Literature DB >> 9235948

Role of the C terminus in histamine H2 receptor signaling, desensitization, and agonist-induced internalization.

Y Fukushima1, T Asano, K Takata, M Funaki, T Ogihara, M Anai, K Tsukuda, T Saitoh, H Katagiri, M Aihara, N Matsuhashi, Y Oka, Y Yazaki, K Sugano.   

Abstract

To evaluate the role of the histamine H2 receptor C terminus in signaling, desensitization, and agonist-induced internalization, canine H2 receptors with truncated C termini were generated. Wild-type (WT) and truncated receptors were tagged at their N termini with a hemagglutinin (HA) epitope and expressed in COS7 cells. Most of the C-terminal intracellular tail could be truncated (51 of 70 residues, termed T308 mutant) without loss of functions: cAMP production, tiotidine binding, and plasma membrane targeting. In fact, the T308 mutant produced more cAMP than the WT when cell-surface expression per cell was equivalent. Pretreatment of cells with 10(-5) M histamine desensitized cAMP productions via WT and T308 receptors to similar extents. Incubation of cells expressing WT receptors with 10(-5) M histamine reduced cell-surface anti-HA antibody binding by approximately 30% (by 30 min, t1/2 approximately 15 min), but did not affect the Bmax of tiotidine in membrane fractions, which represents total receptor amounts, suggesting that WT receptors were internalized from the cell surface. In contrast, no internalization was observed with T308 receptors following histamine treatment. A mutant with a deletion of the 30 C-terminal amino acids, termed T329, was functional but was as potent as the WT in terms of cAMP production. Apart from being desensitized by histamine, the internalization of the receptor was indistinguishable from that of the WT. Internalization was observed in the T320 but not in T313 mutant, narrowing the region involved in internalization to that between Glu314 and Asn320 (ETSLRSN). Of these seven residues, either Thr315, Ser316, or both, were replaced with Ala. Thr315 and Ser316 are conserved among species. The mutation at Thr315 (but not that at Ser316) abolished internalization. Taken together, these results demonstrate that Thr315 is involved in agonist-induced internalization. Furthermore, the finding that T308 receptors were desensitized in the absence of internalization suggests that internalization and desensitization are meditated by independent mechanisms.

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Year:  1997        PMID: 9235948     DOI: 10.1074/jbc.272.31.19464

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  7 in total

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3.  Effects of N-alpha-methyl-histamine on human H(2) receptors expressed in CHO cells.

Authors:  T Saitoh; Y Fukushima; H Otsuka; M Ishikawa; M Tamai; H Takahashi; H Mori; T Asano; M Anai; T Ishikawa; T Katsube; K Ogawa; T Kajiwara; M Omata; S Ohkawa
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Review 5.  The Roles of Cardiovascular H2-Histamine Receptors Under Normal and Pathophysiological Conditions.

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6.  Histamine treatment induces rearrangements of orthogonal arrays of particles (OAPs) in human AQP4-expressing gastric cells.

Authors:  M Carmosino; G Procino; G P Nicchia; R Mannucci; J M Verbavatz; R Gobin; M Svelto; G Valenti
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Authors:  Brahim Tighilet; Christiane Mourre; Michel Lacour
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  7 in total

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