11β-HSD1 inhibition in men mitigates prednisolone-induced adverse effects in a proof-of-concept randomised double-blind placebo-controlled trial

Nantia Othonos; Riccardo Pofi; Anastasia Arvaniti; Sarah White; Ilaria Bonaventura; Nikolaos Nikolaou; Ahmad Moolla; Thomas Marjot; Roland H. Stimson; André P. van Beek; Martijn van Faassen; Andrea M. Isidori; Elizabeth Bateman; Ross Sadler; Fredrik Karpe; Paul M. Stewart; Craig Webster; Joanne Duffy; Richard Eastell; Fatma Gossiel; Thomas Cornfield; Leanne Hodson; K. Jane Escott; Andrew Whittaker; Ufuk Kirik; Ruth L. Coleman; Charles A.B. Scott; Joanne E. Milton; Olorunsola Agbaje; Rury R. Holman; Jeremy W. Tomlinson

doi:10.1038/s41467-023-36541-w

11β-HSD1 inhibition in men mitigates prednisolone-induced adverse effects in a proof-of-concept randomised double-blind placebo-controlled trial

Nantia Othonos
, Riccardo Pofi
, Anastasia Arvaniti
, Sarah White
, Ilaria Bonaventura
, Nikolaos Nikolaou
, Ahmad Moolla
, Thomas Marjot
, Roland H. Stimson
, André P. van Beek
, Martijn van Faassen
, Andrea M. Isidori
, Elizabeth Bateman
, Ross Sadler
, Fredrik Karpe
, Paul M. Stewart
, Craig Webster
, Joanne Duffy
, Richard Eastell
, Fatma Gossiel

Thomas Cornfield, Leanne Hodson, K. Jane Escott, Andrew Whittaker, Ufuk Kirik, Ruth L. Coleman, Charles A.B. Scott, Joanne E. Milton, Olorunsola Agbaje, Rury R. Holman, Jeremy W. Tomlinson^*

^*Corresponding author voor dit werk

Onderzoeksoutput › Academic › peer review

33 Citaten (Scopus)

170 Downloads (Pure)

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Glucocorticoids prescribed to limit inflammation, have significant adverse effects. As 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) regenerates active glucocorticoid, we investigated whether 11β-HSD1 inhibition with AZD4017 could mitigate adverse glucocorticoid effects without compromising their anti-inflammatory actions. We conducted a proof-of-concept, randomized, double-blind, placebo-controlled study at Research Unit, Churchill Hospital, Oxford, UK (NCT03111810). 32 healthy male volunteers were randomized to AZD4017 or placebo, alongside prednisolone treatment. Although the primary endpoint of the study (change in glucose disposal during a two-step hyperinsulinemic, normoglycemic clamp) wasn’t met, hepatic insulin sensitivity worsened in the placebo-treated but not in the AZD4017-treated group. Protective effects of AZD4017 on markers of lipid metabolism and bone turnover were observed. Night-time blood pressure was higher in the placebo-treated but not in the AZD4017-treated group. Urinary (5aTHF+THF)/THE ratio was lower in the AZD4017-treated but remained the same in the placebo-treated group. Most anti-inflammatory actions of prednisolone persisted with AZD4017 co-treatment. Four adverse events were reported with AZD4017 and no serious adverse events. Here we show that co-administration of AZD4017 with prednisolone in men is a potential strategy to limit adverse glucocorticoid effects.

Originele taal-2	English
Artikelnummer	1025
Aantal pagina's	12
Tijdschrift	Nature Communications
Volume	14
Nummer van het tijdschrift	1
DOI's	https://doi.org/10.1038/s41467-023-36541-w
Status	Published - feb.-2023

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10.1038/s41467-023-36541-wLicentie: CC BY

11β-HSD1 inhibition in men mitigates prednisolone-induced adverse effects in a proof-of-concept randomised double-blind placebo-controlled trialFinal publisher's version, 2,24 MBLicentie: CC BY

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Othonos, N., Pofi, R., Arvaniti, A., White, S., Bonaventura, I., Nikolaou, N., Moolla, A., Marjot, T., Stimson, R. H., van Beek, A. P., van Faassen, M., Isidori, A. M., Bateman, E., Sadler, R., Karpe, F., Stewart, P. M., Webster, C., Duffy, J., Eastell, R., ... Tomlinson, J. W. (2023). 11β-HSD1 inhibition in men mitigates prednisolone-induced adverse effects in a proof-of-concept randomised double-blind placebo-controlled trial. Nature Communications, 14(1), Artikel 1025. https://doi.org/10.1038/s41467-023-36541-w

