Cell specific interaction of pasireotide: review of preclinical studies in somatotroph and corticotroph pituitary cells

Gatto, Federico; Arvigo, Marica; Amarù, Jessica; Campana, Claudia; Cocchiara, Francesco; Graziani, Giulia; Bruzzone, Eleonora; Giusti, Massimo; Boschetti, Mara; Ferone, Diego

doi:10.1007/s11102-018-0926-y

Cited by 18 publications

(19 citation statements)

References 56 publications

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“…demonstrated that, in HEK 293 cells stably transfected with human SST 5 , PAS was superior to OCT in decreasing intracellular cAMP levels and in the stimulation of ERK1/2 phosphorylation [104]. This evidence, derived from transfected cell models, is in line with subsequent preclinical studies carried out in corticotroph pituitary cells (mainly expressing SST 5 among all SST subtypes), which show a greater efficacy of PAS, compared to first-generation SRLs, in the inhibition of basal and/or CRH-stimulated ACTH secretion [105,106].…”

Section: “Old” and “New” Somatostatin Receptor Ligandssupporting

confidence: 56%

Biological and Biochemical Basis of the Differential Efficacy of First and Second Generation Somatostatin Receptor Ligands in Neuroendocrine Neoplasms

Gatto

Barbieri²,

Arvigo

et al. 2019

IJMS

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Endogenous somatostatin shows anti-secretory effects in both physiological and pathological settings, as well as inhibitory activity on cell growth. Since somatostatin is not suitable for clinical practice, researchers developed synthetic somatostatin receptor ligands (SRLs) to overcome this limitation. Currently, SRLs represent pivotal tools in the treatment algorithm of neuroendocrine tumors (NETs). Octreotide and lanreotide are the first-generation SRLs developed and show a preferential binding affinity to somatostatin receptor (SST) subtype 2, while pasireotide, which is a second-generation SRL, has high affinity for multiple SSTs (SST5 > SST2 > SST3 > SST1). A number of studies demonstrated that first-generation and second-generation SRLs show distinct functional properties, besides the mere receptor affinity. Therefore, the aim of the present review is to critically review the current evidence on the biological effects of SRLs in pituitary adenomas and neuroendocrine tumors, by mainly focusing on the differences between first-generation and second-generation ligands.

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Section: “Old” and “New” Somatostatin Receptor Ligandssupporting

confidence: 56%

Biological and Biochemical Basis of the Differential Efficacy of First and Second Generation Somatostatin Receptor Ligands in Neuroendocrine Neoplasms

Gatto

Barbieri²,

Arvigo

et al. 2019

IJMS

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“…Patient 1 was never treated with radiotherapy, so the most likely explanation currently is that chronic pasireotide LAR was responsible. The mechanism by which this involution occurred is unknown but we suggest that activation of SST5-predominant anti-proliferative and pro-apoptotic pathways as seen in corticotropes could also be involved in somatotropinomas with disordered AIP function (24, 25). Patient 2 has had a shorter duration of pasireotide LAR treatment overall, but as seen in Fig.…”

Section: Discussionmentioning

confidence: 93%

AIP-mutated acromegaly resistant to first-generation somatostatin analogs: long-term control with pasireotide LAR in two patients

Daly

Rostomyan

Betea

et al. 2019

Endocrine Connections

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Acromegaly is a rare disease due to chronic excess growth hormone (GH) and IGF-1. Aryl hydrocarbon receptor interacting protein (AIP) mutations are associated with an aggressive, inheritable form of acromegaly that responds poorly to SST2-specific somatostatin analogs (SSA). The role of pasireotide, an SSA with affinity for multiple SSTs, in patients with AIP mutations has not been reported. We studied two AIP mutation positive acromegaly patients with early-onset, invasive macroadenomas and inoperable residues after neurosurgery. Patient 1 came from a FIPA kindred and had uncontrolled GH/IGF-1 throughout 10 years of octreotide/lanreotide treatment. When switched to pasireotide LAR, he rapidly experienced hormonal control which was associated with marked regression of his tumor residue. Pasireotide LAR was stopped after >10 years due to low IGF-1 and he maintained hormonal control without tumor regrowth for >18 months off pasireotide LAR. Patient 2 had a pituitary adenoma diagnosed when aged 17 that was not cured by surgery. Chronic pasireotide LAR therapy produced hormonal control and marked tumor shrinkage but control was lost when switched to octreotide. Tumor immunohistochemistry showed absent AIP and SST2 staining and positive SST5. Her AIP mutation positive sister developed a 2.5 cm follicular thyroid carcinoma aged 21 with tumoral loss of heterozygosity at the AIP locus and absent AIP staining. Patients 1 and 2 required multi-modal therapy to control diabetes. On stopping pasireotide LAR after >10 years of treatment, Patient 1’s glucose metabolism returned to baseline levels. Long-term pasireotide LAR therapy can be beneficial in some AIP mutation positive acromegaly patients that are resistant to first-generation SSA.

