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(Received for publication, November 18, 1996, and in revised form, February 17, 1997)
From the Department of Cancer Biology, The Salk Institute for
Biological Studies, San Diego, California 92186-5800
The invariant chain (Ii) targets major
histocompatibility complex class II molecules to an endocytic
processing compartment where they encounter antigenic peptides.
Analysis of Ii-transferrin receptor chimeras expressed in polarized
Madin-Darby canine kidney (MDCK) cells shows that the Ii cytoplasmic
tail contains a dihydrophobic basolateral sorting signal,
Met16-Leu17, which is recognized in both
the biosynthetic and endocytic pathways. Pro15-Met16-Leu17 has previously
been identified as one of two dihydrophobic Ii internalization signals
active in non-polarized cells. Pro15 is also required for
endocytosis in MDCK cells but not for basolateral sorting, indicating
that the internalization signal recognized at the plasma membrane is
distinct from the sorting signal recognized by basolateral sorting
machinery. Another dihydrophobic sequence, Leu7-Ile8, is required for rapid
internalization of the chimeric receptors in MDCK cells but not for
basolateral sorting, providing further evidence that the structural
requirements for basolateral sorting and internalization differ.
Deletion analysis suggests that basolateral sorting of newly
synthesized Ii-TR chimeras is also mediated by the membrane-proximal
region of the Ii cytoplasmic tail. However, this region does not
promote polarized basolateral recycling, indicating that the structural
requirements for polarized sorting in the biosynthetic and endocytic
pathways are not identical.
Volume 272, Number 18,
Issue of May 2, 1997
pp. 11757-11762
©1997 by The American Society for Biochemistry and Molecular Biology, Inc.
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