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Merck
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Key Documents

MAIPN4550

Millipore

Plaque à 96 puits Multiscreen®, membrane PVDF hydrophobe

pore size 0.45 μm, non-sterile

Synonyme(s) :

Hydrophobic 96-Well Plate, PVDF 96-Well Plate, PVDF Membrane Plate

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About This Item

Code UNSPSC :
41104923
eCl@ss :
32039006
Nomenclature NACRES :
NB.22

Matériaux

PVDF membrane (hydrophobic)
acrylic
flat bottom wells

Niveau de qualité

Description

Non-sterile, clear 96-well filter plate with 0.45 um pore size Hydrophobic PVDF membrane for Avidin-biotin Linkages, DNA-binding Proteins, Protein Binding & PAMPA. Comes in a pack of 50.

Stérilité

non-sterile

Gamme de produits

MultiScreen®

Caractéristiques

hydrophobic
lid

Fabricant/nom de marque

MultiScreen®

Paramètres

50-250 μL sample volume (per well)

Technique(s)

parallel artificial membrane permeation assay (PAMPA): suitable

Surface de filtration

0.3 cm2

Taille de la plaque/du plateau

96 wells

Volume maximum des puits

300 μL

Volume de travail

50-250 μL

Matrice

Immobilon®-P

Dimension de pores

0.45 μm pore size

Type de liaison

high binding surface

Conditions d'expédition

ambient

Application

La plaque de filtration MultiScreen®-IP, 0,45 µm, transparente, non stérile a été utilisée :
  • Comme support de membrane artificielle et plaque de récupération dans les tests parallèles de perméation de membrane artificielle (PAMPA) pour déterminer la perméabilité des oximes
  • Dans le test ELISpot (Enzyme-Linked Immunospot)
  • Dans le test ELISPOT spécifique à l'hémocyanine de patelle (KLH) pour l'identification des cellules spécifiques de l'antigène (Ag)

Informations légales

Immobilon is a registered trademark of Merck KGaA, Darmstadt, Germany
MULTISCREEN is a registered trademark of Merck KGaA, Darmstadt, Germany

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Certificats d'analyse (COA)

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Retrouvez la documentation relative aux produits que vous avez récemment achetés dans la Bibliothèque de documents.

Consulter la Bibliothèque de documents

Claudia Giesecke et al.
Journal of immunology (Baltimore, Md. : 1950), 200(12), 3981-3992 (2018-05-08)
There are currently limited insights into the progression of human primary humoral immunity despite numerous studies in experimental models. In this study, we analyzed a primary and related secondary parenteral keyhole limpet hemocyanin (KLH) immunization in five human adults. The
A C Belkina et al.
Journal of dental research, 99(7), 855-862 (2020-03-19)
Periodontitis (PD) is a common source of uncontrolled inflammation in obesity-associated type 2 diabetes (T2D). PD apparently fuels the inflammation of T2D and associates with poor glycemic control and increased T2D morbidity. New therapeutics are critically needed to counter the
Hee Chun Jeong et al.
Bioorganic & medicinal chemistry, 17(17), 6213-6217 (2009-08-12)
A series of fluorinated oxime compounds was designed and synthesized in order to probe the effect of fluorine substitution on reactivation of inhibited acetylcholinesterase (AChE) by organophosphorus agents. Permeability measurements, using the Parallel Artificial Membrane Permeation Assays (PAMPA) method, were

Articles

This is a white paper on the Evaluation of the reproducibility of Parallel Artificial Membrane Permeation Assays (PAMPA) using MultiScreen® Filter Plates.

This is a protocol for a Membrane Integrity test for Lipid-PAMPA Artificial Membranes

Combining solubility & PAMPA assays streamlines drug permeability testing.

Combining solubility & PAMPA assays streamlines drug permeability testing.

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Protocoles

Assays that predict passive absorption of orally administered drugs have become increasingly important in the drug discovery process. As previously described by Faller and Kansy such assays provide rapid, low cost and automation friendly methods to measure a compound’s passive permeability.

Assays that predict passive absorption of orally administered drugs have become increasingly important in the drug discovery process. As previously described by Faller and Kansy such assays provide rapid, low cost and automation friendly methods to measure a compound’s passive permeability.

Assays that predict passive absorption of orally administered drugs have become increasingly important in the drug discovery process. As previously described by Faller and Kansy such assays provide rapid, low cost and automation friendly methods to measure a compound’s passive permeability.

Assays that predict passive absorption of orally administered drugs have become increasingly important in the drug discovery process. As previously described by Faller and Kansy such assays provide rapid, low cost and automation friendly methods to measure a compound’s passive permeability.

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