Permanent Linkers, Hydrophobic Spacer Molecules
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Permanent Linkers, Hydrophobic Spacer Molecules
This class of linkers is considered non-cleavable, meaning linker cleavage and payload release do not depend on the differential properties between plasma and cytoplasmic compartments. Instead, the release of the cytotoxic drug is postulated to occur after internalization of the ADC via antigen-mediated endocytosis and delivery to lysosomal compartments, where the antibody is degraded to the level of amino acids through intracellular proteolytic degradation. This process releases a drug derivative, formed by the cytotoxic drug, the linker, and the amino acid residue to which the linker was covalently attached. The following section displays examples of hetero-bifunctional PEG-based spacer molecules. As payloads are quite often rather hydrophobic, PEG fragments help to solubilize the linker-payload conjugate, which is essential to perform successful conjugation onto the antibody. It further helps to increase the solubility in physiological media and to improve the pharmacokinetic properties of the whole ADC construct.
10-Undecynoyl-OSu
Alkyne-myristic acid
Alkyne-palmitic acid
Alkyne-stearic acid
11-azido-undecanoyl-OSu
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Ordering informations
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Catalog No. |
Product Name |
Size |
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RL-3460 |
10-Undecynoyl-OSu |
250, 500mg, 1 & 5g |
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RL-2055 |
Alkyne-myristic acid |
100, 500mg & 1g |
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RL-2060 |
Alkyne-palmitic acid |
100, 500mg & 1g |
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RL-2065 |
Alkyne-stearic acid |
500mg & 1g |
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RL-3170 |
11-azido-undecanoyl-OSu |
250, 500mg, 1 & 5g |
▣ 관련 페이지 ; Iris Biotech GMBH
- 이전글Permanent Linkers with Maleimide Function 22.04.21
- 다음글Permanent Linkers, PEG-Based Spacer Molecules 22.04.21
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