β-Arrestin 1 and 2 and G protein-coupled receptor kinase 2 expression in pituitary adenomas: Role in the regulation of response to somatostatin analogue treatment in patients with acromegaly

Federico Gatto; Richard Feelders; Rob Van Der Pas; Johan M. Kros; Fadime Dogan; Peter M. Van Koetsveld; Aart Jan Van Der Lelij; Sebastian J.C.M.M. Neggers; Francesco Minuto; Wouter De Herder; Steven W.J. Lamberts; Diego Ferone; Leo J. Hofland

doi:10.1210/en.2013-1672

β-Arrestin 1 and 2 and G protein-coupled receptor kinase 2 expression in pituitary adenomas: Role in the regulation of response to somatostatin analogue treatment in patients with acromegaly

Federico Gatto
, Richard Feelders
, Rob Van Der Pas
, Johan M. Kros
, Fadime Dogan
, Peter M. Van Koetsveld
, Aart Jan Van Der Lelij
, Sebastian J.C.M.M. Neggers
, Francesco Minuto
, Wouter De Herder
, Steven W.J. Lamberts
, Diego Ferone
, Leo J. Hofland

Research output: Contribution to journal › Article › peer-review

62 Citations (Scopus)

Abstract

Recent in vitro studies highlighted G protein-coupled receptor kinase (GRK)2 and β-arrestins as important players in driving somatostatin receptor (SSTR) desensitization and trafficking. Our aim was to characterize GRK2 and β-arrestins expression in different pituitary adenomas and to investigate their potential role in the response to somatostatin analog (SSA) treatment in GH-secreting adenomas (GHomas). We evaluated mRNA expression of multiple SSTRs, GRK2, β-arrestin 1, and β-arrestin 2 in 41 pituitary adenomas (31 GHomas, 6 nonfunctioning [NFPAs], and 4 prolactinomas [PRLomas]). Within the GHomas group, mRNA data were correlated with the in vivo response to an acute octreotide test and with the GH-lowering effect of SSA in cultured primary cells. β-Arrestin 1 expression was low in all 3 adenoma histotypes. However, its expression was significantly lower in GHomas and PRLomas, compared with NFPAs (P < .01). GRK2 expression was higher in PRLomas and NFPAs compared with GHomas (P < .05). In the GHoma group, GRK2 expression was inversely correlated to β-arrestin 1 (P < .05) and positively correlated to β-arrestin 2 (P < .0001). SSA treatment did not affect GRK2 and β-arrestin expression in GHomas or in cultured rat pituitary tumor GH3 cells. Noteworthy, β-arrestin 1 was significantly lower (P < .05) in tumors responsive to octreotide treatment in vitro, whereas GRK2 and SSTR subtype 2 were significantly higher (P < .05). Likewise, β-arrestin 1 levels were inversely correlated with the in vivo response to acute octreotide test (P = .001), whereas GRK2 and SSTR subtype 2 expression were positively correlated (P < .05). In conclusion, for the first time, we characterized GRK2, β-arrestin 1, and β-arrestin 2 expression in a representative number of pituitary adenomas. β-Arrestin 1 and GRK2 seem to have a role in modulating GH secretion during SSA treatment.

Original language	English
Pages (from-to)	4715-4725
Number of pages	11
Journal	Endocrinology
Volume	154
Issue number	12
DOIs	https://doi.org/10.1210/en.2013-1672
Publication status	Published - 1 Dec 2013
Externally published	Yes

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10.1210/en.2013-1672

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Gatto, F., Feelders, R., Van Der Pas, R., Kros, J. M., Dogan, F., Van Koetsveld, P. M., Van Der Lelij, A. J., Neggers, S. J. C. M. M., Minuto, F., De Herder, W., Lamberts, S. W. J., Ferone, D., & Hofland, L. J. (2013). β-Arrestin 1 and 2 and G protein-coupled receptor kinase 2 expression in pituitary adenomas: Role in the regulation of response to somatostatin analogue treatment in patients with acromegaly. Endocrinology, 154(12), 4715-4725. https://doi.org/10.1210/en.2013-1672

