Separate Proteolipid Protein/DM20 Enhancers Serve Different Lineages and Stages of Development

Tuason, Maria Clarita; Rastikerdar, Ali; Kuhlmann, Tanja; Goujet‐Zalc, C.; Zalc, Bernard; Dib, Samar; Friedman, Hana; Peterson, Alan C.

doi:10.1523/jneurosci.4579-07.2008

Cited by 30 publications

(46 citation statements)

References 66 publications

(74 reference statements)

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“…We demonstrate the Plp promoter cassette's capability to drive expression of a Cre recombinase transgene within the CNS, but in a more widespread pattern than initially anticipated. This was particularly true at early developmental stages when the transgene was expressed in neural tissues, and not restricted to the oligodendrocyte lineage, results corroborated by the work of others [3], [14], [16], [21]. During this time, transgene expression was also localized to the PNS (sciatic nerve, ventral and dorsal roots), most likely in Schwann cells.…”

Section: Discussionsupporting

confidence: 82%

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The Proteolipid Protein Promoter Drives Expression outside of the Oligodendrocyte Lineage during Embryonic and Early Postnatal Development

et al. 2011

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The proteolipid protein (Plp) gene promoter is responsible for driving expression of one of the major components of myelin – PLP and its splice variant DM-20. Both products are classically thought to express predominantly in oligodendrocytes. However, accumulating evidence suggests Plp expression is more widespread than previously thought. In an attempt to create a mouse model for inducing oligodendrocyte-specific gene deletions, we have generated transgenic mice expressing a Cre recombinase cDNA under control of the mouse Plp promoter. We demonstrate Plp promoter driven Cre expression is restricted predominantly to mature oligodendrocytes of the central nervous system (CNS) at postnatal day 28. However, crosses into the Rosa26LacZ and mT/mG reporter mouse lines reveal robust and widespread Cre activity in neuronal tissues at E15.5 and E10.5 that is not strictly oligodendrocyte lineage specific. By P28, all CNS tissues examined displayed high levels of reporter gene expression well outside of defined white matter zones. Importantly, our study reinforces the emerging idea that Plp promoter activity is not restricted to the myelinating cell lineage, but rather, has widespread activity both during embryonic and early postnatal development in the CNS. Specificity of the promoter to the oligodendrocyte cell lineage, as shown through the use of a tamoxifen inducible Plp-CreERt line, occurs only at later postnatal stages. Understanding the temporal shift in Plp driven expression is of consequence when designing experimental models to study oligodendrocyte biology.

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Section: Discussionsupporting

confidence: 82%

“…Although the promoter is generally considered oligodendrocyte lineage specific, accumulating evidence suggests a Plp expression pattern outside of defined white matter zones; included are both glial and neuronal CNS subpopulations, implying a role for Plp in activities independent of myelination [11], [12], [13], [14], [15], [16].…”

Section: Introductionmentioning

confidence: 99%

The Proteolipid Protein Promoter Drives Expression outside of the Oligodendrocyte Lineage during Embryonic and Early Postnatal Development

et al. 2011

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“…The wmN2 region was identified in the same study as wmN1, and is believed to mediate high level expression in Schwann cells and their progenitors, dorsal root ganglion (DRG) satellite cells and OECs, and weak expression in oligodendrocyte lineage cells (Tuason et al, 2008). Results presented here suggest that activity of the wmN1 enhancer extends beyond the cell types initially identified by Tuason and coworkers (2008), and includes those ascribed as being regulated by the wmN2 enhancer. It is possible that there is partial redundancy in the cell types affected by the two enhancers, or alternatively, species-specific differences may exist between the enhancers in human and mouse.…”

