The deacylase SIRT5 supports melanoma viability by influencing chromatin dynamics

William Giblin; Lauren Bringman-Rodenbarger; Angela H Guo; Surinder Kumar; Alexander C Monovich; Ahmed M Mostafa; Mary E Skinner; Michelle Azar; Ahmed Sa Mady; Carolina H Chung; Namrata Kadambi; Keith-Allen Melong; Ho-Joon Lee; Li Zhang; Peter Sajjakulnukit; Sophie Trefely; Erika L Varner; Sowmya Iyer; Min Wang; James S Wilmott; H Peter Soyer; Richard A Sturm; Antonia L Pritchard; Aleodor A Andea; Richard A Scolyer; Mitchell S Stark; David A Scott; Douglas R Fullen; Marcus W Bosenberg; Sriram Chandrasekaran; Zaneta Nikolovska-Coleska; Monique E Verhaegen; Nathaniel W Snyder; Miguel N Rivera; Andrei Osterman; Costas A Lyssiotis; David B Lombard

doi:10.1172/JCI138926

The deacylase SIRT5 supports melanoma viability by influencing chromatin dynamics

William Giblin
, Lauren Bringman-Rodenbarger
, Angela H Guo
, Surinder Kumar
, Alexander C Monovich
, Ahmed M Mostafa
, Mary E Skinner
, Michelle Azar
, Ahmed Sa Mady
, Carolina H Chung
, Namrata Kadambi
, Keith-Allen Melong
, Ho-Joon Lee
, Li Zhang
, Peter Sajjakulnukit
, Sophie Trefely
, Erika L Varner
, Sowmya Iyer
, Min Wang
, James S Wilmott

H Peter Soyer, Richard A Sturm, Antonia L Pritchard, Aleodor A Andea, Richard A Scolyer, Mitchell S Stark, David A Scott, Douglas R Fullen, Marcus W Bosenberg, Sriram Chandrasekaran, Zaneta Nikolovska-Coleska, Monique E Verhaegen, Nathaniel W Snyder, Miguel N Rivera, Andrei Osterman, Costas A Lyssiotis, David B Lombard

نتاج البحث: Article › مراجعة النظراء

38 اقتباسات (Scopus)

100 التنزيلات (Pure)

ملخص

Cutaneous melanoma remains the most lethal skin cancer, and ranks third among all malignancies in terms of years of life lost. Despite the advent of immune checkpoint and targeted therapies, only roughly half of patients with advanced melanoma achieves a durable remission. SIRT5 is a member of the sirtuin family of protein deacylases that regulate metabolism and other biological processes. Germline Sirt5 deficiency is associated with mild phenotypes in mice. Here we show that SIRT5 is required for proliferation and survival across all cutaneous melanoma genotypes tested, as well as uveal melanoma, a genetically distinct melanoma subtype that arises in the eye and is incurable once metastatic. Likewise, SIRT5 is required for efficient tumor formation by melanoma xenografts and in an autochthonous mouse Braf;Pten-driven melanoma model. Via metabolite and transcriptomic analyses, we find that SIRT5 is required to maintain histone acetylation and methylation levels in melanoma cells, thereby promoting proper gene expression. SIRT5-dependent genes notably include MITF, a key lineage-specific survival oncogene in melanoma, and the c-MYC proto-oncogene. SIRT5 may represent a novel, druggable genotype-independent addiction in melanoma.

اللغة الأصلية	English
رقم المقال	e138926
الصفحات (من إلى)	1-18
عدد الصفحات	18
دورية	Journal of Clinical Investigation
مستوى الصوت	131
رقم الإصدار	12
تاريخ مبكر على الإنترنت	4 مايو 2021
المعرِّفات الرقمية للأشياء	https://doi.org/10.1172/JCI138926
حالة النشر	Published - 15 يونيو 2021

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10.1172/JCI138926الترخيص: CC BY

138926.1-20210503165220-covered-e0fd13ba177f913fd3156f593ead4cfd
Copyright: © 2021, American Society for Clinical Investigation.
Accepted author manuscript, ١٤٫٤ MBالترخيص: CC BY

