Am. Knight et al., ANTIGEN ENDOCYTOSIS AND PRESENTATION MEDIATED BY HUMAN MEMBRANE IGG1 IN THE ABSENCE OF THE IG-ALPHA IG-BETA DIMER/, EMBO journal, 16(13), 1997, pp. 3842-3850
Membrane immunoglobulin (mIg) M and D heavy chains possess minimal (KV
K) cytoplasmic tails and associate with the Ig alpha/Ig beta (CD79) di
mer to achieve surface expression and antigen presentation function. I
n contrast, the cytoplasmic tail of mIgG is extended by 25 residues (g
amma ct), We have tested the possibility that mIgG can perform antigen
capture and presentation functions independently of the Ig alpha/beta
dimer. We show that CD4/gamma ct chimeras are efficiently endocytosed
partially dependent on a tyrosine residue in yet. In addition, human
mIgG was expressed on the surface of Ig alpha/Ig beta-negative non-lym
phoid cells and mediated antigen capture and endocytosis. Antigen-spec
ific human mIgG targeted antigen to MIIC-type vesicles in the Ig alpha
/beta negative melanoma Mel JuSo and augmented antigen presentation 10
00-fold, identical to the augmentation seen in Ig alpha/beta-positive
B-cells expressing the same transfected mIgG. Thus, unlike mIgM, mIgG
has autonomous antigen capture and presentation capacity, which may ha
ve evolved to reduce or eliminate the BCR's dependence on additional a
ccessory molecules.