@article{7bd460d351ac4abfa347452ef427f583,

title = "11β-HSD1 inhibition in men mitigates prednisolone-induced adverse effects in a proof-of-concept randomised double-blind placebo-controlled trial",

abstract = "Glucocorticoids prescribed to limit inflammation, have significant adverse effects. As 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) regenerates active glucocorticoid, we investigated whether 11β-HSD1 inhibition with AZD4017 could mitigate adverse glucocorticoid effects without compromising their anti-inflammatory actions. We conducted a proof-of-concept, randomized, double-blind, placebo-controlled study at Research Unit, Churchill Hospital, Oxford, UK (NCT03111810). 32 healthy male volunteers were randomized to AZD4017 or placebo, alongside prednisolone treatment. Although the primary endpoint of the study (change in glucose disposal during a two-step hyperinsulinemic, normoglycemic clamp) wasn{\textquoteright}t met, hepatic insulin sensitivity worsened in the placebo-treated but not in the AZD4017-treated group. Protective effects of AZD4017 on markers of lipid metabolism and bone turnover were observed. Night-time blood pressure was higher in the placebo-treated but not in the AZD4017-treated group. Urinary (5aTHF+THF)/THE ratio was lower in the AZD4017-treated but remained the same in the placebo-treated group. Most anti-inflammatory actions of prednisolone persisted with AZD4017 co-treatment. Four adverse events were reported with AZD4017 and no serious adverse events. Here we show that co-administration of AZD4017 with prednisolone in men is a potential strategy to limit adverse glucocorticoid effects.",

author = "Nantia Othonos and Riccardo Pofi and Anastasia Arvaniti and Sarah White and Ilaria Bonaventura and Nikolaos Nikolaou and Ahmad Moolla and Thomas Marjot and Stimson, \{Roland H.\} and \{van Beek\}, \{Andr{\'e} P.\} and \{van Faassen\}, Martijn and Isidori, \{Andrea M.\} and Elizabeth Bateman and Ross Sadler and Fredrik Karpe and Stewart, \{Paul M.\} and Craig Webster and Joanne Duffy and Richard Eastell and Fatma Gossiel and Thomas Cornfield and Leanne Hodson and \{Jane Escott\}, K. and Andrew Whittaker and Ufuk Kirik and Coleman, \{Ruth L.\} and Scott, \{Charles A.B.\} and Milton, \{Joanne E.\} and Olorunsola Agbaje and Holman, \{Rury R.\} and Tomlinson, \{Jeremy W.\}",

note = "Funding Information: The work was supported by the Medical Research Council (industry asset sharing initiative grant to J.W.T. ref. MR/N024591/1); NIHR Oxford Biomedical Research Centre (principal investigator award to J.W.T.); British Heart Foundation (senior fellowship to L.H. ref. FS/15/56/31645); University of Oxford/Novo Nordisk (Clinical research training fellowship awarded to A.M.). Exchange in Endocrinology Expertise Programme of the European Union of Medical Specialists (3E Fellowship awarded to R.P.), European Society of Endocrinology (short-term fellowship awarded to R.P.). R.H.S. is supported by the CSO. R.R.H. is an Emeritus NIHR Senior Investigator. The views expressed are those of the author(s) and not necessarily those of the NHS, the NIHR or the Department of Health. Funding Information: The work was supported by the Medical Research Council (industry asset sharing initiative grant to J.W.T. ref. MR/N024591/1); NIHR Oxford Biomedical Research Centre (principal investigator award to J.W.T.); British Heart Foundation (senior fellowship to L.H. ref. FS/15/56/31645); University of Oxford/Novo Nordisk (Clinical research training fellowship awarded to A.M.). Exchange in Endocrinology Expertise Programme of the European Union of Medical Specialists (3E Fellowship awarded to R.P.), European Society of Endocrinology (short-term fellowship awarded to R.P.). R.H.S. is supported by the CSO. R.R.H. is an Emeritus NIHR Senior Investigator. The views expressed are those of the author(s) and not necessarily those of the NHS, the NIHR or the Department of Health. Funding Information: J.W.T. has been an advisory board member for Lumos, Pfizer AstraZeneca and Poxel. R.R.H. reports research support from AstraZeneca, Bayer and Merck Sharp \& Dohme, and personal fees from Anji Pharmaceuticals, Novartis and Novo Nordisk. A.M.I. received consultation fees, unconditional grants and hospitality to conferences from IBSA, Takeda and IPSEN. R.E. receives consultancy funding from Immunodiagnostic Systems, Sandoz, Samsung, Haoma Medica, CL Bio, Biocon, Coherus, Takeda, meeting presentations for Pharmacosmos, Alexion and Amgen, and grant funding from Roche, Pharmacosmos and Alexion. A.W., K.J.E. and U.K. are full-time employees of AstraZeneca. The work has been supported by the NIHR Oxford Biomedical Research Centre. The remaining authors declare no other competing interests. Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = feb,

