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The antibody against PDF was raised in Rabbit using the recombinant fusion protein containing a sequence corresponding to amino acids 40-243 of human PDF (NP_071736.1) as the immunogen. The polyclonal antibody exists as a isotype IgG, by affinity purification. This antibody has been validated on WB, ELISA.
The antibody against PDF was raised in Rabbit using the recombinant fusion protein containing a sequence corresponding to amino acids 40-243 of human PDF (NP_071736.1) as the immunogen. The polyclonal antibody exists as a isotype IgG, by affinity purification. This antibody has been validated on WB, ELISA.
| Cat.No | ADA-06430A | Clonality | Polyclonal |
|---|---|---|---|
| Host Species | Rabbit | Target Name | |
| Target Synonyms | Form | Liquid | |
| Species Reactivity | Human, Mouse, Rat | Isotype | IgG |
| Storage Buffer | 50% Glycerol, PBS with 0.01% thimerosal, pH7.3. | Purification Method | Affinity purification |
| Positive Samples | Mouse heart, Rat heart, A-549, HepG2, K-562, MCF7, SW620 | Application | ELISA, WB |
| Immunogen Description | Recombinant fusion protein containing a sequence corresponding to amino acids 40-243 of human PDF (NP_071736.1). | Target Species | Human |
|---|---|---|---|
| Uniprot ID | Q9HBH1 | Immunogen Sequence |
Uniprot Id
Q9HBH1
Target Species
Human
Target Name
Target Full Name
Peptide deformylase, mitochondrial
Target Function
Removes the formyl group from the N-terminal Met of newly synthesized proteins.
Target Subcellular Location
Mitochondrion.
Target Protein Families
Polypeptide deformylase family
Target Tissue Specificity
Ubiquitous.
Target Synonyms
PDF; PDF1A; Peptide deformylase; mitochondrial; EC 3.5.1.88; Polypeptide deformylase
Target Background
Protein synthesis proceeds after formylation of methionine by methionyl-tRNA formyl transferase (FMT) and transfer of the charged initiator f-met tRNA to the ribosome. In eubacteria and eukaryotic organelles the product of this gene, peptide deformylase (PDF), removes the formyl group from the initiating methionine of nascent peptides. In eubacteria, deformylation of nascent peptides is required for subsequent cleavage of initiating methionines by methionine aminopeptidase. The discovery that a natural inhibitor of PDF, actinonin, acts as an antimicrobial agent in some bacteria has spurred intensive research into the design of bacterial-specific PDF inhibitors. In human cells, only mitochondrial proteins have N-formylation of initiating methionines. Protein inhibitors of PDF or siRNAs of PDF block the growth of cancer cell lines but have no effect on normal cell growth. In humans, PDF function may therefore be restricted to rapidly growing cells.
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