Yue Guo scite author profile

The chorio-allantoic placenta forms through the fusion of the allantois (progenitor tissue of the umbilical cord), with the chorionic plate. The murine placenta contains high levels of hematopoietic stem cells, and is therefore a stem cell niche. However, it is not known whether the placenta is a site of hematopoietic cell emergence, or whether hematopoietic cells originate from other sites in the conceptus and then colonize the placenta. Here, we show that the allantois and chorion, isolated prior to the establishment of circulation, have the potential to give rise to myeloid and definitive erythroid cells following explant culture. We further show that the hematopoietic potential of the allantois and chorion does not require their union, indicating that it is an intrinsic property of these tissues. These results suggest that the placenta is not only a niche for, but also a source of, hematopoietic cells.

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Core binding factors are necessary for natural killer cell development and cooperate with Notch signaling during T-cell specification

Guo

Maillard

Chakraborti

et al. 2008

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Telomere maintenance in human B lymphocytes

et al. 2002

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Summary. Telomere shortening has been causally linked to replicative senescence in human cells. To characterize telomere-length heterogeneity in peripheral blood cells of normal individuals, we analysed the mean length of telomeric repeat sequences in subpopulations of peripheral blood leucocytes, using fluorescence in situ hybridization and flow cytometry (flow-FISH). Although the telomere length of most haematopoietic subsets was within the same range, the mean telomere length was found to be 15% higher in B compared with T lymphocytes in adult peripheral blood. Whereas telomere loss with ageing corresponded to 33 base pairs (bp) per year in T cells, telomere shortening was slower in B cells, corresponding to 15 bp per year. Separation of adult B-lymphocyte subpopulations based on CD27 expression revealed that telomere length was almost 2 kb longer in CD19 + CD27 + (memory) compared with CD19 + CD27 -(naive) cells. Furthermore, peripheral blood B cells were activated in vitro. Whereas B-cell activation with Staphylococcus aureus Cowan strain (SAC) did not increase telomere length, a striking telomere elongation was observed when cells were stimulated with SAC and interleukin 2 to induce plasma cell differentiation. Our observations support the concept that telomere dynamics in B cells are distinct from other haematopoietic cell lineages and that telomere elongation may play an essential role in the generation of long-term B memory cells.

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CD34⁻Hematopoietic Stem Cells: Current Concepts and Controversies

2003

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Yue Guo

The allantois and chorion, when isolated before circulation or chorio-allantoic fusion, have hematopoietic potential

Core binding factors are necessary for natural killer cell development and cooperate with Notch signaling during T-cell specification

Telomere maintenance in human B lymphocytes

CD34⁻Hematopoietic Stem Cells: Current Concepts and Controversies

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Resources

About

Yue Guo

The allantois and chorion, when isolated before circulation or chorio-allantoic fusion, have hematopoietic potential

Core binding factors are necessary for natural killer cell development and cooperate with Notch signaling during T-cell specification

Telomere maintenance in human B lymphocytes

CD34−Hematopoietic Stem Cells: Current Concepts and Controversies

Contact Info

Product

Resources

About

CD34⁻Hematopoietic Stem Cells: Current Concepts and Controversies