قم بذكر هذا

Giblin, W., Bringman-Rodenbarger, L., Guo, A. H., Kumar, S., Monovich, A. C., Mostafa, A. M., Skinner, M. E., Azar, M., Mady, A. S., Chung, C. H., Kadambi, N., Melong, K.-A., Lee, H.-J., Zhang, L., Sajjakulnukit, P., Trefely, S., Varner, E. L., Iyer, S., Wang, M., ... Lombard, D. B. (2021). The deacylase SIRT5 supports melanoma viability by influencing chromatin dynamics. Journal of Clinical Investigation, 131(12), 1-18. المقال e138926. https://doi.org/10.1172/JCI138926

@article{5c0145356eb04b1b954af63bc4f2f5bb,

title = "The deacylase SIRT5 supports melanoma viability by influencing chromatin dynamics",

abstract = "Cutaneous melanoma remains the most lethal skin cancer, and ranks third among all malignancies in terms of years of life lost. Despite the advent of immune checkpoint and targeted therapies, only roughly half of patients with advanced melanoma achieves a durable remission. SIRT5 is a member of the sirtuin family of protein deacylases that regulate metabolism and other biological processes. Germline Sirt5 deficiency is associated with mild phenotypes in mice. Here we show that SIRT5 is required for proliferation and survival across all cutaneous melanoma genotypes tested, as well as uveal melanoma, a genetically distinct melanoma subtype that arises in the eye and is incurable once metastatic. Likewise, SIRT5 is required for efficient tumor formation by melanoma xenografts and in an autochthonous mouse Braf;Pten-driven melanoma model. Via metabolite and transcriptomic analyses, we find that SIRT5 is required to maintain histone acetylation and methylation levels in melanoma cells, thereby promoting proper gene expression. SIRT5-dependent genes notably include MITF, a key lineage-specific survival oncogene in melanoma, and the c-MYC proto-oncogene. SIRT5 may represent a novel, druggable genotype-independent addiction in melanoma.",

keywords = "Cell Biology, Metabolism",

author = "William Giblin and Lauren Bringman-Rodenbarger and Guo, \{Angela H\} and Surinder Kumar and Monovich, \{Alexander C\} and Mostafa, \{Ahmed M\} and Skinner, \{Mary E\} and Michelle Azar and Mady, \{Ahmed Sa\} and Chung, \{Carolina H\} and Namrata Kadambi and Keith-Allen Melong and Ho-Joon Lee and Li Zhang and Peter Sajjakulnukit and Sophie Trefely and Varner, \{Erika L\} and Sowmya Iyer and Min Wang and Wilmott, \{James S\} and Soyer, \{H Peter\} and Sturm, \{Richard A\} and Pritchard, \{Antonia L\} and Andea, \{Aleodor A\} and Scolyer, \{Richard A\} and Stark, \{Mitchell S\} and Scott, \{David A\} and Fullen, \{Douglas R\} and Bosenberg, \{Marcus W\} and Sriram Chandrasekaran and Zaneta Nikolovska-Coleska and Verhaegen, \{Monique E\} and Snyder, \{Nathaniel W\} and Rivera, \{Miguel N\} and Andrei Osterman and Lyssiotis, \{Costas A\} and Lombard, \{David B\}",

note = "Copyright: {\textcopyright} 2021, American Society for Clinical Investigation.",

year = "2021",

month = jun,

day = "15",

doi = "10.1172/JCI138926",

language = "English",

volume = "131",

pages = "1--18",

journal = "Journal of Clinical Investigation",

issn = "0021-9738",

publisher = "American Society for Clinical Investigation",

number = "12",

}

Giblin, W, Bringman-Rodenbarger, L, Guo, AH, Kumar, S, Monovich, AC, Mostafa, AM, Skinner, ME, Azar, M, Mady, AS, Chung, CH, Kadambi, N, Melong, K-A, Lee, H-J, Zhang, L, Sajjakulnukit, P, Trefely, S, Varner, EL, Iyer, S, Wang, M, Wilmott, JS, Soyer, HP, Sturm, RA, Pritchard, AL, Andea, AA, Scolyer, RA, Stark, MS, Scott, DA, Fullen, DR, Bosenberg, MW, Chandrasekaran, S, Nikolovska-Coleska, Z, Verhaegen, ME, Snyder, NW, Rivera, MN, Osterman, A, Lyssiotis, CA & Lombard, DB 2021, 'The deacylase SIRT5 supports melanoma viability by influencing chromatin dynamics', Journal of Clinical Investigation, المجلد 131, رقم 12, e138926, الصفحات 1-18. https://doi.org/10.1172/JCI138926