doi = "10.1038/s41467-023-36541-w",

language = "English",

volume = "14",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Publishing Group",

number = "1",

}

Othonos, N, Pofi, R, Arvaniti, A, White, S, Bonaventura, I, Nikolaou, N, Moolla, A, Marjot, T, Stimson, RH, van Beek, AP , van Faassen, M, Isidori, AM, Bateman, E, Sadler, R, Karpe, F, Stewart, PM, Webster, C, Duffy, J, Eastell, R, Gossiel, F, Cornfield, T, Hodson, L, Jane Escott, K, Whittaker, A, Kirik, U, Coleman, RL, Scott, CAB, Milton, JE, Agbaje, O, Holman, RR & Tomlinson, JW 2023, '11β-HSD1 inhibition in men mitigates prednisolone-induced adverse effects in a proof-of-concept randomised double-blind placebo-controlled trial', Nature Communications, vol. 14, nr. 1, 1025. https://doi.org/10.1038/s41467-023-36541-w

TY - JOUR

T1 - 11β-HSD1 inhibition in men mitigates prednisolone-induced adverse effects in a proof-of-concept randomised double-blind placebo-controlled trial

AU - Othonos, Nantia

AU - Pofi, Riccardo

AU - Arvaniti, Anastasia

AU - White, Sarah

AU - Bonaventura, Ilaria

AU - Nikolaou, Nikolaos

AU - Moolla, Ahmad

AU - Marjot, Thomas

AU - Stimson, Roland H.

AU - van Beek, André P.

AU - van Faassen, Martijn

AU - Isidori, Andrea M.

AU - Bateman, Elizabeth

AU - Sadler, Ross

AU - Karpe, Fredrik

AU - Stewart, Paul M.

AU - Webster, Craig

AU - Duffy, Joanne

AU - Eastell, Richard

AU - Gossiel, Fatma

AU - Cornfield, Thomas

AU - Hodson, Leanne

AU - Jane Escott, K.

AU - Whittaker, Andrew

AU - Kirik, Ufuk

AU - Coleman, Ruth L.

AU - Scott, Charles A.B.

AU - Milton, Joanne E.

AU - Agbaje, Olorunsola

AU - Holman, Rury R.

AU - Tomlinson, Jeremy W.