@article{e086d9ca22c34a54b4411132d22132b5,

title = "β-Arrestin 1 and 2 and G protein-coupled receptor kinase 2 expression in pituitary adenomas: Role in the regulation of response to somatostatin analogue treatment in patients with acromegaly",

abstract = "Recent in vitro studies highlighted G protein-coupled receptor kinase (GRK)2 and β-arrestins as important players in driving somatostatin receptor (SSTR) desensitization and trafficking. Our aim was to characterize GRK2 and β-arrestins expression in different pituitary adenomas and to investigate their potential role in the response to somatostatin analog (SSA) treatment in GH-secreting adenomas (GHomas). We evaluated mRNA expression of multiple SSTRs, GRK2, β-arrestin 1, and β-arrestin 2 in 41 pituitary adenomas (31 GHomas, 6 nonfunctioning [NFPAs], and 4 prolactinomas [PRLomas]). Within the GHomas group, mRNA data were correlated with the in vivo response to an acute octreotide test and with the GH-lowering effect of SSA in cultured primary cells. β-Arrestin 1 expression was low in all 3 adenoma histotypes. However, its expression was significantly lower in GHomas and PRLomas, compared with NFPAs (P < .01). GRK2 expression was higher in PRLomas and NFPAs compared with GHomas (P < .05). In the GHoma group, GRK2 expression was inversely correlated to β-arrestin 1 (P < .05) and positively correlated to β-arrestin 2 (P < .0001). SSA treatment did not affect GRK2 and β-arrestin expression in GHomas or in cultured rat pituitary tumor GH3 cells. Noteworthy, β-arrestin 1 was significantly lower (P < .05) in tumors responsive to octreotide treatment in vitro, whereas GRK2 and SSTR subtype 2 were significantly higher (P < .05). Likewise, β-arrestin 1 levels were inversely correlated with the in vivo response to acute octreotide test (P = .001), whereas GRK2 and SSTR subtype 2 expression were positively correlated (P < .05). In conclusion, for the first time, we characterized GRK2, β-arrestin 1, and β-arrestin 2 expression in a representative number of pituitary adenomas. β-Arrestin 1 and GRK2 seem to have a role in modulating GH secretion during SSA treatment.",

author = "Federico Gatto and Richard Feelders and \{Van Der Pas\}, Rob and Kros, \{Johan M.\} and Fadime Dogan and \{Van Koetsveld\}, \{Peter M.\} and \{Van Der Lelij\}, \{Aart Jan\} and Neggers, \{Sebastian J.C.M.M.\} and Francesco Minuto and \{De Herder\}, Wouter and Lamberts, \{Steven W.J.\} and Diego Ferone and Hofland, \{Leo J.\}",

year = "2013",

month = dec,

day = "1",

doi = "10.1210/en.2013-1672",

language = "English",

volume = "154",

pages = "4715--4725",

journal = "Endocrinology",

issn = "0013-7227",

publisher = "Endocrine Society",

number = "12",

}

Gatto, F, Feelders, R, Van Der Pas, R, Kros, JM, Dogan, F, Van Koetsveld, PM, Van Der Lelij, AJ, Neggers, SJCMM, Minuto, F, De Herder, W, Lamberts, SWJ, Ferone, D & Hofland, LJ 2013, 'β-Arrestin 1 and 2 and G protein-coupled receptor kinase 2 expression in pituitary adenomas: Role in the regulation of response to somatostatin analogue treatment in patients with acromegaly', Endocrinology, vol. 154, no. 12, pp. 4715-4725. https://doi.org/10.1210/en.2013-1672

β-Arrestin 1 and 2 and G protein-coupled receptor kinase 2 expression in pituitary adenomas: Role in the regulation of response to somatostatin analogue treatment in patients with acromegaly. / Gatto, Federico; Feelders, Richard; Van Der Pas, Rob et al.
In: Endocrinology, Vol. 154, No. 12, 01.12.2013, p. 4715-4725.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - β-Arrestin 1 and 2 and G protein-coupled receptor kinase 2 expression in pituitary adenomas

T2 - Role in the regulation of response to somatostatin analogue treatment in patients with acromegaly

AU - Gatto, Federico

AU - Feelders, Richard

AU - Van Der Pas, Rob

AU - Kros, Johan M.

AU - Dogan, Fadime

AU - Van Koetsveld, Peter M.

AU - Van Der Lelij, Aart Jan

AU - Neggers, Sebastian J.C.M.M.

AU - Minuto, Francesco

AU - De Herder, Wouter

AU - Lamberts, Steven W.J.

AU - Ferone, Diego

AU - Hofland, Leo J.

