2000
DOI: 10.1034/j.1600-0854.2000.011208.x
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Trafficking and Folding Defects in Hereditary Spherocytosis Mutants of the Human Red Cell Anion Exchanger

Abstract: Hereditary spherocytosis (HS) is a common inherited hemolytic anemia caused by mutations in erythrocyte proteins including the anion exchanger, AE1 (band 3). This study examined seven missense mutations (L707P, R760Q, R760W, R808C, H834P, T837M, and R870W) located in the membrane domain of the human AE1 that are associated with this disease. The HS mutants, constructed in full-length AE1 cDNA, could be transiently expressed to similar levels in HEK 293 cells. Immunofluorescence, cell surface biotinylation, and… Show more

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Cited by 56 publications
(72 citation statements)
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References 66 publications
(104 reference statements)
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“…The NMR structure of a synthetic peptide corresponding to Gly 796 -Ile 841 revealed Ile 803 -Leu 810 in ␣-helical conformation (40). The R808C mutation, found in this region, causes hereditary erythroid spherocytosis because of a failure to process AE1 to the cell surface (36). Consistent with that finding, R808C AE1 was not functional and was not biotinylated in the present study.…”
Section: Discussionsupporting
confidence: 80%
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“…The NMR structure of a synthetic peptide corresponding to Gly 796 -Ile 841 revealed Ile 803 -Leu 810 in ␣-helical conformation (40). The R808C mutation, found in this region, causes hereditary erythroid spherocytosis because of a failure to process AE1 to the cell surface (36). Consistent with that finding, R808C AE1 was not functional and was not biotinylated in the present study.…”
Section: Discussionsupporting
confidence: 80%
“…7 and Table I). Human mutations H834P and T837M both cause erythrocyte spherocytosis because of a failure of AE1 to be processed to the cell surface (36). In the present study, mutation to cysteine at each of these sites resulted in inactive protein, which was not labeled by biotin maleimide.…”
Section: Discussionmentioning
confidence: 65%
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“…The oligosaccharide on AE1 in HEK-293 cells remains in the high mannose form and is sensitive to digestion with endoglycosidase H. At steady state, about 30% of wild type AE1 in the high mannose form is present at the cell surface with the remainder in the ER (25). The expression of SAO and HS R760Q in HEK-293 cells results in their intracellular retention in the ER (23,26); however, no enhanced interaction of chaperones with the mutants relative to the wild type protein was detected by co-immunoprecipitation (supplemental Fig. S2).…”
Section: Ae1 and Mutants Can Interact With Cnx In Vivo-mentioning
confidence: 99%
“…The non-functional SAO AE1 protein that arises from a nine-amino acid deletion (⌬400 -408), however, is present in nearly equal amounts to the normal protein in the plasma membrane of red blood cells of heterozygotes (22). HS point mutations in the membrane domain of AE1 lead to a protein that is retained in the ER of transfected HEK-293 cells (23). The HS mutant, AE1 R760Q (Prague II), is completely absent in mature red blood cells (24), indicating defective trafficking to the plasma membrane during erythropoiesis.…”
Section: Ae1 and Mutants Can Interact With Cnx In Vivo-mentioning
confidence: 99%