keyword
https://read.qxmd.com/read/24223164/the-fbi1-akirin2-target-gene-bcam-acts-as-a-suppressive-oncogene
#41
JOURNAL ARTICLE
Hirotada Akiyama, Yoshimasa Iwahana, Mikiya Suda, Atsunori Yoshimura, Hiroyuki Kogai, Ai Nagashima, Hiroko Ohtsuka, Yuko Komiya, Fumio Tashiro
Basal cell adhesion molecule (BCAM), known to be a splicing variant of Lutheran glycoprotein (LU), is an immunoglobulin superfamily membrane protein that acts as a laminin α5 receptor. The high affinity of BCAM/LU for laminin α5 is thought to contribute to the pathogenesis of sickle red blood cells and to various developmental processes. However, the function of BCAM in carcinogenesis is poorly understood. Based on microarray expression analysis, we found that BCAM was one of the target genes of the oncogenic 14-3-3β-FBI1/Akirin2 complex, which acts as a transcriptional repressor and suppresses MAPK phosphatase-1 gene expression...
2013: PloS One
https://read.qxmd.com/read/24036115/the-lutheran-basal-cell-adhesion-molecule-promotes-tumor-cell-migration-by-modulating-integrin-mediated-cell-attachment-to-laminin-511-protein
#42
JOURNAL ARTICLE
Yamato Kikkawa, Takaho Ogawa, Ryo Sudo, Yuji Yamada, Fumihiko Katagiri, Kentaro Hozumi, Motoyoshi Nomizu, Jeffrey H Miner
Cell-matrix interactions are critical for tumor cell migration. Lutheran (Lu), also known as basal cell adhesion molecule (B-CAM), competes with integrins for binding to laminin α5, a subunit of LM-511, a major component of basement membranes. Here we show that the preferential binding of Lu/B-CAM to laminin α5 promotes tumor cell migration. The attachment of Lu/B-CAM transfectants to LM-511 was slightly weaker than that of control cells, and this was because Lu/B-CAM disturbed integrin binding to laminin α5...
October 25, 2013: Journal of Biological Chemistry
https://read.qxmd.com/read/23563364/non-abo-blood-group-systems-phenotyping-in-non-human-primates-for-blood-banking-laboratory-and-xenotransplantation
#43
JOURNAL ARTICLE
G Ramis, L Martínez-Alarcon, J J Quereda, A Mrowiec, C Funes, A Ríos, P Ramírez, A Muñoz, M J Majado
Some biomedical research procedures, such as organ xenotransplantation, usually require intensive hemotherapy. Knowledge of the whole phenotype of blood donor and graft could be useful in the field of xenotransplantation. Human and simian-type categories of blood groups have been established and they can be tested by standard methods used for human blood grouping. The aim of this work was to study the incidence of non-ABO blood group systems in different species of non-human primates, which are employed in biomedical research...
April 2013: Laboratory Animals
https://read.qxmd.com/read/23421542/the-molecular-basis-of-the-lu-7-and-lu-7-phenotypes
#44
JOURNAL ARTICLE
K Hue-Roye, M E Reid
The Lutheran blood group system currently consists of 20 antigens that have been assigned ISBT numbers. Of these, all but LU7 have been associated with one or more nucleotide changes in LU. The purpose of this study was to determine the molecular basis associated with the LU:-7 phenotype. We obtained a stored sample from one proband with this phenotype and sequenced LU. Using genomic DNA, exons 1 through 15, and their flanking intronic regions, of LU were amplified by polymerase-chain reaction, and the products were sequenced...
2012: Immunohematology
https://read.qxmd.com/read/23168236/darc-duffy-and-bcam-lutheran-reduced-expression-in-thyroid-cancer
#45
JOURNAL ARTICLE
Flavia Roche Moreira Latini, André Uchimura Bastos, Carine Prisco Arnoni, Janaína Guilhem Muniz, Rosangela Medeiros Person, Wilson Baleotti, José Augusto Barreto, Lilian Castilho, Janete Maria Cerutti
Duffy or DARC (Duffy Antigen Receptor for Chemokines) is a glycosylated membrane protein that selectively binds angiogenic chemokines. Previous in vivo and in vitro studies of DARC function in cancer have associated DARC over expression with better prognosis, decreased metastatic potential, and inhibition of tumor-associated neovascularization. Another carcinogenesis-associated antigen is Lutheran or BCAM (basal cell adhesion molecule), a surface glycoprotein that acts as a receptor for the extracellular matrix protein, laminin...
