A Subpopulation of Olfactory Bulb GABAergic Interneurons Is Derived from Emx1- and Dlx5/6-Expressing Progenitors

Kohwi, Minoree; Petryniak, Magdalena A.; Long, Jason E.; Ekker, Marc; Obata, Kunihiko; Yanagawa, Yuchio; Rubenstein, John L.R.; Alvarez-Buylla, Arturo

doi:10.1523/jneurosci.0254-07.2007

Cited by 234 publications

(323 citation statements)

References 49 publications

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“…2, available at www.jneurosci.org as supplemental material). Consistent with the predominantly embryonic origin of calbindinϩ neurons (De Marchis et al, 2007) (but see Kohwi et al, 2007), this subset was consistently ␤-galactosidasenegative (supplemental Fig. 2a, available at www.jneurosci.org as supplemental material).…”

Section: Resultssupporting

confidence: 60%

“…These studies revealed that between 10 and 30,000 cells are generated per day (Alvarez-Buylla et al, 2001;Cameron and McKay, 2001) and that about half of these die within the first 4 weeks (Petreanu and Alvarez-Buylla, 2002;Kempermann et al, 2003;Lemasson et al, 2005). Whereas some studies suggested that most cells that survived initial 4 weeks could still be detected after several months (Kempermann et al, 2003;Lemasson et al, 2005), others reported a further decrease in the number of labeled neurons during 365 d of survival (Petreanu and Alvarez-Buylla, 2002;Kohwi et al, 2007). Extrapolating these data from labeling a single or few cohorts would suggest a considerable contribution of adultgenerated neurons to the OB network, leading several studies to propose an increase in the size of the dentate gyrus (DG) and the OB attributable to adult neurogenesis (Kempermann et al, 2003;Merson et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

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Distinct Modes of Neuron Addition in Adult Mouse Neurogenesis

Ninkovic¹,

Mori²,

Götz³

2007

J. Neurosci.

230

205

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Adult neurogenesis is restricted to two distinct areas of the mammalian brain: the olfactory bulb (OB) and the dentate gyrus (DG). Despite its spatial restriction, adult neurogenesis is of crucial importance for sensory processing and learning and memory. Although it has been shown that tens of thousands of new neurons arrive in the OB and DG every day with about half of them surviving after integration, the total contribution of adult neurogenesis to the pre-existing network remains mostly unknown. This is because of previous approaches labeling only a small proportion of adult-generated neurons. Here, we used genetic fate mapping to follow the majority of adult-generated neurons over long periods. Our data demonstrate two distinct modes of neuron addition to the pre-existing network. In the glomerular layer of the OB, there is a constant net addition of adult-generated neurons reaching a third of the total neuronal population within 9 months. In contrast, adult neurogenesis contributes to only a minor fraction of the entire neuronal network in the granular cell layer of the OB and the DG. Although the fraction of adult generated neurons can be further increased by an enriched environment, it still remains a minority of the neuronal network in the DG. Thus, neuron addition is distinct and tightly regulated in the neuronal networks that incorporate new neurons life long.

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Section: Resultssupporting

confidence: 60%

Section: Introductionmentioning

confidence: 99%

Distinct Modes of Neuron Addition in Adult Mouse Neurogenesis

Ninkovic¹,

Mori²,

Götz³

2007

J. Neurosci.

230

205

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“…Consistent with our in vivo results, the ratio of TH + neurons to Tubb3 + neurons was also increased in dissociated cell cultures prepared from the OB of E16.5 Gnao −/− mice, whereas the ratio of CB + neurons to Tubb3 + neurons was decreased. Given that TH + and CB + neurons originate from a common progenitor pool in the dorsal lateral ganglionic eminence during the embryonic period and CR + neurons are derived from progenitor cells located elsewhere (38), it is likely that the reciprocal changes in the number of TH + cells and CB + cells in the OB of Gnao −/− mice are attributable to altered cell-type specification rather than to 6. Model for the roles of the VNO and MOE in the response of male mice to pheromones.…”

