Use your antibodies-online credentials, if available.
Keine Produkte auf Ihrer Vergleichsliste.
Ihr Warenkorb ist leer.
Alle Spezies anzeigen
Weitere Synonyme anzeigen
Wählen Sie die Spezies und Applikation aus
anti-Human MBL2 Antikörper:
anti-Rat (Rattus) MBL2 Antikörper:
anti-Mouse (Murine) MBL2 Antikörper:
Sie gelangen zu unserer vorgefilterten Suche.
Human Monoclonal MBL2 Primary Antibody für IHC (fro), IHC (p) - ABIN2192483
Ramos, Nisihara, Maestri, Bicalho, Carvalho, de Messias Reason: MBL serum concentration in women with HPV presenting CIN III lesions. in Human immunology 2012
Show all 5 Pubmed References
Human Monoclonal MBL2 Primary Antibody für ELISA, WB - ABIN2192485
Fiane, Videm, Lingaas, Heggelund, Nielsen, Geiran, Fung, Mollnes: Mechanism of complement activation and its role in the inflammatory response after thoracoabdominal aortic aneurysm repair. in Circulation 2003
Show all 3 Pubmed References
Human Monoclonal MBL2 Primary Antibody für IP, ELISA - ABIN2192488
Skjoedt, Hummelshoj, Palarasah, Honore, Koch, Skjodt, Garred: A novel mannose-binding lectin/ficolin-associated protein is highly expressed in heart and skeletal muscle tissues and inhibits complement activation. in The Journal of biological chemistry 2010
Show all 3 Pubmed References
Human Monoclonal MBL2 Primary Antibody für ELISA, WB - ABIN2192486
Hein, Honoré, Skjoedt, Munthe-Fog, Hummelshøj, Garred: Functional analysis of Ficolin-3 mediated complement activation. in PLoS ONE 2010
MBL deficiency was significantly more frequent in the juvenile idiopathic arthritis Yersinia-reactive antibodies-positive group than in patients without Yersinia-reactive antibodies or in controls
it can be concluded that molecular analysis of MBL rs1800450 AA genotype and TNF-alpha (zeige TNF Antikörper) rs1800620 AA genotype is important in the early detection and treatment of T2DM with H. pylori cagA (zeige S100A8 Antikörper)(+) infection.
The results suggest that MBL deficiency and the presence of MBL2 gene polymorphisms that lead to MBL deficiency are risk factors for the occurrence of miscarriage in patients with RA.
These results suggest that the MBL2 gene Codon 54 and TNF-alpha (zeige TNF Antikörper) gene G308A polymorphisms are not associated with an increased risk for development of tuberculosis in our patients.
Studies results provide evidence that Crohn's disease patients have an impairment in mannose-binding lectin-mannose-associated serine protease (zeige F2 Antikörper) functional activity and that this defect is associated with mannose-binding lectin 2 and NOD2 (zeige NOD2 Antikörper) variants.
Our data do not support a possible role for MBL2 polymorphisms in the pathogenesis and in the clinical manifestations of rheumatic fever.
The reduced expression of functional MBL secondary to having MBL2 variants may partially mediate the increased susceptibility to TB risk.
MBL2 rs1800450 and rs1800451 polymorphisms play a protective role in TB infection and reinforce their critical significance as a potential genetic marker for TB resistance.
MBL2 exon 1 polymorphic variants were found only in codon 54, and the allele frequencies did not differ significantly between the control and disease groups
These results indicated that polymorphisms in MBL2 gene may influence susceptibility, progression and prognosis of HBV-related liver diseases.
MBL2 polymorphisms were associated with some disease groups and with the presence of some etiologic agents
MBL1 (zeige Mbl1 Antikörper) was also found to be expressed in the lung, testis and brain, whereas low expression of MBL2 was detected in the testis and kidney.
