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Diabetes, Vol 48, Issue 2 279-286, Copyright © 1999 by American Diabetes Association
Functional properties of leptin receptor isoforms: internalization and degradation of leptin and ligand-induced receptor downregulation
S Uotani, C Bjorbaek, J Tornoe and JS Flier
Department of Medicine, Beth Israel Deaconess Medical Center, Boston, Massachusetts 02215, USA.
Long (ObRb) and short (ObRa) leptin receptor isoforms are thought to play
essential roles in mediating leptin signaling and the transport and
degradation of leptin, respectively. Although the capacity of these cloned
receptor species to mediate signal transduction has been reported, there is
no information on the ability of individual receptor species to mediate
leptin internalization and degradation or to undergo ligand-induced
downregulation. We therefore studied these parameters in Chinese hamster
ovary (CHO) cells stably expressing either ObRa or ObRb isoforms of the
leptin receptor. We determined that both ObRa and ObRb mediated
internalization of 125I-labeled leptin by a temperature- and coated
pit-dependent mechanism. Both ObRa and ObRb also mediated degradation of
125I-leptin by a lysosomal mechanism, and this was more efficiently
mediated by ObRa in these cells. Neither leptin internalization nor
degradation by ObRa was affected by mutation of the conserved Box 1 motif.
By studying deletion mutants of ObRa, we found that efficient
internalization was dependent on a motif located between amino acids 8 and
29 of the intracellular domain of ObRa. Exposure of cells expressing ObRa
or ObRb to unlabeled leptin for 90 min at 37 degrees C produced
downregulation of available surface receptors, and this effect was of
greater magnitude in cells expressing ObRb. Whereas CHO cells expressing
the growth hormone receptor showed marked downregulation of ligand binding
after exposure to dexamethasone (DEX) or phorbol myristic acid (PMA), PMA
had no effect on expression of ObRa or ObRb, and DEX reduced binding to
cells expressing ObRb by 15%. Thus, the two leptin receptor isoforms, ObRa
and ObRb, mediate leptin internalization by a coated pit-dependent
mechanism, leptin degradation by a lysosomal pathway, and ligand-induced
receptor downregulation. The differential capacity of the two receptor
isoforms may relate to the different roles of the receptor isoforms in the
biology of leptin.

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Copyright © 1999 by the American Diabetes Association.
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