Browsing by Author "Chanson, Philippe (56249200300)"
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Publication Macimorelin as a diagnostic test for adult GH deficiency(2018) ;Garcia, Jose M. (53873831800) ;Biller, Beverly M. K. (7006404171) ;Korbonits, Márta (7004190977) ;Popovic, Vera (57294508600) ;Luger, Anton (35544522000) ;Strasburger, Christian J. (35402133700) ;Chanson, Philippe (56249200300) ;Medic-Stojanoska, Milica (23389630200) ;Schopohl, Jochen (7003794378) ;Zakrzewska, Anna (57204332617) ;Pekic, Sandra (6602553641) ;Bolanowski, Marek (7003537848) ;Swerdloff, Ronald (7102295009) ;Wang, Christina (57218503311) ;Blevins, Thomas (25027004800) ;Marcelli, Marco (57204289614) ;Ammer, Nicola (57198428983) ;Sachse, Richard (57204317470)Yuen, Kevin C. J. (7202333713)Purpose: The diagnosis of adult GH deficiency (AGHD) is challenging and often requires confirmation with a GH stimulation test (GHST). The insulin tolerance test (ITT) is considered the reference standard GHST but is labor intensive, can cause severe hypoglycemia, and is contraindicated for certain patients. Macimorelin, an orally active GH secretagogue, could be used to diagnose AGHD by measuring stimulated GH levels after an oral dose. Materials and Methods: The present multicenter, open-label, randomized, two-way crossover trial was designed to validate the efficacy and safety of single-dose oral macimorelin for AGHD diagnosis compared with the ITT. Subjects with high (n = 38), intermediate (n = 37), and low (n = 39) likelihood for AGHD and healthy, matched controls (n = 25) were included in the efficacy analysis. Results: After the first test, 99% of macimorelin tests and 82% of ITTs were evaluable. Using GH cutoff levels of 2.8 ng/mL for macimorelin and 5.1 ng/mL for ITTs, the negative agreement was 95.38% (95% CI, 87% to 99%), the positive agreement was 74.32% (95% CI, 63% to 84%), sensitivity was 87%, and specificity was 96%. On retesting, the reproducibility was 97% for macimorelin (n = 33). In post hoc analyses, a GH cutoff of 5.1 ng/mL for both tests resulted in 94% (95% CI, 85% to 98%) negative agreement, 82% (95% CI, 72% to 90%) positive agreement, 92% sensitivity, and 96% specificity. No serious adverse events were reported for macimorelin. Conclusions: Oral macimorelin is a simple, well-tolerated, reproducible, and safe diagnostic test for AGHD with accuracy comparable to that of the ITT. A GH cutoff of 5.1 ng/mL for the macimorelin test provides an excellent balance between sensitivity and specificity. Copyright © 2018 Endocrine Society. - Some of the metrics are blocked by yourconsent settings
Publication Macimorelin as a diagnostic test for adult GH deficiency(2018) ;Garcia, Jose M. (53873831800) ;Biller, Beverly M. K. (7006404171) ;Korbonits, Márta (7004190977) ;Popovic, Vera (57294508600) ;Luger, Anton (35544522000) ;Strasburger, Christian J. (35402133700) ;Chanson, Philippe (56249200300) ;Medic-Stojanoska, Milica (23389630200) ;Schopohl, Jochen (7003794378) ;Zakrzewska, Anna (57204332617) ;Pekic, Sandra (6602553641) ;Bolanowski, Marek (7003537848) ;Swerdloff, Ronald (7102295009) ;Wang, Christina (57218503311) ;Blevins, Thomas (25027004800) ;Marcelli, Marco (57204289614) ;Ammer, Nicola (57198428983) ;Sachse, Richard (57204317470)Yuen, Kevin C. J. (7202333713)Purpose: The diagnosis of adult GH deficiency (AGHD) is challenging and often requires confirmation with a GH stimulation test (GHST). The insulin tolerance test (ITT) is considered the reference standard GHST but is labor intensive, can cause severe hypoglycemia, and is contraindicated for certain patients. Macimorelin, an orally active GH secretagogue, could be used to diagnose AGHD by measuring stimulated GH levels after an oral dose. Materials and Methods: The present multicenter, open-label, randomized, two-way crossover trial was designed to validate the efficacy and safety of single-dose oral macimorelin for AGHD diagnosis compared with the ITT. Subjects with high (n = 38), intermediate (n = 37), and low (n = 39) likelihood for AGHD and healthy, matched controls (n = 25) were included in the efficacy analysis. Results: After the first test, 99% of macimorelin tests and 82% of ITTs were evaluable. Using GH cutoff levels