In vitro and in vivo cell surface expression of a thiol-specific antioxidant-like protein in Candida albicans

We have set up a fast and easy methodology to identify cell-surface proteins in live yeasts. A non-gel proteomic approach was based on a short period of trypsin treatment followed by peptide separation and identification using nano-LC followed by off-line MS/MS. Candida albicans was used as a model

## Abstract We investigated the cell‐killing efficacy of UV light on cancer cells expressing GFP in the nucleus and RFP in the cytoplasm (dual‐color cells). After exposure to various doses of UVA, UVB, or UVC, apoptotic and viable cells were quantitated under fluorescence microscopy using dual‐colo

## Abstract Osteogenic supplements are a requirement for osteoblastic cell differentiation during in vitro culture of human calvarial suture‐derived cell populations. We investigated the ability of ascorbic acid and β‐glycerophosphate with and without the addition of dexamethasone to stimulate in v

Parthenogenetic embryos, which are produced by the spontaneous or artificial stimulation of the oocyte, partially develop in the complete absence of the male gamete but fail to produce live young in many mammalian species. The identification of developmentally regulated molecules on the cell surface

## Abstract Sulfolipid‐immobilizing protein 1 (SLIP1) is a germ cell plasma membrane protein that binds specifically to sulfogalactosylglycerolipid, a sulfoglycolipid found preferentially in mammalian male germ cells (Lingwood, Can. J. Biochem. Cell. Biol. 63:1077–1085, 1985b). SLIP1 in mouse and r

## Abstract There is increasing evidence that chemokines, specialized regulators of the peripheral immune system, are also involved in the physiology and pathology of the CNS. It is known that glial cells (astrocytes and microglia) express various chemokine receptors like CCR1, ‐3, ‐5, and CXCR4. W