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“…In functioning corticotroph tumors, pasireotide is indicated in order to decrease hypercortisolism. In vitro studies on corticotroph tumor cells have found a decrease in ACTH release following use of pasireotide, which seems to be mediated by SST5 (12,17,40,41,42). Indeed, SST5 is the most highly expressed somatostatin receptor in corticotroph tumors (12,20,42), and it has been shown in previous studies that octreotide, which targets SST2, is less effective than pasireotide in decreasing cortisol levels and that SST2 is downregulated in the context of exposure to high glucocorticoid levels (41, 42).…”

Section: Discussionmentioning

confidence: 99%

“…In vitro studies on corticotroph tumor cells have found a decrease in ACTH release following use of pasireotide, which seems to be mediated by SST5 (12,17,40,41,42). Indeed, SST5 is the most highly expressed somatostatin receptor in corticotroph tumors (12,20,42), and it has been shown in previous studies that octreotide, which targets SST2, is less effective than pasireotide in decreasing cortisol levels and that SST2 is downregulated in the context of exposure to high glucocorticoid levels (41, 42). The response rate to pasireotide treatment in Cushing's disease obtained in previously published clinical trials was between 20 to 40% (13,14), which is in agreement with the number of patients with functioning corticotroph tumors expressing SST5 with an IRS score of moderate or strong in our cohort, suggesting that only one-third of functioning corticotroph pituitary tumors are likely to be sensitive to pasireotide treatment.…”

Section: Discussionmentioning

confidence: 99%

SST5 expression and USP8 mutation in functioning and silent corticotroph pituitary tumors

Castellnou

Vasiljevic

Lapras

et al. 2020

Endocrine Connections

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Objective Somatostatin receptor type 5 (SST5) is inconsistently expressed by corticotroph tumors, with higher expression found in corticotropinomas having ubiquitin-specific protease 8 (USP8) mutations. Aims were to study the correlation between characteristics of corticotropinomas and SST5 expression/USP8 mutation status and to describe the response to pasireotide in five patients. Design Retrospective cohort study. Methods Clinico-biochemical, radiological and pathological data of 62 patients, operated for a functioning or silent corticotropinoma between 2013 and 2017, were collected. SST5 expression was measured by immunohistochemistry (clone UMB-4, Abcam, IRS > 1 being considered positive), and Sanger sequencing was performed on 50 tumors to screen for USP8 mutations. Results SST5 expression was positive in 26/62 pituitary tumors. A moderate or strong IRS was found in 15/58 corticotropinomas and in 13/35 functioning corticotropinomas. Among functioning tumors, those expressing SST5 were more frequent in women (22/24 vs 9/15, P = 0.04) and had a lower grade (P = 0.04) compared to others. USP8 mutations were identified in 13/50 pituitary tumors and were more frequent in functioning compared to silent tumors (11/30 vs 2/20, P = 0.05). SST5 expression was more frequent in USP8mut vs USP8wt tumors (10/11 vs 7/19, P = 0.007). Among treated patients, normal urinary free cortisol levels were obtained in three patients (IRS 0, 2 and 6), while a four-fold decrease was observed in one patient (IRS 4). Conclusion SST5 expression appears to be associated with functioning, USP8mut and lower grade corticotropinomas. A correlation between SST5 expression or USP8mut and response to pasireotide remains to be confirmed.

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Cell specific interaction of pasireotide: review of preclinical studies in somatotroph and corticotroph pituitary cells

Cited by 18 publications

References 56 publications

Biological and Biochemical Basis of the Differential Efficacy of First and Second Generation Somatostatin Receptor Ligands in Neuroendocrine Neoplasms

Biological and Biochemical Basis of the Differential Efficacy of First and Second Generation Somatostatin Receptor Ligands in Neuroendocrine Neoplasms

AIP-mutated acromegaly resistant to first-generation somatostatin analogs: long-term control with pasireotide LAR in two patients

SST5 expression and USP8 mutation in functioning and silent corticotroph pituitary tumors

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