Section: Discussionmentioning

confidence: 99%

Development of the main olfactory system and main olfactory epithelium-dependent male mating behavior are altered in G _o -deficient mice

Choi

Kim

Choi

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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In mammals, initial detection of olfactory stimuli is mediated by sensory neurons in the main olfactory epithelium (MOE) and the vomeronasal organ (VNO). The heterotrimeric GTP-binding protein G o is widely expressed in the MOE and VNO of mice. Early studies indicated that G o expression in VNO sensory neurons is critical for directing social and sexual behaviors in female mice [Oboti L, et al. (2014) BMC Biol 12:31]. However, the physiological functions of G o in the MOE have remained poorly defined. Here, we examined the role of G o in the MOE using mice lacking the α subunit of G o . Development of the olfactory bulb (OB) was perturbed in mutant mice as a result of reduced neurogenesis and increased cell death. The balance between cell types of OB interneurons was altered in mutant mice, with an increase in the number of tyrosine hydroxylase-positive interneurons at the expense of calbindin-positive interneurons. Sexual behavior toward female mice and preference for female urine odors by olfactory sensory neurons in the MOE were abolished in mutant male mice. Our data suggest that G o signaling is essential for the structural and functional integrity of the MOE and for specification of OB interneurons, which in turn are required for the transmission of pheromone signals and the initiation of mating behavior with the opposite sex.heterotrimeric G o protein | olfactory mucosa | olfactory bulb interneuron | tyrosine monooxygenase | sexual behavior P heromones evoke diverse social and sexual behaviors in animals of the same species. In mammals, initial detection of olfactory stimuli is mediated by sensory neurons in the main olfactory epithelium (MOE) and vomeronasal organ (VNO). Early studies indicated that the VNO is largely responsible for the detection of pheromones and the consequent direction of social and sexual behaviors (1). VNO sensory neurons (VSNs) express distinct types of vomeronasal receptors: type 1 (V1Rs) in the apical region and type 2 (V2Rs) in the basal region. These receptors couple, respectively, to G i and G o members of the heterotrimeric GTPbinding protein family. It has been suggested that, following ligand binding to V1Rs and V2Rs, the Gβγ subunits released from G i and G o activate phospholipase C and increase the intracellular concentration of Ca 2+ . Ca 2+ ions induce opening of small Ca 2+ -activated K + (SK3) channels, subsequently activating Ca 2+ -activated Cl − channels (CACCs). In the VNO, Gβγ can also directly induce the opening of G protein-activated inward rectifying K + (GIRK) channels independently of transient receptor potential cation channel C2 (TRPC2) (2). Because of the VNO's high luminal K + concentration (2), opening of SK3 and GIRK channels leads to depolarization of VSNs and transmission of pheromone signals. Targeted deletion of the TRPC2 gene abrogates gender identification and intermale aggression without affecting male-to-female mating behavior in male mice (3, 4). Targeted deletion of the GIRK1 gene partially attenuates mating behavior of the male toward fem...

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“…Our studies demonstrate that, at any postnatal age, at least 50% of the NG2 + cells in the SVZ are proliferative and that Cdk2 is a major molecular regulator of their proliferation throughout postnatal development (Belachew et al, 2002;Jablonska et al, 2007). The results of our previous studies also defined the following cellular and molecular properties of NG2 + cells in the SVZ Jablonska et al, 2007): i) NG2 + cells are found scattered through the wall of the lateral ventricle, but they are more abundant in the anterior SVZ; ii) NG2 + cells in the SVZ constitute approximately 12% and 3% of the total cell population at P8 and P30-60, respectively; iii) NG2 + cells in the SVZ are highly proliferative, as demonstrated by the percentages of NG2 + Ki67 + cells in the SVZ -56 and 32% at P8 and P30, respectively; iv) NG2 + cells of the SVZ express cellular markers of neural progenitor cells and stem cells, including the Lewis X antigen (LeX) (Capela and Temple, 2003), and the transcription factors Mash1, Olig2, and Dlx (Doetsch et al, 2002;Parras et al, 2004;Marshall et al, 2005;Menn et al, 2006;Kohwi et al, 2007;Parras et al, 2007); and v) NG2 + cells of the SVZ display a type-C cell phenotype, including expression of the EGFR, PSA-NCAM, and nestin (Capela and Temple, 2002;Doetsch et al, 2002). Consistent with our findings, other reports have also described the presence of NG2 + cells in the SVZ, and demonstrated diverse cellular and molecular properties of these progenitors in this neurogenic region, including co-expression of DCX Tamura et al, 2007), responsiveness to sonic hedgehog (Loulier et al, 2006), and Islet-1-induced migration into striatum (Rogelius et al, 2006).…”

