Pharmacodynamic Study of Miransertib in Individuals with Proteus Syndrome

Kim M. Keppler-Noreuil; Julie C. Sapp; Marjorie J. Lindhurst; Thomas N. Darling; Jasmine Burton-Akright; Mohammadhadi Bagheri; Eva Dombi; Ashlyn Gruber; Paul F. Jarosinski; Staci Martin; Neera Nathan; Scott M. Paul; Ronald E. Savage; Pamela L. Wolters; Brian Schwartz; Brigitte C. Widemann; Leslie G. Biesecker

doi:10.1016/j.ajhg.2019.01.015

Pharmacodynamic Study of Miransertib in Individuals with Proteus Syndrome

Kim M. Keppler-Noreuil, Julie C. Sapp, Marjorie J. Lindhurst, Thomas N. Darling, Jasmine Burton-Akright, Mohammadhadi Bagheri, Eva Dombi, Ashlyn Gruber, Paul F. Jarosinski, Staci Martin, Neera Nathan, Scott M. Paul, Ronald E. Savage, Pamela L. Wolters, Brian Schwartz, Brigitte C. Widemann, Leslie G. Biesecker^*

^*Corresponding author for this work

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

67 Scopus citations

Abstract

Proteus syndrome is a life-threatening segmental overgrowth syndrome caused by a mosaic gain-of-function AKT1 variant. There are no effective treatments for Proteus syndrome. Miransertib is an AKT1 inhibitor that, prior to this study, has been evaluated only in adult oncology trials. We designed a non-randomized, phase 0/1 pilot study of miransertib in adults and children with Proteus syndrome to identify an appropriate dosage starting point for a future efficacy trial using a pharmacodynamic endpoint. The primary endpoint was a 50% reduction in the tissue levels of AKT phosphorylation from biopsies in affected individuals. We also evaluated secondary efficacy endpoints. We found that a dose of 5 mg/m ² /day (1/7 the typical dose used in oncology) led to a 50% reduction in phosphorylated AKT (pAKT) in affected tissues from five of six individuals. This dose was well tolerated. Two of the six efficacy endpoints (secondary objectives) suggested that this agent may be efficacious. We observed a decrease in a cerebriform connective tissue nevus and a reduction in pain in children. We conclude that 5 mg/m ² /day of miransertib is an appropriate starting point for future efficacy trials and that this agent shows promise of therapeutic efficacy in children with Proteus syndrome.

Original language	English
Pages (from-to)	484-491
Number of pages	8
Journal	American Journal of Human Genetics
Volume	104
Issue number	3
DOIs	https://doi.org/10.1016/j.ajhg.2019.01.015
State	Published - 7 Mar 2019
Externally published	Yes

Keywords

connective tissue nevus
miransertib
mosaicism
overgrowth
phase I study
Proteus syndrome

Access to Document

10.1016/j.ajhg.2019.01.015

Cite this

Keppler-Noreuil, K. M., Sapp, J. C., Lindhurst, M. J., Darling, T. N., Burton-Akright, J., Bagheri, M., Dombi, E., Gruber, A., Jarosinski, P. F., Martin, S., Nathan, N., Paul, S. M., Savage, R. E., Wolters, P. L., Schwartz, B., Widemann, B. C., & Biesecker, L. G. (2019). Pharmacodynamic Study of Miransertib in Individuals with Proteus Syndrome. American Journal of Human Genetics, 104(3), 484-491. https://doi.org/10.1016/j.ajhg.2019.01.015

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title = "Pharmacodynamic Study of Miransertib in Individuals with Proteus Syndrome",

abstract = " Proteus syndrome is a life-threatening segmental overgrowth syndrome caused by a mosaic gain-of-function AKT1 variant. There are no effective treatments for Proteus syndrome. Miransertib is an AKT1 inhibitor that, prior to this study, has been evaluated only in adult oncology trials. We designed a non-randomized, phase 0/1 pilot study of miransertib in adults and children with Proteus syndrome to identify an appropriate dosage starting point for a future efficacy trial using a pharmacodynamic endpoint. The primary endpoint was a 50% reduction in the tissue levels of AKT phosphorylation from biopsies in affected individuals. We also evaluated secondary efficacy endpoints. We found that a dose of 5 mg/m 2 /day (1/7 the typical dose used in oncology) led to a 50% reduction in phosphorylated AKT (pAKT) in affected tissues from five of six individuals. This dose was well tolerated. Two of the six efficacy endpoints (secondary objectives) suggested that this agent may be efficacious. We observed a decrease in a cerebriform connective tissue nevus and a reduction in pain in children. We conclude that 5 mg/m 2 /day of miransertib is an appropriate starting point for future efficacy trials and that this agent shows promise of therapeutic efficacy in children with Proteus syndrome.",

keywords = "connective tissue nevus, miransertib, mosaicism, overgrowth, phase I study, Proteus syndrome",

author = "Keppler-Noreuil, {Kim M.} and Sapp, {Julie C.} and Lindhurst, {Marjorie J.} and Darling, {Thomas N.} and Jasmine Burton-Akright and Mohammadhadi Bagheri and Eva Dombi and Ashlyn Gruber and Jarosinski, {Paul F.} and Staci Martin and Neera Nathan and Paul, {Scott M.} and Savage, {Ronald E.} and Wolters, {Pamela L.} and Brian Schwartz and Widemann, {Brigitte C.} and Biesecker, {Leslie G.}",