March 2013: Blood Cells, Molecules & Diseases
https://read.qxmd.com/read/23160466/jak2v617f-activates-lu-bcam-mediated-red-cell-adhesion-in-polycythemia-vera-through-an-epor-independent-rap1-akt-pathway
#46
JOURNAL ARTICLE
Maria De Grandis, Marie Cambot, Marie-Paule Wautier, Bruno Cassinat, Christine Chomienne, Yves Colin, Jean-Luc Wautier, Caroline Le Van Kim, Wassim El Nemer
Polycythemia vera (PV) is characterized by an increased RBC mass, spontaneous erythroid colony formation, and the JAK2V617F mutation. PV is associated with a high risk of mesenteric and cerebral thrombosis. PV RBC adhesion to endothelial laminin is increased and mediated by phosphorylated erythroid Lu/BCAM. In the present work, we investigated the mechanism responsible for Lu/BCAM phosphorylation in the presence of JAK2V617F using HEL and BaF3 cell lines as well as RBCs from patients with PV. High levels of Rap1-GTP were found in HEL and BaF3 cells expressing JAK2V617F compared with BaF3 cells with wild-type JAK2...
January 24, 2013: Blood
https://read.qxmd.com/read/23125034/molecular-analysis-of-the-rare-in-lu-blood-type-toward-decoding-the-phenotypic-outcome-of-haploinsufficiency-for-the-transcription-factor-klf1
#47
JOURNAL ARTICLE
Virginie Helias, Carole Saison, Thierry Peyrard, Eliane Vera, Claude Prehu, Jean-Pierre Cartron, Lionel Arnaud
KLF1 encodes an erythroid transcription factor, whose essential function in erythropoiesis has been demonstrated by extensive studies in mouse models. The first reported mutations in human KLF1 were found in individuals with a rare and asymptomatic blood type called In(Lu). Here, we show that KLF1 haploinsufficiency is responsible for the In(Lu) blood type, after redefining this peculiar blood type using flow cytometry to quantify the levels of BCAM and CD44 on red blood cells. We found 10 (seven novel) heterozygous KLF1 mutations responsible for the In(Lu) blood type...
January 2013: Human Mutation
https://read.qxmd.com/read/23001842/a-new-method-for-quantitative-analysis-of-cell-surface-glycoproteome
#48
JOURNAL ARTICLE
Zhen Sun, Rui Chen, Kai Cheng, Hongwei Liu, Hongqiang Qin, Mingliang Ye, Hanfa Zou
As the altered glycosylation expressions of cell surface proteins are associated with many diseases, glycoproteomics approach has been widely applied to characterization of surface glycosylation alteration. In general, the abundances of proteolytic glycopeptides derived from corresponding glycoproteins can be measured to determine the abundances of glycoproteins. However, this quantification strategy cannot distinguish whether the changes are results from changes of protein abundance or changes in glycosite occupancy...
November 2012: Proteomics
https://read.qxmd.com/read/22954727/blood-group-phenotypes-resulting-from-mutations-in-erythroid-transcription-factors
#49
REVIEW
Belinda K Singleton, Jan Frayne, David J Anstee
PURPOSE OF REVIEW: This review describes the genetics of unusual blood group phenotypes, particularly those with altered expression of Lutheran antigens, and how this area of study has informed our understanding of erythropoiesis in general and haemoglobin switching in particular. RECENT FINDINGS: Mutations in erythroid transcription factors GATA1 (GATA1 binding protein 1) and KLF1 (Kruppel-like factor 1) cause benign and disease phenotypes in humans [X-linked Lu(a-b-) phenotype, In(Lu) blood group phenotype, hereditary persistence of foetal haemoglobin, borderline HbA(2), and congenital dyserythropoietic anaemia (CDA)]...
November 2012: Current Opinion in Hematology
https://read.qxmd.com/read/22739195/-rare-blood-group-screening-by-serological-and-molecular-methods-in-zhejiang-han-population
#50
JOURNAL ARTICLE
Hong Zhu, Ying Liu, Xiao-Zhen Hong, Xiao-Guo Xu, Xiao-Fei Lan, Kai-Rong Ma, Ji He, Fa-Ming Zhu, Hang-Jun Lu
This study was aimed to investigate the distribution of rare blood group in Zhejiang Han population. The H(-) (H system), GPA(-) and s(-) (MNS), Rhnull, Rhmod, D--, CCDEE, CCdEE (variations of Rh), GPC(-) (Gerbich), i(+) (I), Lu(b-) (Lutheran), Js(b-) and k(-) (Kell), Fy(a-) (Duffy), Ok(a-) (Ok), Di(b-) (Diego) phenotypes were screened by serological or molecular methods. Jk (a-b-) phenotype was detected by urea hemolytic test. The results showed that one Di (a+b-) individual was found in 1618 blood donors, three Fy (a-b+) individuals in 1007 donors and one CCdEE individual in 633 Rh negative donors...
