Prolactin stimulates ubiquitination, initial internalization, and degradation of its receptor via catalytic activation of Janus kinase 2

Swaminathan, Gayathri; Varghese, Bentley; Thangavel, Chellappagounder; Carbone, Christopher J.; Plotnikov, A.N.; Kumar, Krishna; Jablonski, Elizabeth M.; Clevenger, Charles V.; Goffin, Vincent; Deng, Luqin; Frank, Stuart J.; Fuchs, Serge Y.

doi:10.1677/joe-07-0554

Cited by 38 publications

(27 citation statements)

References 28 publications

(37 reference statements)

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“…2B). These results indicate that PRLr internalization is clathrin dependent and confirm our previous observations that in this experimental system, endocytosis of recombinant HA-tagged PRLr faithfully recapitulates the processes involved in the regulation of the endogenous receptor (39).…”

Section: Resultssupporting

confidence: 90%

“…Reversible cell surface biotinylation. Cell surface biotinylation was performed as previously described (20,24,39). This procedure uses immunoblotting to measure levels of biotinylated proteins that are protected from debiotinylation as a result of being internalized.…”

Section: Antibodiesmentioning

confidence: 99%

“…Ubiquitination and degradation of PRLr is mainly mediated by the ␤-transducin-repeat-containing protein (␤-TrCP) E3 ubiquitin ligase that is recruited to PRLr in a manner that requires phosphorylation of Ser349 of the receptor (28). Signaling induced by PRL (but not by a PRLr antagonist) and mediated by catalytic activation of Janus kinase 2 (Jak2) stimulates this Ser349 phosphorylation in addition to ubiquitination, initial internalization, and degradation of PRLr (39). Furthermore, the intracellular localization of Ser349-phosphorylated PRLr in human mammary tissues is consistent with its targeting to the lysosomal compartment (27).…”

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confidence: 99%

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Polyubiquitination of Prolactin Receptor Stimulates Its Internalization, Postinternalization Sorting, and Degradation via the Lysosomal Pathway

Varghese

Barrière

Carbone

et al. 2008

Molecular and Cellular Biology

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The ubiquitination of the receptor that mediates signaling induced by the polypeptide pituitary hormone prolactin (PRL) has been shown to lead to the degradation of this receptor and to the ensuing negative regulation of cellular responses to PRL. However, the mechanisms of PRL receptor (PRLr) proteolysis remain largely to be determined. Here we provide evidence that PRLr is internalized and primarily degraded via the lysosomal pathway. Ubiquitination of PRLr is essential for the rapid internalization of PRLr, which proceeds through a pathway dependent on clathrin and the assembly polypeptide 2 (AP2) adaptor complexes. Recruitment of AP2 to PRLr is stimulated by PRLr ubiquitination, which also is required for the targeting of already internalized PRLr to the lysosomal compartment. While mass spectrometry analysis revealed that both monoubiquitination and polyubiquitination (via both K48-and K63-linked chains) occur on PRLr, the results of experiments using forced expression of ubiquitin mutants indicate that PRLr polyubiquitination via K63-linked chains is important for efficient interaction of PRLr with AP2 as well as for efficient internalization, postinternalization sorting, and proteolytic turnover of PRLr. We discuss how specific ubiquitination may regulate early and late stages of endocytosis of PRLr and of related receptors to contribute to the negative regulation of the magnitude and duration of downstream signaling.Endocytosis of signaling receptors is a major mechanism used by cells to restrict the magnitude and duration of signal transduction induced by extracellular ligands. Ligand-induced endocytosis of cell surface receptors may occur through clathrin-dependent or -independent pathways. The clathrin-dependent pathway links receptors with clathrin-coated vesicles, which are specialized invaginations of the plasma membrane that concentrate receptors that become internalized. This pathway relies on the interaction of the assembly polypeptide 2 (AP2) clathrin adaptor complexes with specific endocytic signals located within the cytoplasmic domain of the receptors (5).AP2 complexes, which are involved in the assembly of clathrin triskelions at the plasma membrane, are composed of four components, including two adaptin subunits (␣ and ␤2) and two smaller subunits ( 2 and 2); among these subunits, each has different biological functions (34). There are specific endocytic motifs that are essential for receptor clustering on the membrane and clathrin-dependent internalization of receptors. For example, both tyrosine-and leucine-based motifs can be recognized by the AP2 complex through the interaction with its 2 subunit and with the ␤2 or ␣/ 2 hemicomplexes, respectively (5,8,13).The process of receptor endocytosis is not exclusively regulated by the linear motifs located on the cytoplasmic tail of receptors. Posttranslational modification by ubiquitination has also emerged as an important factor in the endocytosis and sorting of surface receptors. Ubiquitin is a 76-amino-acid protein that forms an isopeptide...

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Section: Resultssupporting

confidence: 90%

Section: Antibodiesmentioning

confidence: 99%

mentioning

confidence: 99%

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Polyubiquitination of Prolactin Receptor Stimulates Its Internalization, Postinternalization Sorting, and Degradation via the Lysosomal Pathway

Varghese

Barrière

Carbone

et al. 2008

Molecular and Cellular Biology

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“…[30][31][32][33] Importantly, Epo-induced EpoR internalization requires both JAK2 kinase activity and the tyrosine residues of the EpoR cytoplasmic domain. These results are consistent with studies demonstrating that ligand-stimulated internalization of the prolactin receptor 34 and the thrombopoietin receptor 31 also depends on associated JAK2 kinase activities. Moreover, as the EpoR/JAK2 complex functions as a unit that is equivalent to a receptor tyrosine kinase, these results are consistent with experiments showing that kinase activity is necessary for maximal rate of internalization and down-regulation of receptor tyrosine kinases.…”

Section: Discussionsupporting

confidence: 92%

Ligand-induced EpoR internalization is mediated by JAK2 and p85 and is impaired by mutations responsible for primary familial and congenital polycythemia

Sulahian¹,

Cleaver

Huang³

2009

Blood

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“…PRL Induces Ubiquitination of ZnT2-PRL stimulates ubiquitination (27), and ubiquitin serves as a sorting signal to regulate protein trafficking through the secretory compartment (reviewed in Ref. 22).…”

Section: Prl Transiently Stimulates Znt2-mediated Zinc Secretionmentioning

confidence: 99%

Prolactin (PRL)-stimulated Ubiquitination of ZnT2 Mediates a Transient Increase in Zinc Secretion Followed by ZnT2 Degradation in Mammary Epithelial Cells

Seo

Lee

Hennigar

et al. 2014

Journal of Biological Chemistry

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Prolactin stimulates ubiquitination, initial internalization, and degradation of its receptor via catalytic activation of Janus kinase 2

Cited by 38 publications

References 28 publications

Polyubiquitination of Prolactin Receptor Stimulates Its Internalization, Postinternalization Sorting, and Degradation via the Lysosomal Pathway

Polyubiquitination of Prolactin Receptor Stimulates Its Internalization, Postinternalization Sorting, and Degradation via the Lysosomal Pathway

Ligand-induced EpoR internalization is mediated by JAK2 and p85 and is impaired by mutations responsible for primary familial and congenital polycythemia

Prolactin (PRL)-stimulated Ubiquitination of ZnT2 Mediates a Transient Increase in Zinc Secretion Followed by ZnT2 Degradation in Mammary Epithelial Cells

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