral ventricle and in the epidural space. The two pressures were recorded twice a week for 59 days and the correlation was studied.RESULTS: The two pressure recordings correlated exceptionally well and the R(2) values on each recording day ranged between 0.99 and 1.00. However, the ventricular probes caused a number of complications including loss of patency and tissue damage probably due to cerebral infection, whereas the epidural probes were safe and reliable throughout the entire study.COMPARISON WITH EXISTING METHODS: Epidural probes are much easier to implant than ventricular probes. In addition, these new probes are far less invasive and induce no apparent mechanical tissue damage and highly decrease the infection risk associated with ICP recordings.CONCLUSION: Epidural ICP recorded with this new method is identical to the ventricular ICP for at least 59 days but is far less complicated and safer for the animals. The long-term method described is reliable, valid, inexpensive, and may be used in multiple disease models to study ICP.

Published

2014

50. MRI Biomarkers and Modifiable Health Factors of Aging and Dementia

Author

Madsen, Sarah, Thompson, Paul M1, Madsen, Sarah, Madsen, Sarah, Thompson, Paul M1, and Madsen, Sarah

Abstract

Alzheimer's dementia is a rising public health crisis that will have an unprecedented social and economic impact in the near future, as elderly individuals make up the fastest growing segment of the population worldwide. The greatest single risk factor for Alzheimer's disease is age, though many genetic and environmental factors also influence disease onset and progression. While current treatment options are sparse and no cure exists, it is critical to (1) identify the disease at its earliest stages, before irreversible brain degeneration has occurred and (2) to develop alternative strategies for reducing dementia risk based on aspects of health that are currently modifiable, such as cardiovascular health as one example. If we can identify individuals who are at high risk for developing Alzheimer's dementia, but who have not yet experienced major neurodegeneration, then it may be possible to apply these alternative strategies to preserve brain health into old age.In regards to the first aim, brain MRI scans identify robust signatures of Alzheimer's dementia at early stages. In my work, we have expanded upon existing brain-based MRI biomarkers by demonstrating changes in caudate nucleus shape in Alzheimer's disease and by showing that patterns of thinner cortical gray matter are associated with longitudinal expansion of the lateral ventricles. The caudate nucleus is a subcortical gray matter structure typically associated with motor planning, but is also involved in procedural memory, and is affected by the molecular pathology of Alzheimer's disease. The lateral ventricles are a fluid-filled space located at the center of the brain, which expand as brain tissue is lost in aging and dementia, within the fixed volume of the skull. Both of these biomarkers can be automatically measured from brain scans with high reliability and often with less manual intervention compared to other brain structures (such as the hippocampus). These biomarkers makes are candidates for use

Published

2013