Section: Discussionmentioning

confidence: 99%

Reduced EGFR signaling in progenitor cells of the adult subventricular zone attenuates oligodendrogenesis after demyelination

Aguirre

Gallo

2007

Neuron Glia Biol.

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Neural progenitor cells expressing the NG2 proteoglycan are found in different regions of the adult mammalian brain, where they display distinct morphologies and proliferative rates. In the developing postnatal and adult mouse, NG2 + cells represent a major cell population of the subventricular zone (SVZ). NG2 + cells divide in the anterior and lateral region of the SVZ, and are stimulated to proliferate and migrate out of the SVZ by focal demyelination of the corpus callosum (CC). Many NG2 + cells are labeled by GFP-retrovirus injection into the adult SVZ, demonstrating that NG2 + cells actively proliferate under physiological conditions and after demyelination. In the wa2 mouse, which is characterized by reduced EGFR signaling, NG2 + cell proliferation, under normal physiological conditions and after focal demyelination, is significantly attenuated. This results in reduced SVZ-to-lesion migration of NG2 + cells and oligodendrogenesis in the lesion. Expression of VEGF and EGFR ligands, such as HB-EGF and TGF-alpha, is upregulated in the SVZ after focal demyelination of the CC. EGF-induced oligodendrogenesis and myelin protein expression in cultured wild-type SVZ cells were significantly attenuated in wa2 SVZ cells. Our results demonstrate that the NG2 + cell response in the SVZ and their subsequent differentiation in CC after focal demyelination are dependent upon EGFR signaling.

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A Subpopulation of Olfactory Bulb GABAergic Interneurons Is Derived from Emx1- and Dlx5/6-Expressing Progenitors

Abstract: The subventricular zone (SVZ) of the postnatal brain continuously generates olfactory bulb (OB) interneurons. We show that calretinin ϩ , calbindin ϩ , and dopaminergic (TH

Cited by 234 publications

References 49 publications

Distinct Modes of Neuron Addition in Adult Mouse Neurogenesis

Distinct Modes of Neuron Addition in Adult Mouse Neurogenesis

Development of the main olfactory system and main olfactory epithelium-dependent male mating behavior are altered in G _o -deficient mice

Reduced EGFR signaling in progenitor cells of the adult subventricular zone attenuates oligodendrogenesis after demyelination

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A Subpopulation of Olfactory Bulb GABAergic Interneurons Is Derived from Emx1- and Dlx5/6-Expressing Progenitors

Abstract: The subventricular zone (SVZ) of the postnatal brain continuously generates olfactory bulb (OB) interneurons. We show that calretinin ϩ , calbindin ϩ , and dopaminergic (TH

Cited by 234 publications

References 49 publications

Distinct Modes of Neuron Addition in Adult Mouse Neurogenesis

Distinct Modes of Neuron Addition in Adult Mouse Neurogenesis

Development of the main olfactory system and main olfactory epithelium-dependent male mating behavior are altered in G o -deficient mice

Reduced EGFR signaling in progenitor cells of the adult subventricular zone attenuates oligodendrogenesis after demyelination

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Resources

About

Development of the main olfactory system and main olfactory epithelium-dependent male mating behavior are altered in G _o -deficient mice