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Endocrine
Erschienen in: Endocrine 1/2021

Open Access 28.09.2020 | Original Article

Pegvisomant in combination or pegvisomant alone after failure of somatostatin analogs in acromegaly patients: an observational French ACROSTUDY cohort study

verfasst von: Emmanuelle Kuhn, Philippe Caron, Brigitte Delemer, Isabelle Raingeard, Hervé Lefebvre, Gérald Raverot, Christine Cortet-Rudelli, Rachel Desailloud, Clementine Geffroy, Robin Henocque, Yves Brault, Thierry Brue, Philippe Chanson

Erschienen in: Endocrine | Ausgabe 1/2021

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Abstract

Objective

After surgery, when somatostatin analogs (SAs) do not normalise IGF-I, pegvisomant (PEG) is indicated. Our aim was to define the medical reasons for the treatment of patients with PEG as monotherapy (M) or combined with SA, either as primary bitherapy, PB (PEG is secondarily introduced after SA) or as secondary bitherapy, SB (SAs secondarily introduced after PEG).

Methods

We retrospectively analysed French data from ACROSTUDY.

Results

167, 88 and 57 patients were treated with M, PB or SB, respectively, during a median time of 80, 42 and 70 months. The median PEG dose was respectively 15, 10 and 20 mg. Before PEG, the mean IGF-I level did not differ between M and PB but the proportion of patients with suprasellar tumour extension was higher in PB group (67.5% vs. 44.4%, P = 0.022). SB regimen was used preferentially in patients with tumour increase and IGF-I level difficult to normalise under PEG. In both secondary regimens, the decrease of the frequency of PEG’s injections, compared to monotherapy was confirmed. However, the mean weekly dose of PEG between M and PB remained the same.