of 2.8 ng/mL for macimorelin and 5.1 ng/mL for ITTs, the negative agreement was 95.38% (95% CI, 87% to 99%), the positive agreement was 74.32% (95% CI, 63% to 84%), sensitivity was 87%, and specificity was 96%. On retesting, the reproducibility was 97% for macimorelin (n = 33). In post hoc analyses, a GH cutoff of 5.1 ng/mL for both tests resulted in 94% (95% CI, 85% to 98%) negative agreement, 82% (95% CI, 72% to 90%) positive agreement, 92% sensitivity, and 96% specificity. No serious adverse events were reported for macimorelin. Conclusions: Oral macimorelin is a simple, well-tolerated, reproducible, and safe diagnostic test for AGHD with accuracy comparable to that of the ITT. A GH cutoff of 5.1 ng/mL for the macimorelin test provides an excellent balance between sensitivity and specificity. Copyright © 2018 Endocrine Society. - Some of the metrics are blocked by yourconsent settings
Publication Reassessing the role of the p.(Arg304Gln) missense AIP variant in pituitary tumorigenesis(2025) ;Loughrey, Paul Benjamin (56993777000) ;Mothojakan, Nadira B. (57207909495) ;Iacovazzo, Donato (55256179800) ;Arni, Ankit (59218014300) ;Aflorei, Elena D. (55957763500) ;Arnaldi, Giorgio (56266312900) ;Barlier, Anne (55747498800) ;Beckers, Albert (7006603216) ;Bizzi, Mariana F. (57190065800) ;Chanson, Philippe (56249200300) ;Dal, Jakob (55227675100) ;Daly, Adrian F. (7102328180) ;Dang, Mary N. (57216196783) ;David, Alessia (8715391700) ;Andrade, Matheus de Oliveira (59285917000) ;Else, Tobias (6505875282) ;Elston, Marianne S. (57217465978) ;Evans, Amy (59739865200) ;Ferrau, Francesco (56426879500) ;Fica, Simona (14053740600) ;Flanagan, Daniel (7103327368) ;Gadelha, Monica R. (6604086845) ;Grossman, Ashley B. (35401342800) ;Kapur, Sonal (57188661661) ;Khoo, Bernard (36185394100) ;Kumar, Ajith V. (56312818100) ;Kumar-Sinha, Chandan (6507499436) ;Lechan, Ronald M. (7005636129) ;Ludman, Mark (6603994288) ;Metherell, Louise A. (6602747281) ;Miljic, Dragana (6505968542) ;Mourougavelou, Vishnou (57193704844) ;Musat, Madalina (6602752334) ;Occhi, Gianluca (6603762575) ;Owens, Martina (23502058900) ;Pascanu, Ionela (35146485800) ;Pinheiro, Sergio V. B. (36055726400) ;Radian, Serban (15770354700) ;Ribeiro-Oliveira, Antonio (16176083100) ;Schöfl, Christof (7004108255) ;Patel, Kashyap A. (57188657944) ;Hernández-Ramírez, Laura C. (55511259300)Korbonits, Márta (7004190977)Objective: Heterozygous germline loss-of-function variants in AIP are associated with young-onset growth hormone and/or prolactin-secreting pituitary tumours. However, the pathogenic role of the c.911G > A; p.(Arg304Gln) (R304Q) AIP variant has been controversial. Recent data from public exome/genome databases show this variant is not infrequent. The objective of this work was to reassess the pathogenicity of R304Q based on clinical, genomic, and functional assay data. Design: Data were collected on published R304Q pituitary neuroendocrine tumour cases and from International Familial Isolated Pituitary Adenoma Consortium R304Q cases (n = 38, R304Q cohort). Clinical features, population cohort frequency, computational analyses, prediction models, presence of loss-of-heterozygosity, and in vitro/in vivo functional studies were assessed and compared with data from pathogenic/likely pathogenic AIP variant patients (AIPmut cohort, n = 184). Results: Of 38 R304Q patients, 61% (23/38) had growth hormone excess, in contrast to 80% of AIPmut cohort (147/184, P < .001). R304Q cohort was older at disease onset and diagnosis than the AIPmut cohort (median [quartiles] onset: 25 y [16-35] vs 16 y [14-23], P < .001; median [quartiles] diagnosis: 36 y [24-44] vs 21 y [15-29], P < .001). R304Q is present in gnomADv2.1 (0.31%) and UK Biobank (0.16%), including three persons with homozygous R304Q. No loss-of-heterozygosity was detected in four R304Q pituitary neuroendocrine tumour samples. In silico predictions and experimental data were conflicting. Conclusions: Evidence suggests that R304Q is not pathogenic for pituitary neuroendocrine tumour. We recommend changing this variant classification to likely benign and do not recommend pre-symptomatic genetic testing of family members or follow-up of already identified unaffected individuals with the R304Q variant. © The Author(s) 2025. Published by Oxford University Press on behalf of European Society of Endocrinology. - Some of the metrics are blocked by yourconsent settings
