Docket #: S01-245A
Anti-Pbx1a monoclonal antibody
Researchers in the laboratory of Dr. Michael Cleary at Stanford University have developed anti-Pbx1a monoclonal antibodies to study transcriptional regulation, embryonic development, and tissue homeostasis. Mammalian Pbx genes encode a family of TALE (three amino acid loop extension) homeodomain proteins that function as transcriptional regulators in numerous cell types.
Pbx1 was originally identified in human pre-B acute lymphoblastic leukemias. Lack of Pbx1 results in embryonic lethality and is associated with multiple patterning malformations, hypoplasia or aplasia of most internal organs, organ malfunctions, and severe fetal anemia. Pbx1 is the prototypic Pbx family member and encodes the alternatively spliced Pbx1a and Pbx1b isoforms that exhibit characteristic biochemical properties. Pbx1a is the high molecular-weight protein form. Pbx1 utilizes the alternative portions of itself to interact with Meis versus Hox proteins. The anti-Pbx1a antibodies could be used in studies of leukemia, embryonic development, and tissue homeostasis.
Applications
- Research related to:
- leukemia
- embryonic development
- tissue homeostasis
Publications
- Jacobs Y, Schnabel CA, Cleary ML., "Trimeric association of Hox and TALE homeodomain proteins mediates Hoxb2 hindbrain enhancer activity." Mol Cell Biol. 1999 Jul;19(7):5134-42.
- Chang CP, Jacobs Y, Nakamura T, Jenkins NA, Copeland NG, Cleary ML., "Meis proteins are major in vivo DNA binding partners for wild-type but not chimeric Pbx proteins." Mol Cell Biol. 1997 Oct;17(10):5679-87.
Web Site
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