Expression of tetraspanins in peripheral blood leukocytes: a comparison between normal and infectious conditions

Tohami, Tali; Drucker, Liat; Radnay, Judith; Shapira, Hava; Lishner, Michael

doi:10.1111/j.1399-0039.2004.00271.x

Cited by 35 publications

(30 citation statements)

References 38 publications

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“…This role suggests that localized release of blocking antibodies against CD9 might have potential as a general and more effective antiinflammatory therapy than the single inhibition of one of these adhesion molecules. However, CD9 is not only expressed by endothelial cells but also by a number of blood cell subsets (including platelets, neutrophils, and monocytes) (7,20). Therefore, the administration of CD9 blockers would require a localized release in inflammatory foci, which could be accomplished by their combination with antibodies against any inflammatory marker in the same MB.…”

Section: Study Of Endothelial Viability After High Mechanical Indexmentioning

confidence: 97%

Specific Targeting of Human Inflamed Endothelium and In Situ Vascular Tissue Transfection by the Use of Ultrasound Contrast Agents

Barreiro

Aguilar

Tejera

et al. 2009

JACC: Cardiovascular Imaging

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Section: Study Of Endothelial Viability After High Mechanical Indexmentioning

confidence: 97%

Specific Targeting of Human Inflamed Endothelium and In Situ Vascular Tissue Transfection by the Use of Ultrasound Contrast Agents

Barreiro

Aguilar

Tejera

et al. 2009

JACC: Cardiovascular Imaging

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“…Interestingly, in both experimental conditions (low and high doses), the age with the maximal number of modulated genes presented an important cluster related to immune response, including Ctse (Sealy et al 1996), Cd53 (Tohami et al 2004), Cd3d (Fischer et al 2005), or secretory leukocyte peptidase inhibitor (Slpi; King et al 2003). In addition, the cytoskeletal protein Coronin-1A (Coro1a), also found up-modulated by effect of low and high doses at 50 and 100 days respectively, has been reported to play a role in T cell differentiation/activation events (Nal et al 2004).…”

Section: Discussionmentioning

confidence: 99%

Effect of prenatal exposure to the endocrine disruptor bisphenol A on mammary gland morphology and gene expression signature

Moral

Wang²,

Russo³

et al. 2007

Journal of Endocrinology

145

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Bisphenol A (BPA), known as an environmental endocrine disruptor, is widely used as a plasticizer. This study aims to investigate whether exposure in utero to BPA alters the architecture, proliferative index, and genomic signature of the rat mammary gland during critical stages of development. Pregnant rats were gavaged with 25 mg BPA/kg body weight (BW; low-dose group) or 250 mg BPA/kg BW (high-dose group) from day 10 post-conception to delivery. Female litters were euthanized at 21, 35, 50, and 100 days, and mammary glands were collected. Analysis of gland morphology was performed from whole-mounted mammary tissue, while proliferative index was determined by detection of bromodeoxyuridine incorporation in the epithelial cells. Genomic profiles were obtained by microarray analysis, and some genes were validated by real-time RT-PCR. BPA exposure induced changes in the mammary gland that were time and dose specific. High-dose exposure resulted in architectural modifications, mainly in the number of undifferentiated epithelial structures of the breast tissue. Proliferative index did not show remarkable differences by the effect of BPA. Low and high doses of BPA changed the gene expression signature of the mammary gland following a different fashion: low dose had the highest effect by 50 days, while high dose had a highest influence on gene expression by 100 days. Both doses presented a significant cluster of up-modulated genes related to the immune system at the age of maximal changes. Moreover, high-dose exposure induced changes in genes related to differentiation suggesting alterations in the normal development of the gland. The increase of undifferentiated structures and the changes in the gene expression profile at different ages suggest that prenatal exposure to BPA can affect the susceptibility of the mammary gland to transformation.

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“…Integrin-␣x (CD11c) and CD81 mRNA were both downregulated significantly in this study. This cannot be attributed to cellular shifts, since CD11c is strongly or moderately expressed in monocytes, macrophages, NK cells and granulocytes, while it is low in T and B cells (26), and CD81 is expressed on polymorphonuclears (PMN), monocytes, and B and T lymphocytes (59). The lymphocytes are the minor population and therefore can hardly explain the strong 50% overall downregulation of gene expression.…”

Section: Gene Expression Changes Not Attributable To Obvious Cellularmentioning

confidence: 99%

cDNA microarray analysis reveals novel candidate genes expressed in human peripheral blood following exhaustive exercise

Zieker

Fehrenbach

Dietzsch

et al. 2005

Physiological Genomics

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Expression of tetraspanins in peripheral blood leukocytes: a comparison between normal and infectious conditions

Cited by 35 publications

References 38 publications

Specific Targeting of Human Inflamed Endothelium and In Situ Vascular Tissue Transfection by the Use of Ultrasound Contrast Agents

Specific Targeting of Human Inflamed Endothelium and In Situ Vascular Tissue Transfection by the Use of Ultrasound Contrast Agents

Effect of prenatal exposure to the endocrine disruptor bisphenol A on mammary gland morphology and gene expression signature

cDNA microarray analysis reveals novel candidate genes expressed in human peripheral blood following exhaustive exercise

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