2006
DOI: 10.1002/ijc.21802
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Nuclear targeting of a midregion PTHrP fragment is necessary for stimulating growth in breast cancer cells

Abstract: Parathyroid-hormone related protein (PTHrP) is the primary factor in humoral hypercalcemia of malignancy and is highly secreted by breast cancers. The pro-hormone undergoes posttranslational processing and cleavage to give rise to mature secretory peptides, one of which is midregion PTHrP (38-94/95/101) containing a nuclear localisation sequence (NLS) in amino acids (87)(88)(89)(90)(91)(92)(93)(94)(95)(96)(97)(98)(99)(100)(101)(102)(103)(104)(105)(106). The current study investigates whether the NLS in midregi… Show more

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Cited by 24 publications
(19 citation statements)
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“…This is consistent with data indicating that midregion PTHrP possesses a nuclear targeting signal (NTS) encompassing aminoacids 87-107 and that the lysine-rich 84-93 domain is per se able to direct importin b/Ran GTPase-mediated import of to the nucleoplasm under the control of phosphorylation/dephosphorylation events in T 85 [24, for review]. Intracrine role for PTHrP in cell growth, adhesion, migration, invasion, and integrin expression regulation has been documented for MCF-7 breast tumor cells over-expressing wild type versus NTS-mutated protein [25,26], and mobilization of intracellular calcium has been observed in different breast cancer cell lines treated with PTHrP (67-101), whose ability to translocate to the nucleus was reported in the same paper by Kumari et al [27]. Noteworthy, intracrine effects of midregion PTHrP domains have been described also in other experimental models [e.g.…”
Section: Introductionmentioning
confidence: 86%
“…This is consistent with data indicating that midregion PTHrP possesses a nuclear targeting signal (NTS) encompassing aminoacids 87-107 and that the lysine-rich 84-93 domain is per se able to direct importin b/Ran GTPase-mediated import of to the nucleoplasm under the control of phosphorylation/dephosphorylation events in T 85 [24, for review]. Intracrine role for PTHrP in cell growth, adhesion, migration, invasion, and integrin expression regulation has been documented for MCF-7 breast tumor cells over-expressing wild type versus NTS-mutated protein [25,26], and mobilization of intracellular calcium has been observed in different breast cancer cell lines treated with PTHrP (67-101), whose ability to translocate to the nucleus was reported in the same paper by Kumari et al [27]. Noteworthy, intracrine effects of midregion PTHrP domains have been described also in other experimental models [e.g.…”
Section: Introductionmentioning
confidence: 86%
“…This approach is in line with the work by other authors to obtain a detectable effect of PTHrP and its fragments in in vitro studies. (19,41,57) In conclusion, we have identified novel pathogenetic functions of PTHrP in MM related to tumor survival, proliferation, and OC hyperactivation. Because serum elevation of PTHrP in patients with solid tumors produces severe skeleton devastation and leads to a poor prognosis, a systematic analysis of PTHrP levels in MM patients would be advisable, to determine whether this peptide is a novel marker of disease progression.…”
Section: Discussionmentioning
confidence: 81%
“…The scrambled sequence (KKVKPKR) was reported as nonfunctional because it is unable to reach the nucleus even when it is localised in the cytoplasm. [44,29,46,47] The bioconjugates of cobaltocenium and ferrocene with NLS scr were totally different in their behaviour towards cellular uptake and nuclear localisation when compared with the wild-type NLS conjugates. These conjugates not only did not gain entry into the nuclei but were also unable to enter the intact cells.…”
Section: Discussionmentioning
confidence: 98%
“…[45] Various scrambled sequences of NLS in which Lys128 is replaced by other amino acids have been shown to be unable to enter cells and translocate into their nuclei. [29,46,47] Ferrocene (11) and cobaltocenium conjugates (13) of the scrambled NLS sequence, both labelled with FITC, were studied along with a metal-free, FITC-labelled scrambled peptide 9. All three compounds 9, 11 and 13 showed similar behaviour.…”
Section: Cellular and Nuclear Uptakementioning
confidence: 99%