June 2012: Zhongguo Shi Yan Xue Ye Xue za Zhi
https://read.qxmd.com/read/22404936/epinephrine-modulates-bcam-lu-and-icam-4-expression-on-the-sickle-cell-trait-red-blood-cell-membrane
#51
JOURNAL ARTICLE
Jamie L Maciaszek, Biree Andemariam, Greg Huber, George Lykotrafitis
Collapse and sudden death in physical training are the most serious complications of sickle cell trait (SCT). There is evidence that erythrocytes in SCT patients aggregate during strenuous exercise, likely because of adhesive interactions with the extracellular matrix (ECM) and endothelial cells, and because of their irregular viscoelastic properties. This results in inflammation, blood flow impairment, and vaso-occlusive events. However, the exact role of stress conditions and how they lead to these complications is virtually unknown...
March 7, 2012: Biophysical Journal
https://read.qxmd.com/read/21858073/an-antibody-to-the-lutheran-glycoprotein-lu-recognizing-the-lu4-blood-type-variant-inhibits-cell-adhesion-to-laminin-%C3%AE-5
#52
JOURNAL ARTICLE
Yamato Kikkawa, Takahiro Miwa, Yukiko Tohara, Takayuki Hamakubo, Motoyoshi Nomizu
BACKGROUND: The Lutheran blood group glycoprotein (Lu), an Ig superfamily (IgSF) transmembrane receptor, is also known as basal cell adhesion molecule (B-CAM). Lu/B-CAM is a specific receptor for laminin α5, a major component of basement membranes in various tissues. Previous reports have shown that Lu/B-CAM binding to laminin α5 contributes to sickle cell vaso-occlusion. However, as there are no useful tools such as function-blocking antibodies or drugs, it is unclear how epithelial and sickled red blood cells adhere to laminin α5 via Lu/B-CAM...
2011: PloS One
https://read.qxmd.com/read/21840761/blood-group-antigens-frequencies-in-the-northeast-of-iran
#53
JOURNAL ARTICLE
Mohammad Reza Keramati, Hossein Shakibaei, Mohammad Ismail Kheiyyami, Hossein Ayatollahi, Zahra Badiei, Maliheh Samavati, Mohammad Hadi Sadeghian
BACKGROUND: Identification of blood group antigen frequencies in a population has various benefits in transfusion medicine. Most data in the literature include frequencies of these antigens in European and American countries. In this study for the first time we have reported frequencies of these antigens in the northeast of Iran. MATERIALS AND METHODS: Blood group antigens were characterized in the 522 blood donors in Mashhad, Iran. The following antigens including ABO, Rh (D, C, E, c, e), MNSs (M, N, S, s), Lutheran (Lu(a), Lu(b)), P (P, P(1)), Kell (K, k, Kp(a), Kp(b)), Lewis (Le(a), Le(b)), Duffy (Fy(a), Fy(b)) and Kidd (Jk(a), Jk(b)) were typed and phenotypes frequencies were expressed as a percentage...
October 2011: Transfusion and Apheresis Science
https://read.qxmd.com/read/21434869/novel-role-for-the-lu-bcam-spectrin-interaction-in-actin-cytoskeleton-reorganization
#54
JOURNAL ARTICLE
Emmanuel Collec, Marie-Christine Lecomte, Wassim El Nemer, Yves Colin, Caroline Le Van Kim
Lu/BCAM (Lutheran/basal cell-adhesion molecule) is a laminin 511/521 receptor expressed in erythroid and endothelial cells, and in epithelial tissues. The RK573-574 (Arg573-Lys574) motif of the Lu/BCAM cytoplasmic domain interacts with αI-spectrin, the main component of the membrane skeleton in red blood cells. In the present paper we report that Lu/BCAM binds to the non-erythroid αII-spectrin via the RK573-574 motif. Alanine substitution of this motif abolished the Lu/BCAM-spectrin interaction, enhanced the half-life of Lu/BCAM at the MDCK (Madin-Darby canine kidney) cell surface, and increased Lu/BCAM-mediated cell adhesion and spreading on laminin 511/521...
