A First-in-Human Phase I Study of BXQ-350, a First-in-Class Sphingolipid Metabolism Regulator, in Patients with Advanced/Recurrent Solid Tumors or High-Grade Gliomas

Olivier Rixe; John L. Villano; Robert Wesolowski; Anne M. Noonan; Vinay K. Puduvalli; Trisha M. Wise-Draper; Richard Curry; Emrullah Yilmaz; Charlie Cruze; Besim Ogretmen; Gilles Tapolsky; Ray Takigiku

doi:10.1158/1078-0432.CCR-24-1721

A First-in-Human Phase I Study of BXQ-350, a First-in-Class Sphingolipid Metabolism Regulator, in Patients with Advanced/Recurrent Solid Tumors or High-Grade Gliomas

Olivier Rixe
, John L. Villano
, Robert Wesolowski
, Anne M. Noonan
, Vinay K. Puduvalli
, Trisha M. Wise-Draper
, Richard Curry
, Emrullah Yilmaz
, Charlie Cruze
, Besim Ogretmen
, Gilles Tapolsky
, Ray Takigiku

Producción científica: Article › revisión exhaustiva

4 Citas (Scopus)

Resumen

Purpose: BXQ-350, a nanovesicle formulation of saposin C, is an allosteric sphingolipid metabolism regulator that increases proapoptotic ceramide and decreases oncogenic sphingosine-1- phosphate levels. We conducted a first-in-human phase I study of BXQ-350. Patients and Methods: Adults (≥18 years old) with advanced/ recurrent, treatment-refractory solid tumors or high-grade gliomas received BXQ-350 intravenously in five dose cohorts (0.7- 2.4 mg/kg) in a 3+3 dose escalation and expansion design. The primary endpoints during dose escalation were dose-limiting toxicities and maximum tolerated dose; the primary objective in expansion parts was assessment of antitumor activity (RECIST v1.1/Response Assessment in Neuro-Oncology criteria). Results: Eighty-six patients were enrolled. Dose-limiting toxicities were not observed during dose escalation (n = 18), and a maximum tolerated dose was not identified. An additional 68 patients received the 2.4 mg/kg dose. Nine patients (10%) discontinued due to adverse events. The most common treatmentrelated adverse events were nausea (24%) and fatigue (23%). Eight patients had a progression-free survival of ≥6 months. Two of these achieved a partial response, and six had stable disease, among whom three had a reduction in ≥1 target lesion. Of those with progression-free survival of ≥6 months, seven remained on study for >12 months, five for >24 months, and after 7 years, two remained on study without disease progression. Conclusions: BXQ-350 was well-tolerated as monotherapy at doses up to 2.4 mg/kg. It provided some lasting clinical benefit in patients with recurrent solid malignancies across several tumor types, consistent with a decreased systemic sphingosine-1-phosphate/ ceramide metabolic rheostat. BXQ-350 warrants further clinical investigation alone and combined with standard of care for advanced solid tumors.

Idioma original	English
Páginas (desde-hasta)	5053-5060
Número de páginas	8
Publicación	Clinical Cancer Research
Volumen	30
N.º	22
DOI	https://doi.org/10.1158/1078-0432.CCR-24-1721
Estado	Published - nov 15 2024

Nota bibliográfica

Publisher Copyright:
© 2024 American Association for Cancer Research.