TY - JOUR

T1 - The deacylase SIRT5 supports melanoma viability by influencing chromatin dynamics

AU - Giblin, William

AU - Bringman-Rodenbarger, Lauren

AU - Guo, Angela H

AU - Kumar, Surinder

AU - Monovich, Alexander C

AU - Mostafa, Ahmed M

AU - Skinner, Mary E

AU - Azar, Michelle

AU - Mady, Ahmed Sa

AU - Chung, Carolina H

AU - Kadambi, Namrata

AU - Melong, Keith-Allen

AU - Lee, Ho-Joon

AU - Zhang, Li

AU - Sajjakulnukit, Peter

AU - Trefely, Sophie

AU - Varner, Erika L

AU - Iyer, Sowmya

AU - Wang, Min

AU - Wilmott, James S

AU - Soyer, H Peter

AU - Sturm, Richard A

AU - Pritchard, Antonia L

AU - Andea, Aleodor A

AU - Scolyer, Richard A

AU - Stark, Mitchell S

AU - Scott, David A

AU - Fullen, Douglas R

AU - Bosenberg, Marcus W

AU - Chandrasekaran, Sriram

AU - Nikolovska-Coleska, Zaneta

AU - Verhaegen, Monique E

AU - Snyder, Nathaniel W

AU - Rivera, Miguel N

AU - Osterman, Andrei

AU - Lyssiotis, Costas A

AU - Lombard, David B

PY - 2021/6/15

Y1 - 2021/6/15

N2 - Cutaneous melanoma remains the most lethal skin cancer, and ranks third among all malignancies in terms of years of life lost. Despite the advent of immune checkpoint and targeted therapies, only roughly half of patients with advanced melanoma achieves a durable remission. SIRT5 is a member of the sirtuin family of protein deacylases that regulate metabolism and other biological processes. Germline Sirt5 deficiency is associated with mild phenotypes in mice. Here we show that SIRT5 is required for proliferation and survival across all cutaneous melanoma genotypes tested, as well as uveal melanoma, a genetically distinct melanoma subtype that arises in the eye and is incurable once metastatic. Likewise, SIRT5 is required for efficient tumor formation by melanoma xenografts and in an autochthonous mouse Braf;Pten-driven melanoma model. Via metabolite and transcriptomic analyses, we find that SIRT5 is required to maintain histone acetylation and methylation levels in melanoma cells, thereby promoting proper gene expression. SIRT5-dependent genes notably include MITF, a key lineage-specific survival oncogene in melanoma, and the c-MYC proto-oncogene. SIRT5 may represent a novel, druggable genotype-independent addiction in melanoma.

AB - Cutaneous melanoma remains the most lethal skin cancer, and ranks third among all malignancies in terms of years of life lost. Despite the advent of immune checkpoint and targeted therapies, only roughly half of patients with advanced melanoma achieves a durable remission. SIRT5 is a member of the sirtuin family of protein deacylases that regulate metabolism and other biological processes. Germline Sirt5 deficiency is associated with mild phenotypes in mice. Here we show that SIRT5 is required for proliferation and survival across all cutaneous melanoma genotypes tested, as well as uveal melanoma, a genetically distinct melanoma subtype that arises in the eye and is incurable once metastatic. Likewise, SIRT5 is required for efficient tumor formation by melanoma xenografts and in an autochthonous mouse Braf;Pten-driven melanoma model. Via metabolite and transcriptomic analyses, we find that SIRT5 is required to maintain histone acetylation and methylation levels in melanoma cells, thereby promoting proper gene expression. SIRT5-dependent genes notably include MITF, a key lineage-specific survival oncogene in melanoma, and the c-MYC proto-oncogene. SIRT5 may represent a novel, druggable genotype-independent addiction in melanoma.

KW - Cell Biology

KW - Metabolism

U2 - 10.1172/JCI138926

DO - 10.1172/JCI138926

M3 - Article

C2 - 33945506

SN - 0021-9738

VL - 131

SP - 1

EP - 18

JO - Journal of Clinical Investigation

JF - Journal of Clinical Investigation

IS - 12

M1 - e138926

ER -

The deacylase SIRT5 supports melanoma viability by influencing chromatin dynamics

ملخص

أهداف الأمم المتحدة للتنمية المستدامة

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