June 15, 2011: Biochemical Journal
https://read.qxmd.com/read/21175664/the-functional-importance-of-blood-group-active-molecules-in-human-red-blood-cells
#55
REVIEW
D J Anstee
Antigens of 23 of the 30 human blood group systems are defined by the amino acid sequence of red cell membrane proteins. The antigens of DI, RH, RHAG, MNS, GE and CO systems are carried on blood group-active proteins (Band 3, D and CE polypeptides, RhAG, Glycophorins A and B, Glycophorins C and D and Aquaporin 1, respectively) which are expressed at high levels (>200,000 copies/red cell). These major proteins contribute to essential red cell functions either directly as membrane transporters and by providing linkage to the underlying red cell skeleton or by facilitating the membrane assembly of the protein complexes involved in these processes...
January 2011: Vox Sanguinis
https://read.qxmd.com/read/21175663/structural-modelling-of-red-cell-surface-proteins
#56
REVIEW
N M Burton, G Daniels
The red cell surface membranes contain a large variety of proteins, many of which express blood group activity as a result of variation in their oligosaccharide or amino acid sequences. To understand the nature of the blood group epitopes, the functions of the proteins that express them and their relationship to each other, computer modelling has been employed to provide predictions of their structures. Modelling is an excellent method of first resort when experimental structural data for the protein of interest are absent or incomplete...
January 2011: Vox Sanguinis
https://read.qxmd.com/read/21086783/evaluation-of-a-new-monoclonal-anti-k-anti-kel2-reagent
#57
JOURNAL ARTICLE
Erwin Strobel
BACKGROUND: The first monoclonal anti-k (anti-KEL2) reagent of the IgM-class (clone: LK1) for the tube spin method is now commercially available. As this reagent is directly agglutinating in contrast to conventional polyclonal anti-k reagents requiring an indirect antiglobulin test, we studied the reaction characteristics of this new reagent carefully before starting its use in our routine blood grouping laboratory. METHODS: The titer of the monoclonal anti-k reagent (manufacturer: Biotest, D-63303 Dreieich) was compared with that of two polyclonal anti-k reagents...
2010: Clinical Laboratory
https://read.qxmd.com/read/20942180/-lutheran-blood-group-system
#58
JOURNAL ARTICLE
Teruo Endoh, Naoki Watanabe
No abstract text is available yet for this article.
June 2010: Nihon Rinsho. Japanese Journal of Clinical Medicine
https://read.qxmd.com/read/20655789/role-of-lu-bcam-glycoproteins-in-red-cell-diseases
#59
JOURNAL ARTICLE
W El Nemer, Y Colin, C Le Van Kim
Lu/BCAM glycoproteins (gps) are the unique erythroid receptors of laminin alpha5 chain, a major component of the extracellular matrix. They interact with the membrane skeleton by binding directly to spectrin via the Lu/BCAM RK573-574 motif. Lu/BCAM gps are involved in abnormal sickle red blood cell (RBC) adhesion to components of the vascular wall. This adhesion is activated by the phosphorylation of the Lu/BCAM long isoform Lu in a protein kinase A-dependent manner. A similar high adhesion to laminin was also observed with RBCs from Hereditary Spherocytosis (HS) patients suffering from haemolytic anaemia subsequent to spectrin deficiencies...
September 2010: Transfusion Clinique et Biologique: Journal de la Société Française de Transfusion Sanguine
https://read.qxmd.com/read/20566895/decreased-sickle-red-blood-cell-adhesion-to-laminin-by-hydroxyurea-is-associated-with-inhibition-of-lu-bcam-protein-phosphorylation
#60
JOURNAL ARTICLE
Pablo Bartolucci, Vicky Chaar, Julien Picot, Dora Bachir, Anoosha Habibi, Christine Fauroux, Frédéric Galactéros, Yves Colin, Caroline Le Van Kim, Wassim El Nemer
Sickle cell disease is characterized by painful vaso-occlusive crises during which abnormal interactions between erythroid adhesion molecules and vessel-wall proteins are thought to play a critical role. Hydroxyurea, the only drug with proven benefit in sickle cell disease, diminishes these interactions, but its mechanism of action is not fully understood. We report that, under hydroxyurea, expression of the unique erythroid laminin receptor Lu/BCAM was increased, but red blood cell adhesion to laminin decreased...
September 23, 2010: Blood
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