Financiación

We thank the patients and their families for making this trial possible and the investigators and clinical study teams who participated. We thank Drs Mike Gazda and Tariq Arshad for their editorial review and comments. Adam Gill, MRes (Rude Health Consulting Ltd.) provided medical writing and editorial support, which was funded by Bexion Pharmaceuticals, Inc. Research was supported in part by the Medical University of South Carolina's Lipidomics Shared Resource through funding of laboratory space for the Analytical Unit located in 505C Children's Research Institute: Hollings Cancer Center (P30 CA138313), the Lipidomics Shared Resource in the South Carolina Lipidomics and Pathobiology COBRE; Medical University of South Carolina Department of Biochemistry (P20 RR017677), and the National Center for Research Resources and Office of the Director of the NIH (C06 RR018823). Research was also supported by the NIH/NIC grant 5R44CA136017-06 to Bexion Pharmaceuticals, Inc. O. Rixe reports grants from Bexion Pharmaceuticals during the conduct of the study, as well as other support from Bexion Pharmaceuticals outside the submitted work. R. Wesolowski reports other support from Bexion Pharmaceuticals during the conduct of the study. A.M. Noonan reports personal fees from AstraZeneca, Taiho Oncology, Elevar Therapeutics, DAVA Oncology, and OncLive outside the submitted work, as well as a patent for PCT/US2022/011731 pending. V.K. Puduvalli reports other support from Bexion Pharmaceuticals during the conduct of the study, as well as personal fees from Bayer, Boehringer Ingelheim, Servier, Telix Pharma, Tango Pharmaceuticals, Insightec, Novocure, Orbus Therapeutics, and Med-IQ and nonfinancial support from Karyopharm outside the submitted work. R. Curry III reports other support from Bexion Pharmaceuticals outside the submitted work. E. Yilmaz reports personal fees from Astellas Pharma and Johnson & Johnson outside the submitted work. C. Cruze reports personal fees from Bexion Pharmaceuticals during the conduct of the study, as well as personal fees from Bexion Pharmaceuticals outside the submitted work; in addition, C. Cruze reports a patent for Bexion Pharmaceuticals pending. G. Tapolsky reports a patent for U.S. App. No. 18/260677 pending. R. Takigiku reports other support from Bexion Pharmaceuticals, Inc outside the submitted work, as well as a patent for US 10682411 issued, a patent for US 11590227 issued, a patent for WO2021111842A1 pending and issued, and a patent for WO2020228150A1 pending and issued. No disclosures were reported by the other authors. We thank the patients and their families for making this trial possible and the investigators and clinical study teams who participated. We thank Drs Mike Gazda and Tariq Arshad for their editorial review and comments. Adam Gill, MRes (Rude Health Consulting Ltd.) provided medical writing and editorial support, which was funded by Bexion Pharmaceuticals, Inc. Research was supported in part by the Medical University of South Carolina’s Lipidomics Shared Resource through funding of laboratory space for the Analytical Unit located in 505C Children’s Research Institute: Hollings Cancer Center (P30 CA138313), the Lipidomics Shared Resource in the South Carolina Lip-idomics and Pathobiology COBRE; Medical University of South Carolina Department of Biochemistry (P20 RR017677), and the National Center for Research Resources and Office of the Director of the NIH (C06 RR018823). Research was also supported by the NIH/NIC grant 5R44CA136017-06 to Bexion Pharmaceuticals, Inc.

Financiadores	Número del financiador
Medical University South Carolina
Drs Mike Gazda and Tariq Arshad
Alexion Pharmaceuticals
Rude Health Consulting Ltd.
Bexion Pharmaceuticals, Inc.
National Center for Research Resources and Office
Department of Public Health Sciences, Hollings Cancer Center, Medical University of South Carolina	P30 CA138313
Medical University of South Carolina Department of Biochemistry	P20 RR017677
National Institutes of Health (NIH)	C06 RR018823
National Institute of Corrections	5R44CA136017-06

ODS de las Naciones Unidas

Este resultado contribuye a los siguientes Objetivos de Desarrollo Sostenible

Good health and well being

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/1078-0432.CCR-24-1721

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Rixe, O., Villano, J. L., Wesolowski, R., Noonan, A. M., Puduvalli, V. K., Wise-Draper, T. M., Curry, R., Yilmaz, E., Cruze, C., Ogretmen, B., Tapolsky, G., & Takigiku, R. (2024). A First-in-Human Phase I Study of BXQ-350, a First-in-Class Sphingolipid Metabolism Regulator, in Patients with Advanced/Recurrent Solid Tumors or High-Grade Gliomas. Clinical Cancer Research, 30(22), 5053-5060. https://doi.org/10.1158/1078-0432.CCR-24-1721