Conclusions

The medical rationale for continuing SAs rather than switching to PEG alone in patients who do not normalise IGF-I under SAs was a tumour concern with suprasellar extension and tumour shrinkage under SA. A potential explanation for introducing SA in association with PEG appears to be a tumour enlargement and difficulties to normalise IGF-I levels under PEG given alone. In both regimens, the prospect of lowering PEG injection frequency favoured the choice.
Literatur
1.
P. Chanson, Medical treatment of acromegaly with dopamine agonists or somatostatin analogs. Neuroendocrinology 103, 50–58 (2016)PubMed
2.
A. Giustina, P. Chanson, D. Kleinberg, M.D. Bronstein, D.R. Clemmons, A. Klibanski, A.J. van der Lely, C.J. Strasburger, S.W. Lamberts, K.K. Ho, F.F. Casanueva, S. Melmed, Expert consensus document: a consensus on the medical treatment of acromegaly. Nat. Rev. Endocrinol. 10, 243–248 (2014)PubMed
3.
L. Katznelson, E.R. Laws Jr., S. Melmed, M.E. Molitch, M.H. Murad, A. Utz, J.A. Wass, Acromegaly: an endocrine society clinical practice guideline. J. Clin. Endocrinol. Metab. 99, 3933–3951 (2014)PubMed
4.
S. Melmed, M.D. Bronstein, P. Chanson, A. Klibanski, F.F. Casanueva, J.A.H. Wass, C.J. Strasburger, A. Luger, D.R. Clemmons, A. Giustina, A consensus statement on acromegaly therapeutic outcomes. Nat. Rev. Endocrinol. 14, 552–561 (2018)PubMedPubMedCentral
5.
P. Nomikos, M. Buchfelder, R. Fahlbusch, The outcome of surgery in 668 patients with acromegaly using current criteria of biochemical ‘cure’. Eur. J. Endocrinol. 152, 379–387 (2005)PubMed
6.
J.A. Jane Jr., R.M. Starke, M.A. Elzoghby, D.L. Reames, S.C. Payne, M.O. Thorner, J.C. Marshall, E.R. Laws Jr., M.L. Vance, Endoscopic transsphenoidal surgery for acromegaly: remission using modern criteria, complications, and predictors of outcome. J. Clin. Endocrinol. Metab. 96, 2732–2740 (2011)PubMed
7.
F. Roelfsema, N.R. Biermasz, A.M. Pereira, Clinical factors involved in the recurrence of pituitary adenomas after surgical remission: a structured review and meta-analysis. Pituitary 15, 71–83 (2012)PubMed
8.
A.M. Abu Dabrh, K. Mohammed, N. Asi, W.H. Farah, Z. Wang, M.H. Farah, L.J. Prokop, L. Katznelson, M.H. Murad, Surgical interventions and medical treatments in treatment-naive patients with acromegaly: systematic review and meta-analysis. J. Clin. Endocrinol. Metab. 99, 4003–4014 (2014)PubMedPubMedCentral
9.
J.D. Carmichael, V.S. Bonert, M. Nuno, D. Ly, S. Melmed, Acromegaly clinical trial methodology impact on reported biochemical efficacy rates of somatostatin receptor ligand treatments: a meta-analysis. J. Clin. Endocrinol. Metab. 99, 1825–1833 (2014)PubMedPubMedCentral
10.
P.U. Freda, L. Katznelson, A.J. van der Lely, C.M. Reyes, S. Zhao, D. Rabinowitz, Long-acting somatostatin analog therapy of acromegaly: a meta-analysis. J. Clin. Endocrinol. Metab. 90, 4465–4473 (2005)PubMed
11.
P.J. Trainer, W.M. Drake, L. Katznelson, P.U. Freda, V. Herman-Bonert, A.J. van der Lely, E.V. Dimaraki, P.M. Stewart, K.E. Friend, M.L. Vance, G.M. Besser, J.A. Scarlett, M.O. Thorner, C. Parkinson, A. Klibanski, J.S. Powell, A.L. Barkan, M.C. Sheppard, M. Malsonado, D.R. Rose, D.R. Clemmons, G. Johannsson, B.A. Bengtsson, S. Stavrou, D.L. Kleinberg, D.M. Cook, L.S. Phillips, M. Bidlingmaier, C.J. Strasburger, S. Hackett, K. Zib, W.F. Bennett, R.J. Davis, Treatment of acromegaly with the growth hormone-receptor antagonist pegvisomant. N Engl. J. Med. 342, 1171–1177 (2000)PubMed
12.
A.J. van der Lely, R.K. Hutson, P.J. Trainer, G.M. Besser, A.L. Barkan, L. Katznelson, A. Klibanski, V. Herman-Bonert, S. Melmed, M.L. Vance, P.U. Freda, P.M. Stewart, K.E. Friend, D.R. Clemmons, G. Johannsson, S. Stavrou, D.M. Cook, L.S. Phillips, C.J. Strasburger, S. Hackett, K.A. Zib, R.J. Davis, J.A. Scarlett, M.O. Thorner, Long-term treatment of acromegaly with pegvisomant, a growth hormone receptor antagonist. Lancet 358, 1754–1759 (2001)PubMed
13.
A.J. van der Lely, B.M. Biller, T. Brue, M. Buchfelder, E. Ghigo, R. Gomez, J. Hey-Hadavi, F. Lundgren, N. Rajicic, C.J. Strasburger, S.M. Webb, M. Koltowska-Haggstrom, Long-term safety of pegvisomant in patients with acromegaly: comprehensive review of 1288 subjects in ACROSTUDY. J. Clin. Endocrinol. Metab. 97, 1589–1597 (2012)PubMed
14.
