Dichotomous Nitric Oxide–Dependent Post-Translational Modifications of STAT1 Are Associated with Ipilimumab Benefits in Melanoma

SIMPLE SUMMARY: Nitric oxide is typically thought of as an inhibitory molecule in cancer. In our previous studies, nitric oxide (NO) increased in the immune effector cells among patients with longer RFS after adjuvant ipilimumab, whereas NO increased in the immune suppressor cells among patients wit...

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Autores principales: Garg, Saurabh K., Sun, James, Kim, Youngchul, Whiting, Junmin, Sarnaik, Amod, Conejo-Garcia, José R., Phelps, Mitch, Weber, Jeffrey S., Mulé, James J., Markowitz, Joseph
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10046641/
https://www.ncbi.nlm.nih.gov/pubmed/36980641
http://dx.doi.org/10.3390/cancers15061755
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author Garg, Saurabh K.
Sun, James
Kim, Youngchul
Whiting, Junmin
Sarnaik, Amod
Conejo-Garcia, José R.
Phelps, Mitch
Weber, Jeffrey S.
Mulé, James J.
Markowitz, Joseph
author_facet Garg, Saurabh K.
Sun, James
Kim, Youngchul
Whiting, Junmin
Sarnaik, Amod
Conejo-Garcia, José R.
Phelps, Mitch
Weber, Jeffrey S.
Mulé, James J.
Markowitz, Joseph
author_sort Garg, Saurabh K.
collection PubMed
description SIMPLE SUMMARY: Nitric oxide is typically thought of as an inhibitory molecule in cancer. In our previous studies, nitric oxide (NO) increased in the immune effector cells among patients with longer RFS after adjuvant ipilimumab, whereas NO increased in the immune suppressor cells among patients with shorter RFS. Herein, we utilize samples derived from the same patients to measure the post-translational modifications of STAT1 (nitration-nSTAT1 and phosphorylation-pSTAT1) important for regulating its activity via flow cytometry and mass spectrometry approaches. Ipilimumab-treated patients with high nSTAT1 levels before and after therapy in PBMCs experienced decreased RFS, but the change in nSTAT1 levels before and after ipilimumab therapy was associated with longer RFS. This study reveals a dichotomous role for nitric oxide in melanoma and may lead to therapeutic implications. ABSTRACT: Although Ipilimumab (anti-CTLA-4) is FDA-approved for stage III/IV melanoma adjuvant treatment, it is not used clinically in first-line therapy, given the superior relapse-free survival (RFS)/toxicity benefits of anti-PD-1 therapy. However, it is important to understand anti-CTLA-4’s mechanistic contribution to combination anti-PD-1/CTLA-4 therapy and investigate anti-CTLA-4 therapy for BRAF-wild type melanoma cases reresected after previous adjuvant anti-PD-1 therapy. Our group published that nitric oxide (NO) increased within the immune effector cells among patients with longer RFS after adjuvant ipilimumab, whereas NO increased within the immune suppressor cells among patients with shorter RFS. Herein, we measured the post-translational modifications of STAT1 (nitration-nSTAT1 and phosphorylation-pSTAT1) that are important for regulating its activity via flow cytometry and mass spectrometry approaches. PBMCs were analyzed from 35 patients undergoing adjuvant ipilimumab treatment. Shorter RFS was associated with higher pSTAT1 levels before (p = 0.007) and after (p = 0.036) ipilimumab. Ipilimumab-treated patients with high nSTAT1 levels before and after therapy in PBMCs experienced decreased RFS, but the change in nSTAT1 levels before and after ipilimumab therapy was associated with longer RFS (p = 0.01). The measurement of post-translational modifications in STAT1 may distinguish patients with prolonged RFS from ipilimumab and provide mechanistic insight into responses to ipilimumab combination regimens.