@article{7d6e80245cb746b5b5c5517e797af47e,

title = "A First-in-Human Phase I Study of BXQ-350, a First-in-Class Sphingolipid Metabolism Regulator, in Patients with Advanced/Recurrent Solid Tumors or High-Grade Gliomas",

abstract = "Purpose: BXQ-350, a nanovesicle formulation of saposin C, is an allosteric sphingolipid metabolism regulator that increases proapoptotic ceramide and decreases oncogenic sphingosine-1- phosphate levels. We conducted a first-in-human phase I study of BXQ-350. Patients and Methods: Adults (≥18 years old) with advanced/ recurrent, treatment-refractory solid tumors or high-grade gliomas received BXQ-350 intravenously in five dose cohorts (0.7- 2.4 mg/kg) in a 3+3 dose escalation and expansion design. The primary endpoints during dose escalation were dose-limiting toxicities and maximum tolerated dose; the primary objective in expansion parts was assessment of antitumor activity (RECIST v1.1/Response Assessment in Neuro-Oncology criteria). Results: Eighty-six patients were enrolled. Dose-limiting toxicities were not observed during dose escalation (n = 18), and a maximum tolerated dose was not identified. An additional 68 patients received the 2.4 mg/kg dose. Nine patients (10\%) discontinued due to adverse events. The most common treatmentrelated adverse events were nausea (24\%) and fatigue (23\%). Eight patients had a progression-free survival of ≥6 months. Two of these achieved a partial response, and six had stable disease, among whom three had a reduction in ≥1 target lesion. Of those with progression-free survival of ≥6 months, seven remained on study for >12 months, five for >24 months, and after 7 years, two remained on study without disease progression. Conclusions: BXQ-350 was well-tolerated as monotherapy at doses up to 2.4 mg/kg. It provided some lasting clinical benefit in patients with recurrent solid malignancies across several tumor types, consistent with a decreased systemic sphingosine-1-phosphate/ ceramide metabolic rheostat. BXQ-350 warrants further clinical investigation alone and combined with standard of care for advanced solid tumors.",

author = "Olivier Rixe and Villano, \{John L.\} and Robert Wesolowski and Noonan, \{Anne M.\} and Puduvalli, \{Vinay K.\} and Wise-Draper, \{Trisha M.\} and Richard Curry and Emrullah Yilmaz and Charlie Cruze and Besim Ogretmen and Gilles Tapolsky and Ray Takigiku",

note = "Publisher Copyright: {\textcopyright} 2024 American Association for Cancer Research.",

year = "2024",

month = nov,

day = "15",

doi = "10.1158/1078-0432.CCR-24-1721",

language = "English",

volume = "30",

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Rixe, O, Villano, JL, Wesolowski, R, Noonan, AM, Puduvalli, VK, Wise-Draper, TM, Curry, R, Yilmaz, E, Cruze, C, Ogretmen, B, Tapolsky, G & Takigiku, R 2024, 'A First-in-Human Phase I Study of BXQ-350, a First-in-Class Sphingolipid Metabolism Regulator, in Patients with Advanced/Recurrent Solid Tumors or High-Grade Gliomas', Clinical Cancer Research, vol. 30, n.º 22, pp. 5053-5060. https://doi.org/10.1158/1078-0432.CCR-24-1721

TY - JOUR

T1 - A First-in-Human Phase I Study of BXQ-350, a First-in-Class Sphingolipid Metabolism Regulator, in Patients with Advanced/Recurrent Solid Tumors or High-Grade Gliomas

AU - Rixe, Olivier

AU - Villano, John L.

AU - Wesolowski, Robert

AU - Noonan, Anne M.

AU - Puduvalli, Vinay K.

AU - Wise-Draper, Trisha M.