N1 - Funding Information: The work was supported by the Medical Research Council (industry asset sharing initiative grant to J.W.T. ref. MR/N024591/1); NIHR Oxford Biomedical Research Centre (principal investigator award to J.W.T.); British Heart Foundation (senior fellowship to L.H. ref. FS/15/56/31645); University of Oxford/Novo Nordisk (Clinical research training fellowship awarded to A.M.). Exchange in Endocrinology Expertise Programme of the European Union of Medical Specialists (3E Fellowship awarded to R.P.), European Society of Endocrinology (short-term fellowship awarded to R.P.). R.H.S. is supported by the CSO. R.R.H. is an Emeritus NIHR Senior Investigator. The views expressed are those of the author(s) and not necessarily those of the NHS, the NIHR or the Department of Health. Funding Information: The work was supported by the Medical Research Council (industry asset sharing initiative grant to J.W.T. ref. MR/N024591/1); NIHR Oxford Biomedical Research Centre (principal investigator award to J.W.T.); British Heart Foundation (senior fellowship to L.H. ref. FS/15/56/31645); University of Oxford/Novo Nordisk (Clinical research training fellowship awarded to A.M.). Exchange in Endocrinology Expertise Programme of the European Union of Medical Specialists (3E Fellowship awarded to R.P.), European Society of Endocrinology (short-term fellowship awarded to R.P.). R.H.S. is supported by the CSO. R.R.H. is an Emeritus NIHR Senior Investigator. The views expressed are those of the author(s) and not necessarily those of the NHS, the NIHR or the Department of Health. Funding Information: J.W.T. has been an advisory board member for Lumos, Pfizer AstraZeneca and Poxel. R.R.H. reports research support from AstraZeneca, Bayer and Merck Sharp & Dohme, and personal fees from Anji Pharmaceuticals, Novartis and Novo Nordisk. A.M.I. received consultation fees, unconditional grants and hospitality to conferences from IBSA, Takeda and IPSEN. R.E. receives consultancy funding from Immunodiagnostic Systems, Sandoz, Samsung, Haoma Medica, CL Bio, Biocon, Coherus, Takeda, meeting presentations for Pharmacosmos, Alexion and Amgen, and grant funding from Roche, Pharmacosmos and Alexion. A.W., K.J.E. and U.K. are full-time employees of AstraZeneca. The work has been supported by the NIHR Oxford Biomedical Research Centre. The remaining authors declare no other competing interests. Publisher Copyright: © 2023, The Author(s).

PY - 2023/2

Y1 - 2023/2

N2 - Glucocorticoids prescribed to limit inflammation, have significant adverse effects. As 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) regenerates active glucocorticoid, we investigated whether 11β-HSD1 inhibition with AZD4017 could mitigate adverse glucocorticoid effects without compromising their anti-inflammatory actions. We conducted a proof-of-concept, randomized, double-blind, placebo-controlled study at Research Unit, Churchill Hospital, Oxford, UK (NCT03111810). 32 healthy male volunteers were randomized to AZD4017 or placebo, alongside prednisolone treatment. Although the primary endpoint of the study (change in glucose disposal during a two-step hyperinsulinemic, normoglycemic clamp) wasn’t met, hepatic insulin sensitivity worsened in the placebo-treated but not in the AZD4017-treated group. Protective effects of AZD4017 on markers of lipid metabolism and bone turnover were observed. Night-time blood pressure was higher in the placebo-treated but not in the AZD4017-treated group. Urinary (5aTHF+THF)/THE ratio was lower in the AZD4017-treated but remained the same in the placebo-treated group. Most anti-inflammatory actions of prednisolone persisted with AZD4017 co-treatment. Four adverse events were reported with AZD4017 and no serious adverse events. Here we show that co-administration of AZD4017 with prednisolone in men is a potential strategy to limit adverse glucocorticoid effects.

AB - Glucocorticoids prescribed to limit inflammation, have significant adverse effects. As 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) regenerates active glucocorticoid, we investigated whether 11β-HSD1 inhibition with AZD4017 could mitigate adverse glucocorticoid effects without compromising their anti-inflammatory actions. We conducted a proof-of-concept, randomized, double-blind, placebo-controlled study at Research Unit, Churchill Hospital, Oxford, UK (NCT03111810). 32 healthy male volunteers were randomized to AZD4017 or placebo, alongside prednisolone treatment. Although the primary endpoint of the study (change in glucose disposal during a two-step hyperinsulinemic, normoglycemic clamp) wasn’t met, hepatic insulin sensitivity worsened in the placebo-treated but not in the AZD4017-treated group. Protective effects of AZD4017 on markers of lipid metabolism and bone turnover were observed. Night-time blood pressure was higher in the placebo-treated but not in the AZD4017-treated group. Urinary (5aTHF+THF)/THE ratio was lower in the AZD4017-treated but remained the same in the placebo-treated group. Most anti-inflammatory actions of prednisolone persisted with AZD4017 co-treatment. Four adverse events were reported with AZD4017 and no serious adverse events. Here we show that co-administration of AZD4017 with prednisolone in men is a potential strategy to limit adverse glucocorticoid effects.

U2 - 10.1038/s41467-023-36541-w

DO - 10.1038/s41467-023-36541-w

M3 - Article

C2 - 36823106

AN - SCOPUS:85148830348

SN - 2041-1723

VL - 14

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 1025

ER -

11β-HSD1 inhibition in men mitigates prednisolone-induced adverse effects in a proof-of-concept randomised double-blind placebo-controlled trial

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