Increased serum levels of soluble CD44 standard, but not of variant isoforms v5 and v6, in B cell chronic lymphocytic leukemia

被引:0
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作者
G De Rossi
P Marroni
M Paganuzzi
FR Mauro
C Tenca
D Zarcone
A Velardi
S Molica
CE Grossi
机构
[1] University of Rome,Department of Human Biopathology
[2] National Institute for Cancer Research,Department of Human Anatomy
[3] University of Genova,Department of Clinical Medicine
[4] Pathology and Pharmacology,Division of Hematology
[5] University of Perugia,undefined
[6] Catanzaro Hospital,undefined
来源
Leukemia | 1997年 / 11卷
关键词
B-CLL; adhesion molecules; CD44;
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学科分类号
摘要
The CD44 cell surface proteoglycan participates in a variety of functions including lymphohematopoiesis, lymphocyte homing and tumor metastasis. In addition to the standard form (CD44st), a large family of variant isoforms (CD44v) is generated by alternative splicing of a single gene. Certain CD44v (v5 and V6) are upregulated in the course of neoplastic progression and reflect the metastatic potential of tumor cells. CD44 v6 is expressed in high-grade non-Hodgkin’s lymphoma cells and is released in the serum, thus providing a soluble marker that reflects tumor burden, disease progression and treatment response. Here we show that serum CD44st is elevated in approximately half of B-CLL patients. In contrast, CD44v5 and v6 are detected at normal levels in the large majority of the cases. CD44st serum levels correlate significantly with the number of circulating leukemic B cells and with the levels of another soluble B-CLL marker, β2-microglobulin. Immunoprecipitation analyses of B-CLL sera allow detection of several high molecular weight bands and of a 78 kDa band that represents a soluble form of CD44st and is 4 kDa lower than a similar band (82 kDa) detected in B-CLL cell lysates. Elevated serum CD44st associates with a number of unfavorable prognostic factors such as high peripheral blood lymphocytosis, splenomegaly, advanced disease stage and therapy requirement. A follow-up study indicates that serum levels of CD44st are related to disease status, thus reinforcing our veiw that this molecule may represent a reliable tumor marker in B-CLL.
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页码:134 / 141
页数:7
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