AU - Curry, Richard

AU - Yilmaz, Emrullah

AU - Cruze, Charlie

AU - Ogretmen, Besim

AU - Tapolsky, Gilles

AU - Takigiku, Ray

PY - 2024/11/15

Y1 - 2024/11/15

N2 - Purpose: BXQ-350, a nanovesicle formulation of saposin C, is an allosteric sphingolipid metabolism regulator that increases proapoptotic ceramide and decreases oncogenic sphingosine-1- phosphate levels. We conducted a first-in-human phase I study of BXQ-350. Patients and Methods: Adults (≥18 years old) with advanced/ recurrent, treatment-refractory solid tumors or high-grade gliomas received BXQ-350 intravenously in five dose cohorts (0.7- 2.4 mg/kg) in a 3+3 dose escalation and expansion design. The primary endpoints during dose escalation were dose-limiting toxicities and maximum tolerated dose; the primary objective in expansion parts was assessment of antitumor activity (RECIST v1.1/Response Assessment in Neuro-Oncology criteria). Results: Eighty-six patients were enrolled. Dose-limiting toxicities were not observed during dose escalation (n = 18), and a maximum tolerated dose was not identified. An additional 68 patients received the 2.4 mg/kg dose. Nine patients (10%) discontinued due to adverse events. The most common treatmentrelated adverse events were nausea (24%) and fatigue (23%). Eight patients had a progression-free survival of ≥6 months. Two of these achieved a partial response, and six had stable disease, among whom three had a reduction in ≥1 target lesion. Of those with progression-free survival of ≥6 months, seven remained on study for >12 months, five for >24 months, and after 7 years, two remained on study without disease progression. Conclusions: BXQ-350 was well-tolerated as monotherapy at doses up to 2.4 mg/kg. It provided some lasting clinical benefit in patients with recurrent solid malignancies across several tumor types, consistent with a decreased systemic sphingosine-1-phosphate/ ceramide metabolic rheostat. BXQ-350 warrants further clinical investigation alone and combined with standard of care for advanced solid tumors.

AB - Purpose: BXQ-350, a nanovesicle formulation of saposin C, is an allosteric sphingolipid metabolism regulator that increases proapoptotic ceramide and decreases oncogenic sphingosine-1- phosphate levels. We conducted a first-in-human phase I study of BXQ-350. Patients and Methods: Adults (≥18 years old) with advanced/ recurrent, treatment-refractory solid tumors or high-grade gliomas received BXQ-350 intravenously in five dose cohorts (0.7- 2.4 mg/kg) in a 3+3 dose escalation and expansion design. The primary endpoints during dose escalation were dose-limiting toxicities and maximum tolerated dose; the primary objective in expansion parts was assessment of antitumor activity (RECIST v1.1/Response Assessment in Neuro-Oncology criteria). Results: Eighty-six patients were enrolled. Dose-limiting toxicities were not observed during dose escalation (n = 18), and a maximum tolerated dose was not identified. An additional 68 patients received the 2.4 mg/kg dose. Nine patients (10%) discontinued due to adverse events. The most common treatmentrelated adverse events were nausea (24%) and fatigue (23%). Eight patients had a progression-free survival of ≥6 months. Two of these achieved a partial response, and six had stable disease, among whom three had a reduction in ≥1 target lesion. Of those with progression-free survival of ≥6 months, seven remained on study for >12 months, five for >24 months, and after 7 years, two remained on study without disease progression. Conclusions: BXQ-350 was well-tolerated as monotherapy at doses up to 2.4 mg/kg. It provided some lasting clinical benefit in patients with recurrent solid malignancies across several tumor types, consistent with a decreased systemic sphingosine-1-phosphate/ ceramide metabolic rheostat. BXQ-350 warrants further clinical investigation alone and combined with standard of care for advanced solid tumors.

UR - https://www.scopus.com/pages/publications/85209827879

UR - https://www.scopus.com/pages/publications/85209827879#tab=citedBy

U2 - 10.1158/1078-0432.CCR-24-1721

DO - 10.1158/1078-0432.CCR-24-1721

M3 - Article

C2 - 39264252

AN - SCOPUS:85209827879

SN - 1078-0432

VL - 30

SP - 5053

EP - 5060

JO - Clinical Cancer Research

JF - Clinical Cancer Research

IS - 22

ER -

A First-in-Human Phase I Study of BXQ-350, a First-in-Class Sphingolipid Metabolism Regulator, in Patients with Advanced/Recurrent Solid Tumors or High-Grade Gliomas

Resumen

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Financiación

ODS de las Naciones Unidas

ASJC Scopus subject areas

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