Mouse Anti-ARL8B Recombinant Antibody (CBYC-A781) (CBMAB-A3609-YC)

Mouse

Human, Mouse, Rat

CBYC-A781

IgG2b, κ

WB, IP, IF, ELISA

Amino acids 121-186 mapping at the C-terminus of ARL8B of human origin.

Human, Mouse, Rat

IgG2b, κ

Monoclonal

The COA includes recommended starting dilutions, optimal dilutions should be determined by the end user.

Application	Note
WB	1:100-1:1,000
IP	1-2 µg per 100-500 µg of total protein (1 ml of cell lysate)
IF(ICC)	1:50-1:500
ELISA	1:100-1:1,000

Liquid

PBS, 0.1% gelatin

< 0.1% sodium azide

0.2 mg/ml

Store at 4°C short term (1-2 weeks). Aliquot and store at -20°C long term. Avoid repeated freeze/thaw cycles.

ARL8B may play a role in lysosome motility and play a role in chromosome segregation.

ADP Ribosylation Factor Like GTPase 8B; Novel Small G Protein Indispensable For Equal Chromosome Segregation 1; ADP-Ribosylation Factor-Like Protein 10C; ADP-Ribosylation Factor-Like 10C; ADP-Ribosylation Factor-Like 8B; ARL10C; Gie1; ADP-Ribosylation Fac

Small GTPase which cycles between active GTP-bound and inactive GDP-bound states (PubMed:15331635, PubMed:16537643).
In its active state, binds to a variety of effector proteins playing a key role in the regulation of lysosomal positioning which is important for nutrient sensing, natural killer cell-mediated cytotoxicity and antigen presentation. Along with its effectors, orchestrates lysosomal transport and fusion (PubMed:16650381, PubMed:16537643, PubMed:28325809, PubMed:25898167).
Localizes specifically to lysosomal membranes and mediates anterograde lysosomal motility by recruiting PLEKHM2, which in turn recruits the motor protein kinesin-1 on lysosomes. Required for lysosomal and cytolytic granule exocytosis (PubMed:22172677, PubMed:29592961, PubMed:24088571).
Critical factor involved in NK cell-mediated cytotoxicity. Drives the polarization of cytolytic granules and microtubule-organizing centers (MTOCs) toward the immune synapse between effector NK lymphocytes and target cells (PubMed:24088571).
In neurons, mediates the anterograde axonal long-range transport of presynaptic lysosome-related vesicles required for presynaptic biogenesis and synaptic function (By similarity).
Also acts as a regulator of endosome to lysosome trafficking pathways of special significance for host defense (PubMed:21802320).
Regulates cargo trafficking to lysosomes by binding to PLEKHM1 and recruiting the HOPS subunit VPS41, resulting in functional assembly of the HOPS complex on lysosomal membranes (PubMed:16537643, PubMed:25908847).
Plays an important role in cargo delivery to lysosomes for antigen presentation and microbial killing. Directs the intersection of CD1d with lipid antigens in lysosomes, and plays a role in intersecting phagosomes with lysosomes to generate phagolysosomes that kill microbes (PubMed:25908847, PubMed:21802320).
Involved in the process of MHC II presentation. Regulates the delivery of antigens to lysosomes and the formation of MHC II-peptide complexes through the recruitment of the HOPS complex to lysosomes allowing the fusion of late endosomes to lysosomes (By similarity).
May play a role in chromosome segregation (PubMed:15331635).
(Microbial infection) During Mycobacterium tuberculosis (Mtb) infection, is required for plasma membrane repair by controlling the exocytosis of lysosomes in macrophages. ARL8B secretion pathway is crucial to control the type of cell death of the M. tuberculosis-infected macrophages, distinguishing avirulent from virulent Mtb induced necrotic cell death.
(Microbial infection) During infection, coronaviruses such as SARS-CoV-2 and the chaperone HSPA5/GRP78 are probably co-released through ARL8B-dependent lysosomal exocytic pathway for unconventional egress.

Anterograde axonal transport Source: Ensembl
Antigen processing and presentation following phagocytosis Source: UniProtKB
Antigen processing and presentation of polysaccharide antigen via MHC class II Source: UniProtKB
Autophagosome-lysosome fusion Source: UniProtKB
Calcium ion regulated lysosome exocytosis Source: UniProtKB
Cell cycle Source: UniProtKB-KW
Cell division Source: UniProtKB-KW
Chromosome segregation Source: UniProtKB
Endosomal transport Source: Ensembl
Endosome to lysosome transport of low-density lipoprotein particle Source: UniProtKB
Late endosome to lysosome transport Source: UniProtKB
Lysosome localization Source: UniProtKB
Natural killer cell mediated cytotoxicity Source: UniProtKB
Phagosome-lysosome fusion Source: UniProtKB
Plasma membrane repair Source: UniProtKB
Protein transport Source: UniProtKB-KW
Viral exocytosis Source: UniProtKB

Late endosome membrane; Lysosome membrane; Cytolytic granule membrane; Spindle; Axon; Synapse. GTP-bound form resides on lysosomal membranes, whereas GDP-bound form is likely associated with microtubular structures (PubMed:16650381). Localizes with microtubules at the spindle mid-zone during mitosis. In dendritic cells, localizes to MHC II+ compartments (By similarity).