Tyrosine phosphatase activity of lymphoma CD45 (GP180) is regulated by a direct interaction with the cytoskeleton.

GP180 is one of the major transmembrane glycoproteins in mouse T-lymphoma cells. This molecule is an isoform of CD45 and is known to contain an intrinsic protein tyrosine phosphatase (PTPase) activity. Using several complementary biochemical techniques, we have found that fodrin (a spectrin-like protein) is preferentially co-isolated with CD45 (GP180), suggesting that a complex between CD45 (GP180) and the cytoskeleton exists in mouse T-lymphoma cells. Furthermore, we have determined that this CD45 (GP180)-fodrin complex is dissociated by high salt treatment. Using in vitro binding assays, we have shown that CD45 (GP180) binds directly and specifically to fodrin (Kd approximately 1.1 nM) or spectrin (Kd approximately 3.2 nM) in a saturable manner. Additional analyses indicate that a 48-kDa phosphopeptide of CD45 (GP180) contains the fodrin/spectrin-binding domain. Most importantly, the direct binding of fodrin/spectrin to CD45 (GP180) is found to significantly stimulate the PTPase activity of CD45. Enzyme kinetic analysis indicates that fodrin and spectrin increase the Vmax of CD45 (GP180)-mediated dephosphorylation by 7.5 and 3.2-fold, respectively, without significantly changing the Km value. These results strongly suggest that the cytoskeletal proteins, fodrin and spectrin, play an important role in the regulation of the CD45 (GP180) PTPase activity during lymphocyte activation.     

The involvement of cAMP in lymphocyte capping

We have observed that agents that are known to elevate intracellular levels of cAMP such as N⁶,O²-dibutyryl adenosine 3′,5′-cyclic monophosphoric acid (dbcAMP) and theophylline cause a remarkable stimulatory effect on the lymphocyte receptor mobility phenomenon. Increased intracellular concentration of cAMP enhances not only antibody-induced but also Con A-induced lymphocyte capping events in T-lymphoma cells. In addition, we have noted that N²,O²-dibutyryl guanosine 3′,5′-cyclic monophosphoric acid (dbcGMP) does not stimulate but actually slightly inhibits the receptor movement. Furthermore, we have determined cAMP levels to increase greater than twofold during ligand-induced capping using a radioimmunoassay. Therefore, our data strongly suggest that cyclic adenylic monophosphoric acid (and not cGMP) is specifically involved in the redistribution of lymphocyte membrane proteins induced by both antibody and Con A.     

Rapid separation of mouse T and B lymphocytes using wheat germ agglutinin.

A separation procedure has been developed for mouse splenic T and B lymphocytes which is based on their differential agglutination by wheat germ agglutinin (WGA). In the presence of 50-100 micrograms/ml of WGA, multicellular aggregates are formed which are enriched in B cells. These aggregates can be separated from monodisperse T cells by gravity sedimentation and subsequently dissociated into single cells by treatment with N-acetylglucosamine (NAG). Immunocytochemical analyses and mitogenic assays indicate approximately 10-15% cross contamination of the resultant B and T cell fractions. The separation procedure is not only convenient and rapid but also allows the simultaneous recovery of viable T and B cells from the same spleen preparation.     

Human plasma inter-alpha-trypsin inhibitor is encoded by four genes on three chromosomes

Human inter-alpha-trypsin inhibitor is a plasma protein of Mr 180,000 which has long been described as a single polypeptide chain. However, we have previously demonstrated that it is synthesized in liver by two different mRNA populations coding for heavy or light polypeptide chains [Bourguignon, J. et al. (1983) FEBS Lett. 162, 379-383] and cDNA clones for the heavy or light chains have recently been isolated and characterized [Bourguignon, J. et. al. (1985) Biochem. Biophys. Res. Commun. 131, 1146-1153; Salier, J.P. et al. (1987) Proc. Natl Acad. Sci. USA 84, 8272-8276]. In the present study, we show that human poly(A)-rich RNAs hybrid-selected with various heavy-chain-encoding cDNA clones translate three different heavy chains, designated H1 (Mr 92,000), H2 (Mr 98,000) and H3 (Mr 107,000). We previously characterized two heavy-chain cDNA clones. We now report that they correspond to H1 and H2 chains. We have also determined the sequence of an additional cDNA clone which codes for H3 chain. Its insert size is 1.79 kb with a single open reading frame and a poly(A) tail. The deduced amino acid sequence of the H3 chain is highly similar to those of the H1 (54%) and H2 (44%) chains. Northern analysis of human liver poly(A)-rich RNAs with the three heavy-chain cDNAs as probes clearly identified a single major mRNA population of 3.3 +/- 0.1 kb. Chromosomal localization by in situ hybridization shows that inter-alpha-trypsin inhibitor genes are located on three different human chromosomes. The H1 and H3 genes are located in the p211-p212 region of chromosome 3, whereas the H2 gene resides in the p15 band of chromosome 10. The light-chain gene is located in the q32-q33 region of chromosome 9. These results indicate that heavy and light chains of inter-alpha-trypsin inhibitor are encoded by at least four functional genes.     

Skewed soldier sex ratio in termites: testing the size-threshold hypothesis

Social insect colonies contain multiple phenotypes, i.e. castes, and this caste polyphenism is often linked to sexual dimorphism. Unlike social hymenopterans, both termite sexes are diploid and contribute to helper-type tasks within the colony. Nonetheless, a biased sex ratio is frequently observed in termites, especially in soldiers. To explain this bias in soldier sex ratio, Matsuura (Evol. Ecol. 20: 565–574, 2006) postulated the existence of a size threshold for workers molting into soldiers. Under the influence of sexual size dimorphism (SSD), such a threshold was considered to indirectly favor one sex. We conducted a literature survey of sex ratio among termite soldiers and tested this size-threshold hypothesis using data for 67 termite species from a variety of termite lineages. We demonstrated the existence of a size threshold for individuals molting into soldiers, resulting in the acquisition of soldiers of only one sex in species exhibiting strong SSD. In species exhibiting weak SSD, the size threshold skews the sex ratio of soldiers, but does not necessarily cause the loss of one sex. Finally, we observed a prevalence of single-sex soldiers in the Termitidae, regardless of SSD, suggesting that the ancestral developmental mechanisms that constrain soldier differentiation from one sex are maintained in certain extant species.