Publication Reassessing the role of the p.(Arg304Gln) missense AIP variant in pituitary tumorigenesis(2025) ;Loughrey, Paul Benjamin (56993777000) ;Mothojakan, Nadira B. (57207909495) ;Iacovazzo, Donato (55256179800) ;Arni, Ankit (59218014300) ;Aflorei, Elena D. (55957763500) ;Arnaldi, Giorgio (56266312900) ;Barlier, Anne (55747498800) ;Beckers, Albert (7006603216) ;Bizzi, Mariana F. (57190065800) ;Chanson, Philippe (56249200300) ;Dal, Jakob (55227675100) ;Daly, Adrian F. (7102328180) ;Dang, Mary N. (57216196783) ;David, Alessia (8715391700) ;Andrade, Matheus de Oliveira (59285917000) ;Else, Tobias (6505875282) ;Elston, Marianne S. (57217465978) ;Evans, Amy (59739865200) ;Ferrau, Francesco (56426879500) ;Fica, Simona (14053740600) ;Flanagan, Daniel (7103327368) ;Gadelha, Monica R. (6604086845) ;Grossman, Ashley B. (35401342800) ;Kapur, Sonal (57188661661) ;Khoo, Bernard (36185394100) ;Kumar, Ajith V. (56312818100) ;Kumar-Sinha, Chandan (6507499436) ;Lechan, Ronald M. (7005636129) ;Ludman, Mark (6603994288) ;Metherell, Louise A. (6602747281) ;Miljic, Dragana (6505968542) ;Mourougavelou, Vishnou (57193704844) ;Musat, Madalina (6602752334) ;Occhi, Gianluca (6603762575) ;Owens, Martina (23502058900) ;Pascanu, Ionela (35146485800) ;Pinheiro, Sergio V. B. (36055726400) ;Radian, Serban (15770354700) ;Ribeiro-Oliveira, Antonio (16176083100) ;Schöfl, Christof (7004108255) ;Patel, Kashyap A. (57188657944) ;Hernández-Ramírez, Laura C. (55511259300)Korbonits, Márta (7004190977)Objective: Heterozygous germline loss-of-function variants in AIP are associated with young-onset growth hormone and/or prolactin-secreting pituitary tumours. However, the pathogenic role of the c.911G > A; p.(Arg304Gln) (R304Q) AIP variant has been controversial. Recent data from public exome/genome databases show this variant is not infrequent. The objective of this work was to reassess the pathogenicity of R304Q based on clinical, genomic, and functional assay data. Design: Data were collected on published R304Q pituitary neuroendocrine tumour cases and from International Familial Isolated Pituitary Adenoma Consortium R304Q cases (n = 38, R304Q cohort). Clinical features, population cohort frequency, computational analyses, prediction models, presence of loss-of-heterozygosity, and in vitro/in vivo functional studies were assessed and compared with data from pathogenic/likely pathogenic AIP variant patients (AIPmut cohort, n = 184). Results: Of 38 R304Q patients, 61% (23/38) had growth hormone excess, in contrast to 80% of AIPmut cohort (147/184, P < .001). R304Q cohort was older at disease onset and diagnosis than the AIPmut cohort (median [quartiles] onset: 25 y [16-35] vs 16 y [14-23], P < .001; median [quartiles] diagnosis: 36 y [24-44] vs 21 y [15-29], P < .001). R304Q is present in gnomADv2.1 (0.31%) and UK Biobank (0.16%), including three persons with homozygous R304Q. No loss-of-heterozygosity was detected in four R304Q pituitary neuroendocrine tumour samples. In silico predictions and experimental data were conflicting. Conclusions: Evidence suggests that R304Q is not pathogenic for pituitary neuroendocrine tumour. We recommend changing this variant classification to likely benign and do not recommend pre-symptomatic genetic testing of family members or follow-up of already identified unaffected individuals with the R304Q variant. © The Author(s) 2025. Published by Oxford University Press on behalf of European Society of Endocrinology. - Some of the metrics are blocked by yourconsent settings
