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Angiopoietins 1-4 (Ang-1,
Ang-2, Ang-3, and Ang-4) Antibodies
Angiopoietin 1 (Ang-1 proteins and Antibodies)
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Items |
Antigen
peptide
location |
Ab
Host |
Neat Antisera
(100 ul) Cat # |
Aff. Pure Ab
(100 ug) Cat # |
* Control Peptide
(100 ug) Cat# |
|
Ang-1 |
M 20 aa ~NT |
Rb, poly |
ANG11-S |
ANG11-A |
ANG11-P |
|
Ang-1 |
H, Ang-1
Protein |
M, mono |
|
ANG13-M |
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Ang-1
|
Purified Human Recombinant
Ang-1 protein for WB (Biologically inactive); Cat # ANG12-C; 100 ul
Purified Human Recombinant Ang-1 protein (Biologically Active); Cat #
ANG15-R-25; 25 ug
|
Angiopoietin 2 (Ang-2 proteins and Antibodies)
|
Items |
Antigen
peptide
location |
Ab
Host |
Neat Antisera
(100 ul)
Cat # |
Aff. Pure Ab
(100 ug)
Cat # |
* Control Peptide
(100 ug)
Cat# |
|
Ang-2
ab # 1 |
M
21 aa ~NT |
Rb, poly |
ANG21-S |
ANG21-A |
ANG21-P |
|
Ang-2
ab # 3
|
H , Ang-2
protein
|
m, mono
|
-
|
ANG23-M
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.
|
|
Ang-2
ab # 4
|
H , Ang-2
protein
|
G, poly
|
-
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ANG24-A
|
.
|
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Ang-2
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Purified Human Recombinant
Ang-2 protein for WB (Biologically inactive), Cat # ANG22-C; 100 ul
Purified Human Recombinant
Ang-2 protein (Biologically Active), Cat # ANG25-R-25; 25 ug
|
|
Ang-2 ELISA kit
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Human Angiopoietin 2 ELISA kit, Cat # 100-180-APH |
Angiopoietin 3-4(Ang-3 and Ang-4 proteins and Antibodies)
|
Items |
Antigen
peptide
location |
Ab
Host |
Neat Antisera
(100 ul) Cat # |
Aff. Pure Ab
(100 ug) Cat # |
* Control Peptide
(100 ug) Cat# |
|
Ang-3 |
M, Ang-3
protein |
R, mono |
|
ANG31-M
|
|
|
Ang-4 |
H, Ang-4
protein |
M, mono |
|
ANG41-M
|
|
|
Ang-3 pure Protein |
Recombinant Purified Mouse Ang-3
protein for WB (Biologically inactive), Cat # ANG31-C; 100 ul
Recombinant Purified Mouse Ang-3 protein (Biologically active), Cat #
ANG35-R-25; 25 ug |
|
Ang-4
pure Protein |
Recombinant Purified Human Ang-4
protein for WB (Biologically inactive), Cat # ANG41-C; 100 ul
Recombinant Purified Human Ang-4 protein (Biologically active), Cat #
ANG45-R-25; 25 ug |
M= Mouse; R=Rat; H=Human; Rb=Rabbit; G=goat; B=Bovine,
MO=Monkey; P=pig; CT= near C-terminus; NT=near N-terminus; Internal=Middle of
protein. EC=extracellular; CP=cytoplasmic domains
*
Related Items TIEs (Tek), VEGF, and VEGF
Receptors 1-3 (FLK-1, Flt-1, and Flt-4) Antibodies
Angiopoietin-1 (Ang-1) and Angiopoietin-2 (Ang-2) General
Information
Embryonic vascular system undergoes
a series of complex, highly regulated series of events involving
differentiation, migration and association of primitive endothelial cells. This
process is termed vasculogenesis. A further remodeling of the primitive vascular
system forms the mature cardiovascular system. This process is known as
angiogenesis (sprouting of new capillary vessels from pre-existing vasculature).
The development of primordia of the heart and large vessels, primary capillary
networks in the embryo and the extraembryonic structures in the yolk sac.
Angiogenesis accounts for the formation of vasculature into previously avascular
organs such as brain and kidney. Angiogenic activity in the adult is required
during the normal tissue repair, and for the remodeling of the female
reproductive organs (ovulation and placental development). Certain pathological
conditions, such as tumor growth and diabetic retinopathy, also require
angiogenesis. The genetic and molecular mechanism that influence angiogenesis
has only recently begun to be studied and identified. Study of tumor
angiogenesis has led to the identification of several proteins including basic
fibroblast growth factor (bFGF) and vascular endothelial growth factor. VEGF
acts by interacting with a family of largely endothelial-specific receptor
tyrosine kinases that includes VEGFR-1 (flt-1), VEGFR-2 (flk-1/KDR), and
VEGFR-3/Flt-4. Disruption of VEGFRs interferes with differentiation of
endothelial cells and it is lethal for the embryo.
Angiopoietin-1 (mouse and human Ang-1; 498 AA; ~ 98% identity) is an angiogenic
secreted protein that interact with endothelial specific Tie-2 receptor. During
embryonic development, Ang-1 binds and induces tyrosine phosphorylation of
Tie-2. Ang-1 deficient mice mimic the phenotype exhibited by animals deficient
in Tie-2. The role of Ang-1 in angiogenesis appears to be different from VEGF. A
homolog of Ang-1, termed Angiopoietin-2 (mouse and human Ang-2, 496 AA; ~85%
identity) has recently been identified. It may act an antagonist for Ang-1 and
Tie-2. Ang-1 and Ang-2 have ~60% sequence homology.
Ang-1 is prominently expressed in the myocardium of atrium and ventricle,
mesenchymal and smooth muscle cells surrounding most blood vessels, and lung.
Ang-2 expression is abundant in the dorsal aorta and major aortic branches.
Ang-2 transcripts in fetal liver were restricted to cells at the lumen of
hepatic vessels. In the adult, Ang-1 was also expressed in the heart and liver.
In contrast, Ang-2 was found in tissues that may undergo vascular remodeling
(ovary, placenta, and uterus). Defects in Tie-2 have been linked to dominantly
negative venous malformation, an error of vascular morphogenesis characterized
by dilated serpiginous channels.
A homology-based cloning approach has led to the identification of
angiopoietin-3 (Angpt3, 509 aa, chromosome 2) in mouse, and angiopoietin-4
(ANGPT4, 504 aa, chromosome 20p13) in human. Although angiopoietin-3 and
angiopoietin-4 are more structurally diverged from each other than are the mouse
and human versions of angiopoietin-1 and angiopoietin-2, they appear to
represent the mouse and human counterparts of the same gene locus, as revealed
in chromosomal localization studies of all the angiopoietins in mouse and human.
Angiopoietin-3 was expressed as multiple mouse tissues , whereas angiopoietin-4
was expressed primarily in human lung. It is also suggested that angiopoietin-3
acts as an antagonist, whereas angiopoietin-4 functions as an agonist.
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