P.U. Freda, M.B. Gordon, N. Kelepouris, P. Jonsson, M. Koltowska-Haggstrom, A.J. van der Lely, Long-term treatment with pegvisomant as monotherapy in patients with acromegaly: experience from ACROSTUDY. Endocr. Pr. 21, 264–274 (2015)
15.
P. Chanson, T. Brue, B. Delemer, P. Caron, F. Borson-Chazot, H. Zouater, A. Medecins de l’Etude, Pegvisomant treatment in patients with acromegaly in clinical practice: the French ACROSTUDY. Ann. Endocrinol. 76, 664–670 (2015)
16.
M. Buchfelder, A.J. van der Lely, B.M.K. Biller, S.M. Webb, T. Brue, C.J. Strasburger, E. Ghigo, C. Camacho-Hubner, K. Pan, J. Lavenberg, P. Jonsson, J.H. Hey-Hadavi, Long-term treatment with pegvisomant: observations from 2090 acromegaly patients in ACROSTUDY. Eur. J. Endocrinol. 179, 419–427 (2018)PubMed
17.
J. Feenstra, W.W. de Herder, S.M. ten Have, A.W. van den Beld, R.A. Feelders, J.A. Janssen, A.J. van der Lely, Combined therapy with somatostatin analogues and weekly pegvisomant in active acromegaly. Lancet 365, 1644–1646 (2005)PubMed
18.
J.O. Jorgensen, U. Feldt-Rasmussen, J. Frystyk, J.W. Chen, L.O. Kristensen, C. Hagen, H. Orskov, Cotreatment of acromegaly with a somatostatin analog and a growth hormone receptor antagonist. J. Clin. Endocrinol. Metab. 90, 5627–5631 (2005)PubMed
19.
S.J. Neggers, M.O. van Aken, J.A. Janssen, R.A. Feelders, W.W. de Herder, A.J. van der Lely, Long-term efficacy and safety of combined treatment of somatostatin analogs and pegvisomant in acromegaly. J. Clin. Endocrinol. Metab. 92, 4598–4601 (2007)PubMed
20.
S.J. Neggers, A.J. van der Lely, Somatostatin analog and pegvisomant combination therapy for acromegaly. Nat. Rev. Endocrinol. 5, 546–552 (2009)PubMed
21.
P.J. Trainer, S. Ezzat, G.A. D’Souza, G. Layton, C.J. Strasburger, A randomized, controlled, multicentre trial comparing pegvisomant alone with combination therapy of pegvisomant and long-acting octreotide in patients with acromegaly. Clin. Endocrinol. 71, 549–557 (2009)
22.
S.J.C.M.M. Neggers, M.O. van Aken, W.W. de Herder, R.A. Feelders, J.A.M.J.L. Janssen, X. Badia, S.M. Webb, A.J. van der Lely, Quality of life in acromegalic patients during long-term somatostatin analog treatment with and without pegvisomant. J. Clin. Endocrinol. Metab. 93, 3853–3859 (2008)PubMed
23.
M. Madsen, P.L. Poulsen, H. Orskov, N. Moller, J.O. Jorgensen, Cotreatment with pegvisomant and a somatostatin analog (SA) in SA-responsive acromegalic patients. J. Clin. Endocrinol. Metab. 96, 2405–2413 (2011)PubMed
24.
C.J. Strasburger, A. Mattsson, P. Wilton, F. Aydin, J. Hey-Hadavi, B.M.K. Biller, Increasing frequency of combination medical therapy in the treatment of acromegaly with the GH receptor antagonist pegvisomant. Eur. J. Endocrinol. 178, 321–329 (2018)PubMedPubMedCentral
25.
J.H. Buhk, S. Jung, M.N. Psychogios, S. Goricke, S. Hartz, S. Schulz-Heise, R. Klingebiel, M. Forsting, H. Bruckmann, A. Dorfler, M. Jordan, M. Buchfelder, M. Knauth, Tumor volume of growth hormone-secreting pituitary adenomas during treatment with pegvisomant: a prospective multicenter study. J. Clin. Endocrinol. Metab. 95, 552–558 (2010)PubMed
26.
M. Buchfelder, D. Weigel, M. Droste, K. Mann, B. Saller, K. Brubach, G.K. Stalla, M. Bidlingmaier, C.J. Strasburger; Investigators of German Pegvisomant Observational Study, Pituitary tumor size in acromegaly during pegvisomant treatment: experience from MR re-evaluations of the German Pegvisomant Observational Study. Eur. J. Endocrinol. 161, 27–35 (2009)PubMed
27.
M. Marazuela, A.E. Paniagua, M.D. Gahete, T. Lucas, C. Alvarez-Escola, R. Manzanares, J. Cameselle-Teijeiro, M. Luque-Ramirez, R.M. Luque, E. Fernandez-Rodriguez, J.P. Castano, I. Bernabeu, Somatotroph tumor progression during pegvisomant therapy: a clinical and molecular study. J. Clin. Endocrinol. Metab. 96, E251–E259 (2011)PubMed
28.
A.L. Barkan, P. Burman, D.R. Clemmons, W.M. Drake, R.F. Gagel, P.E. Harris, P.J. Trainer, A.J. van der Lely, M.L. Vance, Glucose homeostasis and safety in patients with acromegaly converted from long-acting octreotide to pegvisomant. J. Clin. Endocrinol. Metab. 90, 5684–5691 (2005)PubMed
29.
W.M. Drake, S.V. Rowles, M.E. Roberts, F.K. Fode, G.M. Besser, J.P. Monson, P.J. Trainer, Insulin sensitivity and glucose tolerance improve in patients with acromegaly converted from depot octreotide to pegvisomant. Eur. J. Endocrinol. 149, 521–527 (2003)PubMed
30.