PY - 2013/12/1

Y1 - 2013/12/1

N2 - Recent in vitro studies highlighted G protein-coupled receptor kinase (GRK)2 and β-arrestins as important players in driving somatostatin receptor (SSTR) desensitization and trafficking. Our aim was to characterize GRK2 and β-arrestins expression in different pituitary adenomas and to investigate their potential role in the response to somatostatin analog (SSA) treatment in GH-secreting adenomas (GHomas). We evaluated mRNA expression of multiple SSTRs, GRK2, β-arrestin 1, and β-arrestin 2 in 41 pituitary adenomas (31 GHomas, 6 nonfunctioning [NFPAs], and 4 prolactinomas [PRLomas]). Within the GHomas group, mRNA data were correlated with the in vivo response to an acute octreotide test and with the GH-lowering effect of SSA in cultured primary cells. β-Arrestin 1 expression was low in all 3 adenoma histotypes. However, its expression was significantly lower in GHomas and PRLomas, compared with NFPAs (P < .01). GRK2 expression was higher in PRLomas and NFPAs compared with GHomas (P < .05). In the GHoma group, GRK2 expression was inversely correlated to β-arrestin 1 (P < .05) and positively correlated to β-arrestin 2 (P < .0001). SSA treatment did not affect GRK2 and β-arrestin expression in GHomas or in cultured rat pituitary tumor GH3 cells. Noteworthy, β-arrestin 1 was significantly lower (P < .05) in tumors responsive to octreotide treatment in vitro, whereas GRK2 and SSTR subtype 2 were significantly higher (P < .05). Likewise, β-arrestin 1 levels were inversely correlated with the in vivo response to acute octreotide test (P = .001), whereas GRK2 and SSTR subtype 2 expression were positively correlated (P < .05). In conclusion, for the first time, we characterized GRK2, β-arrestin 1, and β-arrestin 2 expression in a representative number of pituitary adenomas. β-Arrestin 1 and GRK2 seem to have a role in modulating GH secretion during SSA treatment.

AB - Recent in vitro studies highlighted G protein-coupled receptor kinase (GRK)2 and β-arrestins as important players in driving somatostatin receptor (SSTR) desensitization and trafficking. Our aim was to characterize GRK2 and β-arrestins expression in different pituitary adenomas and to investigate their potential role in the response to somatostatin analog (SSA) treatment in GH-secreting adenomas (GHomas). We evaluated mRNA expression of multiple SSTRs, GRK2, β-arrestin 1, and β-arrestin 2 in 41 pituitary adenomas (31 GHomas, 6 nonfunctioning [NFPAs], and 4 prolactinomas [PRLomas]). Within the GHomas group, mRNA data were correlated with the in vivo response to an acute octreotide test and with the GH-lowering effect of SSA in cultured primary cells. β-Arrestin 1 expression was low in all 3 adenoma histotypes. However, its expression was significantly lower in GHomas and PRLomas, compared with NFPAs (P < .01). GRK2 expression was higher in PRLomas and NFPAs compared with GHomas (P < .05). In the GHoma group, GRK2 expression was inversely correlated to β-arrestin 1 (P < .05) and positively correlated to β-arrestin 2 (P < .0001). SSA treatment did not affect GRK2 and β-arrestin expression in GHomas or in cultured rat pituitary tumor GH3 cells. Noteworthy, β-arrestin 1 was significantly lower (P < .05) in tumors responsive to octreotide treatment in vitro, whereas GRK2 and SSTR subtype 2 were significantly higher (P < .05). Likewise, β-arrestin 1 levels were inversely correlated with the in vivo response to acute octreotide test (P = .001), whereas GRK2 and SSTR subtype 2 expression were positively correlated (P < .05). In conclusion, for the first time, we characterized GRK2, β-arrestin 1, and β-arrestin 2 expression in a representative number of pituitary adenomas. β-Arrestin 1 and GRK2 seem to have a role in modulating GH secretion during SSA treatment.

UR - https://www.scopus.com/pages/publications/84888253134

U2 - 10.1210/en.2013-1672

DO - 10.1210/en.2013-1672

M3 - Article

C2 - 24169548

AN - SCOPUS:84888253134

SN - 0013-7227

VL - 154

SP - 4715

EP - 4725

JO - Endocrinology

JF - Endocrinology

IS - 12

ER -

β-Arrestin 1 and 2 and G protein-coupled receptor kinase 2 expression in pituitary adenomas: Role in the regulation of response to somatostatin analogue treatment in patients with acromegaly

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