Publication Sensitivity and specificity of the macimorelin test for diagnosis of AGHD(2021) ;Garcia, Jose M. (53873831800) ;Biller, Beverly M K. (7006404171) ;Korbonits, Márta (7004190977) ;Popovic, Vera (35451450900) ;Luger, Anton (35544522000) ;Strasburger, Christian J. (35402133700) ;Chanson, Philippe (56249200300) ;Swerdloff, Ronald (7102295009) ;Wang, Christina (57218503311) ;Fleming, Rosa Rosanna (24376444900) ;Cohen, Fredric (36883931900) ;Ammer, Nicola (57198428983) ;Mueller, Gilbert (57222369045) ;Kelepouris, Nicky (6505997049) ;Strobl, Frank (57220923037) ;Ostrow, Vlady (35332793500)Yuen, Kevin C J. (7202333713)Objective: The macimorelin test is approved for the diagnosis of adult growth hormone deficiency (AGHD) based on its efficacy vs the insulin tolerance test (ITT). Macimorelin has a significant advantage over ITT in avoiding hypoglycemia. Analyses were conducted to determine whether macimorelin performance is affected by age, BMI, or sex, and evaluate its performance vs ITT over a range of GH cutpoints. Design: Post hoc analyses of data from a previous randomized phase 3 study included participants aged 18–66 years with BMI <37 kg/m2 and high (Group A), intermediate (Group B), or low (Group C) likelihood for AGHD based on pituitary history, and matched controls (Group D). Methods: Probability of AGHD was estimated using unadjusted, age-adjusted, BMI-adjusted, and sex-adjusted logistic models. Area under the curve (AUC) of the estimated receiver operating characteristic (ROC) curve (range, 0–1; 1 = perfect) was compared for adjusted vs unadjusted models. Separate analyses evaluated agreement, sensitivity, and specificity for macimorelin and ITT using cutpoints of 2.8, 4.0, 5.1, and 6.5 ng/mL. Results: For participants in Group A (n = 41) and Group D (n = 29), unadjusted, age-adjusted, BMI-adjusted, and sex-adjusted models had ROC AUCs (95% CIs) of 0.9924 (0.9807–1), 0.9924 (0.9807–1), 0.9916 (0.9786–1), and 0.9950 (0.9861–1), respectively. Conclusions: Macimorelin performance was not meaningfully affected by age, BMI, or sex, indicating robustness for AGHD diagnosis. Of the 4 GH cutpoints evaluated, the cutpoint of 5.1 ng/mL provided maximal specificity (96%) and high sensitivity (92%) and was in good overall agreement with the ITT at the same cutpoint (87%). © 2021 The authors Published by Bioscientifica Ltd. - Some of the metrics are blocked by yourconsent settings
Publication Sensitivity and specificity of the macimorelin test for diagnosis of AGHD(2021) ;Garcia, Jose M. (53873831800) ;Biller, Beverly M K. (7006404171) ;Korbonits, Márta (7004190977) ;Popovic, Vera (35451450900) ;Luger, Anton (35544522000) ;Strasburger, Christian J. (35402133700) ;Chanson, Philippe (56249200300) ;Swerdloff, Ronald (7102295009) ;Wang, Christina (57218503311) ;Fleming, Rosa Rosanna (24376444900) ;Cohen, Fredric (36883931900) ;Ammer, Nicola (57198428983) ;Mueller, Gilbert (57222369045) ;Kelepouris, Nicky (6505997049) ;Strobl, Frank (57220923037) ;Ostrow, Vlady (35332793500)Yuen, Kevin C J. (7202333713)Objective: The macimorelin test is approved for the diagnosis of adult growth hormone deficiency (AGHD) based on its efficacy vs the insulin tolerance test (ITT). Macimorelin has a significant advantage over ITT in avoiding hypoglycemia. Analyses were conducted to determine whether macimorelin performance is affected by age, BMI, or sex, and evaluate its performance vs ITT over a range of GH cutpoints. Design: Post hoc analyses of data from a previous randomized phase 3 study included participants aged 18–66 years with BMI <37 kg/m2 and high (Group A), intermediate (Group B), or low (Group C) likelihood for AGHD based on pituitary history, and matched controls (Group D). Methods: Probability of AGHD was estimated using unadjusted, age-adjusted, BMI-adjusted, and sex-adjusted logistic models. Area under the curve (AUC) of the estimated receiver operating characteristic (ROC) curve (range, 0–1; 1 = perfect) was compared for adjusted vs unadjusted models. Separate analyses evaluated agreement, sensitivity, and specificity for macimorelin and ITT using cutpoints of 2.8, 4.0, 5.1, and 6.5 ng/mL. Results: For participants in Group A (n = 41) and Group D (n = 29), unadjusted, age-adjusted, BMI-adjusted, and sex-adjusted models had ROC AUCs (95% CIs) of 0.9924 (0.9807–1), 0.9924 (0.9807–1), 0.9916 (0.9786–1), and 0.9950 (0.9861–1), respectively. Conclusions: Macimorelin performance was not meaningfully affected by age, BMI, or sex, indicating robustness for AGHD diagnosis. Of the 4 GH cutpoints evaluated, the cutpoint of 5.1 ng/mL provided maximal specificity (96%) and high sensitivity (92%) and was in good overall agreement with the ITT at the same cutpoint (87%). © 2021 The authors Published by Bioscientifica Ltd.
