Abstract
BackgroundDeregulation of platelet-derived growth factor (PDGF) signaling is a hallmark of malignant glioma. Two alternatively spliced PDGF-A mRNAs have been described, corresponding to a long (L) and a short (S) isoform of PDGF-A. In contrast to PDGF-A(S), the PDGF-A(L) isoform has a lysine and arginine rich carboxy-terminal extension that acts as an extracellular matrix retention motif. However, the exact role of PDGF-A(L) and how it functionally differs from the shorter isoform is not well understood.Methodology/Principal FindingsWe overexpressed PDGF-A(L) as a transgene under control of the glial fibrillary acidic protein (GFAP) promoter in the mouse brain. This directs expression of the transgene to astrocytic cells and GFAP expressing neural stem cells throughout the developing and adult central nervous system. Transgenic mice exhibited a phenotype with enlarged skull at approximately 6-16 weeks of age and they died between 1.5 months and 2 years of age. We detected an increased number of undifferentiated cells in all areas of transgene expression, such as in the subependymal zone around the lateral ventricle and in the cerebellar medulla. The cells stained positive for Pdgfr-α, Olig2 and NG2 but this population did only partially overlap with cells positive for Gfap and the transgene reporter. Interestingly, a few mice presented with overt neoplastic glioma-like lesions composed of both Olig2 and Gfap positive cell populations and with microvascular proliferation, in a wild-type p53 background.ConclusionsOur findings show that PDGF-A(L) can induce accumulation of immature cells in the mouse brain. The strong expression of NG2, Pdgfr-α and Olig2 in PDGF-A(L) brains suggests that a fraction of these cells are oligodendrocyte progenitors. In addition, accumulation of fluid in the subarachnoid space and skull enlargement indicate that an increased intracranial pressure contributed to the observed lethality.
Highlights
The family of platelet-derived growth factor (PDGF) includes four different polypeptides: PDGF-A, -B, -C and -D, encoded by four different genes [1]
Our findings show that PDGF-A(L) can induce accumulation of immature cells in the mouse brain
The strong expression of NG2, Pdgfr-a and Olig2 in PDGF-A(L) brains suggests that a fraction of these cells are oligodendrocyte progenitors
Summary
The family of platelet-derived growth factor (PDGF) includes four different polypeptides: PDGF-A, -B, -C and -D, encoded by four different genes [1]. Exon number 6 in both PDGFA and –B encodes a highly basic stretch of 18 amino acids with a high proportion of lysine and arginine at the carboxy-terminus. This positively charged retention motif can associate with heparin/ heparan sulfate proteoglycans of the extracellular matrix [4]. PDGF-A exists as two isoforms corresponding to a long (L) and a short (S) form due to alternative splicing of exon 6 [5]. The exact role of PDGF-A(L) and how it functionally differs from the shorter isoform is not well understood
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