T. Feola, A. Cozzolino, I. Simonelli, E. Sbardella, C. Pozza, E. Giannetta, D. Gianfrilli, P. Pasqualetti, A. Lenzi, A.M. Isidori, Pegvisomant improves glucose metabolism in acromegaly: a meta-analysis of prospective interventional studies. J. Clin. Endocrinol. Metab. 104, 2892–2902 (2019)PubMed
31.
C.E. Higham, S. Rowles, D. Russell-Jones, A.M. Umpleby, P.J. Trainer, Pegvisomant improves insulin sensitivity and reduces overnight free fatty acid concentrations in patients with acromegaly. J. Clin. Endocrinol. Metab. 94, 2459–2463 (2009)PubMed
32.
R. Lindberg-Larsen, N. Moller, O. Schmitz, S. Nielsen, M. Andersen, H. Orskov, J.O. Jorgensen, The impact of pegvisomant treatment on substrate metabolism and insulin sensitivity in patients with acromegaly. J. Clin. Endocrinol. Metab. 92, 1724–1728 (2007)PubMed
33.
D.R. Rose, D.R. Clemmons, Growth hormone receptor antagonist improves insulin resistance in acromegaly. Growth Horm. IGF Res. 12, 418–424 (2002)PubMed
34.
S.J. Neggers, S.E. Franck, F.W. de Rooij, A.H. Dallenga, R.M. Poublon, R.A. Feelders, J.A. Janssen, M. Buchfelder, L.J. Hofland, J.O. Jorgensen, A.J. van der Lely, Long-term efficacy and safety of pegvisomant in combination with long-acting somatostatin analogs in acromegaly. J. Clin. Endocrinol. Metab. 99, 3644–3652 (2014)PubMed
35.
S.J. Neggers, A.J. van der Lely, Combination treatment with somatostatin analogues and pegvisomant in acromegaly. Growth Horm. IGF Res. 21, 129–133 (2011)PubMed
36.
A.J. van der Lely, I. Bernabeu, J. Cap, P. Caron, A. Colao, J. Marek, S. Neggers, P. Birman, Coadministration of lanreotide Autogel and pegvisomant normalizes IGF1 levels and is well tolerated in patients with acromegaly partially controlled by somatostatin analogs alone. Eur. J. Endocrinol. 164, 325–333 (2011)PubMed
37.
V.S. Bonert, L. Kennedy, S. Petersenn, A. Barkan, J. Carmichael, S. Melmed, Lipodystrophy in patients with acromegaly receiving pegvisomant. J. Clin. Endocrinol. Metab. 93, 3515–3518 (2008)PubMed
38.
P. Maffei, C. Martini, C. Pagano, N. Sicolo, F. Corbetti, Lipohypertrophy in acromegaly induced by the new growth hormone receptor antagonist pegvisomant. Ann. Intern. Med. 145, 310–312 (2006)PubMed
39.
G. Sesmilo, E. Resmini, I. Bernabeu, J. Aller, A. Soto, M. Mora, A. Pico, C. Fajardo, E. Torres, C. Alvarez-Escola, R. Garcia, C. Blanco, R. Camara, S. Gaztambide, I. Salinas, C.D. Pozo, I. Castells, C. Villabona, B. Biagetti, S.M. Webb, Escape and lipodystrophy in acromegaly during pegvisomant therapy, a retrospective multicentre Spanish study. Clin. Endocrinol. 81, 883–890 (2014)
40.
S.E. Franck, A. Muhammad, A.J. van der Lely, S.J. Neggers, Combined treatment of somatostatin analogues with pegvisomant in acromegaly. Endocrine 52, 206–213 (2016)PubMed
41.
A. Giustina, M.R. Ambrosio, P. Beck Peccoz, F. Bogazzi, S. Cannavo, L. De Marinis, E. De Menis, S. Grottoli, R. Pivonello, Use of Pegvisomant in acromegaly. An Italian Society of Endocrinology guideline. J. Endocrinol. Invest. 37, 1017–1030 (2014)PubMedPubMedCentral
42.
A. Giustina, G. Arnaldi, F. Bogazzi, S. Cannavo, A. Colao, L. De Marinis, E. De Menis, E. Degli Uberti, F. Giorgino, S. Grottoli, A.G. Lania, P. Maffei, R. Pivonello, E. Ghigo, Pegvisomant in acromegaly: an update. J. Endocrinol. Invest. 40, 577–589 (2017)PubMedPubMedCentral
43.
A. Bianchi, F. Valentini, R. Iuorio, M. Poggi, R. Baldelli, M. Passeri, A. Giampietro, L. Tartaglione, S. Chiloiro, M. Appetecchia, P. Gargiulo, A. Fabbri, V. Toscano, A. Pontecorvi, L. De Marinis, Long-term treatment of somatostatin analog-refractory growth hormone-secreting pituitary tumors with pegvisomant alone or combined with long-acting somatostatin analogs: a retrospective analysis of clinical practice and outcomes. J. Exp. Clin. Cancer Res. 32, 40 (2013)PubMedPubMedCentral
Metadaten
Titel
Pegvisomant in combination or pegvisomant alone after failure of somatostatin analogs in acromegaly patients: an observational French ACROSTUDY cohort study
verfasst von
Emmanuelle Kuhn
Philippe Caron
Brigitte Delemer
Isabelle Raingeard
Hervé Lefebvre
Gérald Raverot
Christine Cortet-Rudelli
Rachel Desailloud
Clementine Geffroy
Robin Henocque
Yves Brault
Thierry Brue
Philippe Chanson
Publikationsdatum
28.09.2020
Verlag
Springer US
Erschienen in
Endocrine / Ausgabe 1/2021
Print ISSN: 1355-008X
Elektronische ISSN: 1559-0100
DOI
https://doi.org/10.1007/s12020-020-02501-3

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