Single nucleotide polymorphisms in MBL2 at exon 1 were detected using polymerase chain reaction single-strand conformation polymorphism analysis and DNA sequencing techniques in 825 Chinese Holstein cows.
the relationship between the variants of the bovine MBL2 gene and milk production traits, mastitis, serum MBL-C levels and hemolytic complement activity in both classical pathway (CH50) and alternative pathway (ACH50) in Chinese Holstein cattle
this study shows that MBL-C expression is induced in the gut (zeige GUSB Antikörper) in response to Candida albicans sensing and is required for intestinal homeostasis and host defense against Candida albicans
Targeted deletion of Mbl1 (zeige Mbl1 Antikörper)/2 causes differential levels of inflammation-related gene sets at baseline and after exposure to ozone and significantly reduces pulmonary inflammation, thus indicating an important innate immunomodulatory role of the Mbl1 (zeige Mbl1 Antikörper)/2 genes.
Human and murine data together indicate that SP-A, SP-D and MBL are synthesized in early gestational tissues, and may contribute to regulation of immune response at the feto-maternal interface during pregnancy.
These data show that modulation of MBL is involved in the protection against renal I/RI induced by dietary restriction, and suggest that the mechanisms of protection induced by dietary restriction and fasting may be different.
ALI in H5N1-infected mice was caused by excessive complement activation, as demonstrated by deposition of C3, C5b-9, and MBL-C in lung tissue, and by up-regulation of MBL-associated serine protease-2 (zeige MASP2 Antikörper) and the complement receptors C3aR (zeige C3AR1 Antikörper) and C5aR (zeige C5AR1 Antikörper).
demonstrate that apolipoprotein E (Apoe (zeige APOE Antikörper)), mannose-binding lectin 2 (Mbl2), and parotid secretory protein (Psp (zeige BPIFA2 Antikörper)) are present at significantly different quantities in depleted plasma of diabetic NZO mice compared to non-diabetic controls
Data indicate that no change of mannan-binding lectin MBL-A (zeige Mbl1 Antikörper) during the study, however, mannan-binding lectin MBL-C concentration increased in median by 3.6-fold (2.9; 4.5-fold) during the study in the diabetic group.
These observations point to a previously unappreciated role for MBL in regulating host resistance and cardiac inflammation during infection with a major human pathogen.
MBL plays a key role in clearing influenza A virus and maintaining lung homeostasis.
Data show that genetically defined MBL-deficiency is associated with a better outcome after acute stroke.
MBL binding can be inhibited by at least two separate and independent mechanisms.
report multiple copies of MBL-like genes, with up to three copies tightly linked within a cluster spanning approximately 15 kb on chromosome 2
This gene encodes the soluble mannose-binding lectin or mannose-binding protein found in serum. The protein encoded belongs to the collectin family and is an important element in the innate immune system. The protein recognizes mannose and N-acetylglucosamine on many microorganisms, and is capable of activating the classical complement pathway. Deficiencies of this gene have been associated with susceptibility to autoimmune and infectious diseases.
, mannan-binding lectin
, mannose-binding lectin (protein C) 2, soluble (opsonic defect)
, mannose-binding lectin 2, soluble (opsonic defect)
, mannose-binding protein C
, 27 kDa mannan-binding protein monomeric subunit
, mannose-binding lectin 2, soluble
, Mannose-binding protein C
, c-type lectin
, mannose binding lectin, liver (A)
, mannose-binding lectin 2
, soluble mannose-binding lectin
, mannan-binding protein
, RA-reactive factor P28A subunit
, mannose binding lectin 2 (protein C)
, mannose-binding protein C (liver)
, ra-reactive factor polysaccharide-binding component p28A
, raRF p28A
, mannose binding lectin (C)
, mannose binding lectin, liver (C)
, mannose-binding lectin (protein C) 2, soluble
, Mannan-binding protein
, Mannose-binding lectin
, hexose-binding lectin 3
, mannose binding lectin 2
, mannose binding-like lectin