Section: Discussionmentioning

confidence: 95%

The wmN1 enhancer region in intron 1 is required for expression of human PLP1

Hamdan

Patyal

Kockara

et al. 2018

Glia

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The myelin proteolipid protein gene (PLP1) encodes the most abundant protein present in myelin from the central nervous system (CNS). Its expression must be tightly controlled as evidenced by mutations that alter PLP1 dosage; both overexpression (elevated PLP1 copy number) and lack thereof (PLP1 deletion) result in X-linked genetic disorders in man. However, not much is known about the mechanisms that govern expression of the human gene. To address this, transgenic mice were generated which utilize human PLP1 (hPLP1) sequences (proximal 6.2 kb of 5'-flanking DNA to the first 38 bp of exon 2) to drive expression of a lacZ reporter cassette. LoxP sites were incorporated around a 1.5-kb section of hPLP1 intron 1 since it contains sequence orthologous to the wmN1 region from mouse which, previously, was shown to augment expression of a minimally-promoted transgene coincident with the active myelination period of CNS development. Eight transgenic lines were generated with the parental, 6.2hPLP(+)Z/FL, transgene. All lines expressed the transgene appropriately in brain as evidenced by staining with X-gal in white matter regions and olfactory bulb. Removal of the "wmN1" region from 6.2hPLP(+)Z/FL with a ubiquitously expressed Cre-driver caused a dramatic reduction in transgene activity. These results demonstrate for the first time that the wmN1 enhancer region: (1) is functional in hPLP1; (2) works in collaboration with its native promoter-not just a basal heterologous promoter; (3) is required for high levels of hPLP1 gene activity; (4) has a broader effect, both spatially and temporally, than originally projected with mPlp1.

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“…The plp gene encodes myelin proteolipid protein in myelinating oligodendrocytes and a smaller isoform, DM-20, which, in the mouse, is expressed in embryonic neuroepithelial cells (embryonic day 9.1, E9.5), radial glial cells (E13.5) and progenitors expressing the proteoglycan, NG2 (E14.5) (Ikenaka et al, 1992; Timsit et al, 1992; Timsit et al, 1995; Spassky et al, 1998; Belachew et al, 2001; Tuason et al, 2008; Delaunay et al, 2008). These plp promoter expressing embryonic progenitors are multipotent both in vivo and in vitro , giving rise to oligodendrocytes, astrocytes and neurons (Le Bras et al, 2005; Delaunay et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

Early Postnatal Proteolipid Promoter-Expressing Progenitors Produce Multilineage CellsIn Vivo

Guo¹,

Ma²,

McCauley³

et al. 2009

J. Neurosci.

122

140

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Proteolipid promoter (plp promoter) activity in the newborn mouse CNS is restricted to NG2-expressing oligodendroglial progenitor cells and oligodendrocytes. There are two populations of NG2 progenitors based on their plp promoter expression. Whereas the general population of NG2 progenitors has been shown to be multipotent in vitro and after transplantation, it is not known whether the subpopulation of plp promoter-expressing NG2 progenitors [i.e., plp promoter-expressing NG2 progenitors (PPEPs)] has the potential to generate multilineage cells during normal development in vivo. We addressed this issue by fate mapping Plp-Cre-ER T2 /Rosa26-EYFP (PCE/R) double-transgenic mice, which carried an inducible Cre gene under the control of the plp promoter. Expression of the enhanced yellow fluorescent protein (EYFP) reporter gene in PPEPs was elicited by administering tamoxifen to postnatal day 7 PCE/R mice. We have demonstrated that early postnatal PPEPs, which had been thought to be restricted to the oligodendroglial lineage, also unexpectedly gave rise to a subset of immature, postmitotic, protoplasmic astrocytes in the gray matter of the spinal cord and ventral forebrain, but not in white matter. Furthermore, these PPEPs also gave rise to small numbers of immature, DCX (doublecortin)-negative neurons in the ventral forebrain, dorsal cerebral cortex, and hippocampus. EYFP-labeled representatives of each of these lineages survived to adulthood. These findings indicate that there are regional differences in the fates of neonatal PPEPs, which are multipotent in vivo, giving rise to oligodendrocytes, astrocytes, and neurons.

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Separate Proteolipid Protein/DM20 Enhancers Serve Different Lineages and Stages of Development

Cited by 30 publications

References 66 publications

The Proteolipid Protein Promoter Drives Expression outside of the Oligodendrocyte Lineage during Embryonic and Early Postnatal Development

The Proteolipid Protein Promoter Drives Expression outside of the Oligodendrocyte Lineage during Embryonic and Early Postnatal Development

The wmN1 enhancer region in intron 1 is required for expression of human PLP1

Early Postnatal Proteolipid Promoter-Expressing Progenitors Produce Multilineage CellsIn Vivo

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