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spelling pubmed-100466412023-03-29 Dichotomous Nitric Oxide–Dependent Post-Translational Modifications of STAT1 Are Associated with Ipilimumab Benefits in Melanoma Garg, Saurabh K. Sun, James Kim, Youngchul Whiting, Junmin Sarnaik, Amod Conejo-Garcia, José R. Phelps, Mitch Weber, Jeffrey S. Mulé, James J. Markowitz, Joseph Cancers (Basel) Article SIMPLE SUMMARY: Nitric oxide is typically thought of as an inhibitory molecule in cancer. In our previous studies, nitric oxide (NO) increased in the immune effector cells among patients with longer RFS after adjuvant ipilimumab, whereas NO increased in the immune suppressor cells among patients with shorter RFS. Herein, we utilize samples derived from the same patients to measure the post-translational modifications of STAT1 (nitration-nSTAT1 and phosphorylation-pSTAT1) important for regulating its activity via flow cytometry and mass spectrometry approaches. Ipilimumab-treated patients with high nSTAT1 levels before and after therapy in PBMCs experienced decreased RFS, but the change in nSTAT1 levels before and after ipilimumab therapy was associated with longer RFS. This study reveals a dichotomous role for nitric oxide in melanoma and may lead to therapeutic implications. ABSTRACT: Although Ipilimumab (anti-CTLA-4) is FDA-approved for stage III/IV melanoma adjuvant treatment, it is not used clinically in first-line therapy, given the superior relapse-free survival (RFS)/toxicity benefits of anti-PD-1 therapy. However, it is important to understand anti-CTLA-4’s mechanistic contribution to combination anti-PD-1/CTLA-4 therapy and investigate anti-CTLA-4 therapy for BRAF-wild type melanoma cases reresected after previous adjuvant anti-PD-1 therapy. Our group published that nitric oxide (NO) increased within the immune effector cells among patients with longer RFS after adjuvant ipilimumab, whereas NO increased within the immune suppressor cells among patients with shorter RFS. Herein, we measured the post-translational modifications of STAT1 (nitration-nSTAT1 and phosphorylation-pSTAT1) that are important for regulating its activity via flow cytometry and mass spectrometry approaches. PBMCs were analyzed from 35 patients undergoing adjuvant ipilimumab treatment. Shorter RFS was associated with higher pSTAT1 levels before (p = 0.007) and after (p = 0.036) ipilimumab. Ipilimumab-treated patients with high nSTAT1 levels before and after therapy in PBMCs experienced decreased RFS, but the change in nSTAT1 levels before and after ipilimumab therapy was associated with longer RFS (p = 0.01). The measurement of post-translational modifications in STAT1 may distinguish patients with prolonged RFS from ipilimumab and provide mechanistic insight into responses to ipilimumab combination regimens. MDPI 2023-03-14 /pmc/articles/PMC10046641/ /pubmed/36980641 http://dx.doi.org/10.3390/cancers15061755 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Garg, Saurabh K.
Sun, James
Kim, Youngchul
Whiting, Junmin
Sarnaik, Amod
Conejo-Garcia, José R.
Phelps, Mitch
Weber, Jeffrey S.
Mulé, James J.
Markowitz, Joseph
Dichotomous Nitric Oxide–Dependent Post-Translational Modifications of STAT1 Are Associated with Ipilimumab Benefits in Melanoma
title Dichotomous Nitric Oxide–Dependent Post-Translational Modifications of STAT1 Are Associated with Ipilimumab Benefits in Melanoma
title_full Dichotomous Nitric Oxide–Dependent Post-Translational Modifications of STAT1 Are Associated with Ipilimumab Benefits in Melanoma
title_fullStr Dichotomous Nitric Oxide–Dependent Post-Translational Modifications of STAT1 Are Associated with Ipilimumab Benefits in Melanoma
title_full_unstemmed Dichotomous Nitric Oxide–Dependent Post-Translational Modifications of STAT1 Are Associated with Ipilimumab Benefits in Melanoma
title_short Dichotomous Nitric Oxide–Dependent Post-Translational Modifications of STAT1 Are Associated with Ipilimumab Benefits in Melanoma
title_sort dichotomous nitric oxide–dependent post-translational modifications of stat1 are associated with ipilimumab benefits in melanoma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10046641/
https://www.ncbi.nlm.nih.gov/pubmed/36980641
http://dx.doi.org/10.3390/cancers15061755
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