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Creative Biolabs

NeuroMab™ Anti-TfR BBB Shuttle Antibody(NRZP-1022-ZP2560)

[CAT#: NRZP-1022-ZP2560]

Host Species:
Humanized
Species Reactivity:
Human; Cynomolgus Monkey
Applications:
ELISA; FC; ADCC; In Vitro; In Vivo

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Product Overview

Description

Brain uptake of therapeutic antibodies is severely limited by their size. To achieve enhanced BBB crossing, Creative Biolabs developed a BBB shuttle antibody platform by utilizing the endogenous macromolecule transportation pathway, known as receptor-mediated transcytosis (RMT). The engineered antibody-based carrier is believed to significantly to increase the macromolecule brain entry to combat CNS diseases.
Notes: The BBB antibody is made-to order and available in a customized format. Please don't hesitate contact us for more details.

Species Reactivity

Human; Cynomolgus Monkey

Clonality

Monoclonal

Host Species

Humanized

Applications

ELISA; FC; ADCC; In Vitro; In Vivo

Relevant Diseases

Tumor
Product Properties

Storage

Store at -20°C. Do not aliquot the antibody.

Research Use Only

For research use only
Target

Target

TransferrinReceptor

Official Name

TfR

Full Name

Transferrin Receptor

Alternative Names

CD71; TFR1
Product Pictures
FCM

Fig.1 depict FACS analysis of mouse hybridoma parental clone supernatants binding to human and cynomolgus TfR transiently expressed in 293 cells in the presence of 1 μM human holo-Tf.

The results shown are a titration of 5 concentrations.
1: monomer, free N-terminus, 4.2 mg/mL, never thawed;
2: monomer, His-tagged N-terminus, 4.8 mg/mL;
3: dimer, free N-terminus, 1.6 mg/mL.

ELISA

Fig.2 depicts the binding of hu7A4.v15, hu15G11.v5 and hu7G7.v1 to huTfR in the presence of 6.3 μM holo-Tf.

Antibody binding to immobilized huTfR is shown in the presence (open symbols and dashed lines) or absence (filled symbols and solid lines) of 6.3 μM holo-Tf.

Block

Fig.3 depict the results of the HFE-HuTfR binding and the HFE blocking assays.

The binding of antibody to increasing concentrations of huTfR captured via immobilized HFE. FIG. 6B shows the binding of huTfR to immobilized HFE in the presence of increasing concentrations of antibody.

Block

Fig.4 depict the results of the HFE-HuTfR binding and the HFE blocking assays.

The binding of huTfR to immobilized HFE in the presence of increasing concentrations of antibody.

Cyt

Fig.5 depict the results of experiments assessing the impact of effector function status on ADCC activity of anti-human TfR (“anti-hTFR”) antibodies in primary human bone marrow mononuclear cells or in a human erythroblast cell line.

The binding of huTfR to immobilized HFE in the presence of increasing concentrations of antibody.

FuncS

Fig.6 depict the brain antibody concentrations of the experiments.

The figure shows individual anti-TfR1/BACE1, anti-TfR2/BACE1, anti-gD, and anti-BACE1 concentrations of antibody in various brain regions at 24 hours post-dose.

FuncS

Fig.7 The pharmacodynamic results of the experiments in cynomolgus monkeys.

sAPPβ/sAPPα ratio over time.

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