The CD44 Receptor of Lymphoma Cells: Structure-Function Relationships and Mechanism of Activation

Rochman, Mark; Moll, Jürgen; Herrlich, Peter; Wallach, Shulamit Batya; Nedvetzki, Shlomo; Sionov, Ronit Vogt; Golan, Itshak; Ish-Shalom, Dvorah; Naor, David

doi:10.3109/15419060009015004

Cited by 24 publications

(12 citation statements)

References 59 publications

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“…PGE 2 has been demonstrated to enhance hyaluronan production by various cell types (34). Glycosylation of cell surface CD44, including the presence of sialic acid residues, seems to decrease hyaluronic acid binding to cells (35). Therefore, if hyaluronan were the sole mediator of the crystal binding effects observed in this study, then one would predict that treatment with PGE 2 , neuraminidase, or tunicamycin might increase crystal binding to cells, whereas the opposite was observed.…”

Section: Discussionmentioning

confidence: 50%

Modulation of Proliferating Renal Epithelial Cell Affinity for Calcium Oxalate Monohydrate Crystals

Farell¹,

Huang

Kim

et al. 2004

Journal of the American Society of Nephrology

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Abstract. Adhesion of urinary crystals to distal tubular cells could be a critical event that triggers a cascade of responses ending in kidney stone formation. Monolayer cultures of distal nephronderived MDCKI cells were used as a model to study crystal-cell interactions. COM crystal adhesion reached a peak 2 d after plating and progressively fell thereafter. The decline in crystal binding was accelerated by prostaglandin E 2 (PGE 2 ) supplementation and delayed by blockade of PG production. Crystals avidly adhered to cells that migrated in to repair a scrape wound made in the monolayer and after a transient hypoglycemic insult. Exposure of MDCKI cells to uric acid crystals and soluble uric acid was also associated with increased crystal adhesion. Treatment of physically or hypoglycemically injured cells with trypsin or neuraminidase reduced crystal binding to baseline levels, suggesting that increased exposure of cell surface glycoproteins mediated the effect, whereas PGE 2 treatment blunted crystal binding to regenerating cells. Furthermore, when cells were grown in the presence of synthetic D-mannosamine analogues that can modify the conformation of cell surface sialoglycoconjugates, crystal binding to proliferating cells was decreased, whereas blockade of N-

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Section: Discussionmentioning

confidence: 50%

Modulation of Proliferating Renal Epithelial Cell Affinity for Calcium Oxalate Monohydrate Crystals

Farell¹,

Huang

Kim

et al. 2004

Journal of the American Society of Nephrology

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“…24,[34][35][36][37][38] Indeed, flow cytometric analysis revealed that the majority of thymocytes and …”

Section: Clonal Expansion and Peripheral Infiltration Of Activated Ptmentioning

confidence: 99%

T-cell lymphomas in T-cell-specific Pten-deficient mice originate in the thymus

Hagenbeek

Spits

2007

Leukemia

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Phosphatase and tensin homolog deleted on chromosome 10 (Pten) is a tumor suppressor protein whose loss of lipid phosphatase activity is associated with lymphomagenesis. We made use of the Cre-loxP system to delete Pten expression in Lck-or CD4-expressing T-lineage cells. Mice initially showed modest thymic hyperplasia and subsequently developed expanding and infiltrating T-cell lymphomas, leading to a premature death within 5 to 23 weeks. Frequently, all thymocyte and peripheral T-cell populations displayed phenotypes characteristic for immature developing thymocyte precursors and shared elevated levels of clonally rearranged T-cell receptor (TCR) b chains. In concert, CD2, CD5, CD3e and CD44, proteins associated with increased expression and signaling capacity of both the immature pre-TCR and the mature abTCR, were more abundantly expressed, reflecting a constitutive state of activation. Although most T-cell lymphomas had acquired the capability to infiltrate the periphery, not all populations left the thymus and expanded clonally exclusively in the thymus. In line with this, only transplantation of thymocytes with infiltrating capacity gave rise to T-cell lymphoma in immunodeficient recipients. These results indicate that T-cell-specific Pten deletion during various stages of thymocyte development gives rise to clonally expanding T-cell lymphomas that frequently infiltrate the periphery, but originate in the thymus.

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“…To determine this, recipients received the tolerogenic regimen along with mAbs to the VLA-4␣ (CD49d) integrin, responsible for homing to vascular and lymphatic endothelium, through binding to its ligands fibronectin, VCAM-1, and mucosal addressin cell adhesion molecule-1 (30,31), or mAbs to CD44, the mucin receptor, responsible for homing to endothelium (32). The results (Fig.…”

Section: Anti-cd62l Mab Prevents Tolerance Induction and Has No Costimentioning

confidence: 99%

L-Selectin-Dependent Lymphoid Occupancy Is Required to Induce Alloantigen-Specific Tolerance

Bai

Liu

Wang

et al. 2002

The Journal of Immunology

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Maneuvers that interfere with signals 1, 2, 3, or Ag processing can result in indefinite allograft survival. However, they are not applicable to all tissues, strains, or species, suggesting that there are additional levels of immune regulation. We hypothesized that secondary lymphoid organs are important for interactions among lymphocytes, alloantigen, and immunosuppressants that lead to tolerance. To explore this, cardiac allografts were performed with a tolerogenic immunosuppressive regimen. Concurrent administration of anti-L-selectin (CD62L) Ab, which prevents lymph node homing, prevents indefinite allograft survival and tolerance. Anti-CD62L Ab is not costimulatory, and Fab and F(ab′)2 anti-CD62L have similar activities. Flow cytometry and histologic examination show that Ab shifts T cells away from lymph nodes and into spleen, peripheral blood, and graft. Tolerance is not induced in CD62L−/− mice, and adoptive transfer of CD62L−/−, but not CD62L+/+, T cells prevents tolerization in wild-type recipients. FTY720, an immunosuppressant that promotes chemokine-dependent, but CD62L-independent, lymph node homing, reverses the Ab effect. Blockade of other homing receptors also prevents tolerization. These results indicate that T lymphocytes use CD62L-dependent migration for alloantigen-specific tolerance, and suggest that lymph nodes or other lymphoid tissues are an important site for peripheral tolerization to alloantigen.

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The CD44 Receptor of Lymphoma Cells: Structure-Function Relationships and Mechanism of Activation

Cited by 24 publications

References 59 publications

Modulation of Proliferating Renal Epithelial Cell Affinity for Calcium Oxalate Monohydrate Crystals

Modulation of Proliferating Renal Epithelial Cell Affinity for Calcium Oxalate Monohydrate Crystals

T-cell lymphomas in T-cell-specific Pten-deficient mice originate in the thymus

L-Selectin-Dependent Lymphoid Occupancy Is Required to Induce Alloantigen-Specific Tolerance

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