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year = "2019",

month = mar,

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doi = "10.1016/j.ajhg.2019.01.015",

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Keppler-Noreuil, KM, Sapp, JC, Lindhurst, MJ, Darling, TN, Burton-Akright, J, Bagheri, M, Dombi, E, Gruber, A, Jarosinski, PF, Martin, S, Nathan, N, Paul, SM, Savage, RE, Wolters, PL, Schwartz, B, Widemann, BC & Biesecker, LG 2019, 'Pharmacodynamic Study of Miransertib in Individuals with Proteus Syndrome', American Journal of Human Genetics, vol. 104, no. 3, pp. 484-491. https://doi.org/10.1016/j.ajhg.2019.01.015

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T1 - Pharmacodynamic Study of Miransertib in Individuals with Proteus Syndrome

AU - Keppler-Noreuil, Kim M.

AU - Sapp, Julie C.

AU - Lindhurst, Marjorie J.

AU - Darling, Thomas N.

AU - Burton-Akright, Jasmine

AU - Bagheri, Mohammadhadi

AU - Dombi, Eva

AU - Gruber, Ashlyn

AU - Jarosinski, Paul F.

AU - Martin, Staci

AU - Nathan, Neera

AU - Paul, Scott M.

AU - Savage, Ronald E.

AU - Wolters, Pamela L.

AU - Schwartz, Brian

AU - Widemann, Brigitte C.

AU - Biesecker, Leslie G.

PY - 2019/3/7

Y1 - 2019/3/7

N2 - Proteus syndrome is a life-threatening segmental overgrowth syndrome caused by a mosaic gain-of-function AKT1 variant. There are no effective treatments for Proteus syndrome. Miransertib is an AKT1 inhibitor that, prior to this study, has been evaluated only in adult oncology trials. We designed a non-randomized, phase 0/1 pilot study of miransertib in adults and children with Proteus syndrome to identify an appropriate dosage starting point for a future efficacy trial using a pharmacodynamic endpoint. The primary endpoint was a 50% reduction in the tissue levels of AKT phosphorylation from biopsies in affected individuals. We also evaluated secondary efficacy endpoints. We found that a dose of 5 mg/m 2 /day (1/7 the typical dose used in oncology) led to a 50% reduction in phosphorylated AKT (pAKT) in affected tissues from five of six individuals. This dose was well tolerated. Two of the six efficacy endpoints (secondary objectives) suggested that this agent may be efficacious. We observed a decrease in a cerebriform connective tissue nevus and a reduction in pain in children. We conclude that 5 mg/m 2 /day of miransertib is an appropriate starting point for future efficacy trials and that this agent shows promise of therapeutic efficacy in children with Proteus syndrome.

AB - Proteus syndrome is a life-threatening segmental overgrowth syndrome caused by a mosaic gain-of-function AKT1 variant. There are no effective treatments for Proteus syndrome. Miransertib is an AKT1 inhibitor that, prior to this study, has been evaluated only in adult oncology trials. We designed a non-randomized, phase 0/1 pilot study of miransertib in adults and children with Proteus syndrome to identify an appropriate dosage starting point for a future efficacy trial using a pharmacodynamic endpoint. The primary endpoint was a 50% reduction in the tissue levels of AKT phosphorylation from biopsies in affected individuals. We also evaluated secondary efficacy endpoints. We found that a dose of 5 mg/m 2 /day (1/7 the typical dose used in oncology) led to a 50% reduction in phosphorylated AKT (pAKT) in affected tissues from five of six individuals. This dose was well tolerated. Two of the six efficacy endpoints (secondary objectives) suggested that this agent may be efficacious. We observed a decrease in a cerebriform connective tissue nevus and a reduction in pain in children. We conclude that 5 mg/m 2 /day of miransertib is an appropriate starting point for future efficacy trials and that this agent shows promise of therapeutic efficacy in children with Proteus syndrome.

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KW - miransertib

KW - mosaicism

KW - overgrowth

KW - phase I study

KW - Proteus syndrome

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DO - 10.1016/j.ajhg.2019.01.015

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