The Interaction between NKAP and HDAC3 Is Critical for T Cell Maturation

Barsha Dash; Michael J. Shapiro; Puspa Thapa; Sinibaldo Romero Arocha; Ji Young Chung; Aaron D. Schwab; Shaylene A. McCue; Matthew J. Rajcula; Virginia Smith Shapiro

doi:10.4049/immunohorizons.1900052

The Interaction between NKAP and HDAC3 Is Critical for T Cell Maturation

Barsha Dash, Michael J. Shapiro, Puspa Thapa, Sinibaldo Romero Arocha, Ji Young Chung, Aaron D. Schwab, Shaylene A. McCue, Matthew J. Rajcula, Virginia Smith Shapiro

Immunology

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

Abstract

NKAP and HDAC3 are critical for T cell maturation. NKAP and HDAC3 physically associate, and a point mutation in NKAP, NKAP(Y352A), abrogates this interaction. To evaluate the significance of NKAP and HDAC3 association in T cell maturation, transgenic mice were engineered for cre-mediated endogenous NKAP gene deletion coupled to induction of NKAP(Y352A) or a wild type (WT) control transgene, NKAP(WT), in double positive thymocytes or regulatory T cells (Tregs). T cell maturation was normal in mice with endogenous NKAP deletion coupled to NKAP(WT) induction. However, severe defects occurred in T cell and Treg maturation and in iNKT cell development when NKAP(Y352A) was induced, recapitulating NKAP deficiency. Conventional T cells expressing NKAP(Y352A) failed to enter the long-term T cell pool, did not produce cytokines, and remained complement susceptible, whereas Tregs expressing NKAP(Y352A) were eliminated as recent thymic emigrants leading to lethal autoimmunity. Overall, these results demonstrate the significance of NKAP–HDAC3 association in T cells.

Original language	English (US)
Pages (from-to)	352-367
Number of pages	16
Journal	ImmunoHorizons
Volume	3
Issue number	8
DOIs	https://doi.org/10.4049/immunohorizons.1900052
State	Published - Aug 1 2019

ASJC Scopus subject areas

Medicine(all)
Immunology and Allergy
Immunology

Access to Document

10.4049/immunohorizons.1900052

Cite this

@article{b7caa84c298e49a5a252d9ff5ad8df71,

title = "The Interaction between NKAP and HDAC3 Is Critical for T Cell Maturation",

abstract = "NKAP and HDAC3 are critical for T cell maturation. NKAP and HDAC3 physically associate, and a point mutation in NKAP, NKAP(Y352A), abrogates this interaction. To evaluate the significance of NKAP and HDAC3 association in T cell maturation, transgenic mice were engineered for cre-mediated endogenous NKAP gene deletion coupled to induction of NKAP(Y352A) or a wild type (WT) control transgene, NKAP(WT), in double positive thymocytes or regulatory T cells (Tregs). T cell maturation was normal in mice with endogenous NKAP deletion coupled to NKAP(WT) induction. However, severe defects occurred in T cell and Treg maturation and in iNKT cell development when NKAP(Y352A) was induced, recapitulating NKAP deficiency. Conventional T cells expressing NKAP(Y352A) failed to enter the long-term T cell pool, did not produce cytokines, and remained complement susceptible, whereas Tregs expressing NKAP(Y352A) were eliminated as recent thymic emigrants leading to lethal autoimmunity. Overall, these results demonstrate the significance of NKAP–HDAC3 association in T cells.",

author = "Barsha Dash and Shapiro, {Michael J.} and Puspa Thapa and Arocha, {Sinibaldo Romero} and Chung, {Ji Young} and Schwab, {Aaron D.} and McCue, {Shaylene A.} and Rajcula, {Matthew J.} and Shapiro, {Virginia Smith}",

note = "Funding Information: Received for publication July 3, 2019. Accepted for publication July 9, 2019. Address correspondence and reprint requests to: Dr. Virginia Smith Shapiro, Mayo Clinic, Department of Immunology, 4-01 C Guggenheim Building, 200 First Street SW, Rochester, MN 55905. E-mail address: Shapiro.Virginia1@mayo.edu ORCIDs: 0000-0003-0037-0848 (M.J.S.); 0000-0003-1142-7790 (A.D.S.); 0000-0001-9978-341X (V.S.S.). 1Equal contributions. This work was supported by National Institutes of Health Grant R01 AI083279 to V.S.S. B.D. designed experiments, analyzed data and wrote and edited the manuscript, M.J.S. generated the lines of mice and edited the manuscript. P.T. designed experiments, performed experiments and analyzed data, S.R.A., J.-Y.C., A.D.S., S.A.M., and M.J.R. maintained the mouse colony and genotyped the mice. V.S.S. oversaw the study, designed experiments and edited the manuscript. Abbreviations used in this article: ANA, anti-nuclear Ab; cKO, conditional knockout; DP, double positive; gMFI, geometric mean fluorescence intensity; HDAC3, histone deacetylase 3; HSC, hematopoietic stem cell; iNKT, invariant NKT; M1, mature 1; M2, mature 2; RTE, recent thymic emigrant; SM, semimature; SP, single positive; Treg, regulatory T cell; WT, wild type. The online version of this article contains supplemental material. This article is distributed under the terms of the CC BY-NC-ND 4.0 Unported license. Copyright {\textcopyright} 2019 The Authors Publisher Copyright: Copyright {\textcopyright} 2019 The Authors.",

year = "2019",

month = aug,

day = "1",

doi = "10.4049/immunohorizons.1900052",

language = "English (US)",

volume = "3",

pages = "352--367",

journal = "ImmunoHorizons",

issn = "2573-7732",

publisher = "NLM (Medline)",

number = "8",

}

TY - JOUR

T1 - The Interaction between NKAP and HDAC3 Is Critical for T Cell Maturation

AU - Dash, Barsha

AU - Shapiro, Michael J.

AU - Thapa, Puspa

AU - Arocha, Sinibaldo Romero

AU - Chung, Ji Young

AU - Schwab, Aaron D.

AU - McCue, Shaylene A.

AU - Rajcula, Matthew J.

AU - Shapiro, Virginia Smith

N1 - Funding Information: Received for publication July 3, 2019. Accepted for publication July 9, 2019. Address correspondence and reprint requests to: Dr. Virginia Smith Shapiro, Mayo Clinic, Department of Immunology, 4-01 C Guggenheim Building, 200 First Street SW, Rochester, MN 55905. E-mail address: Shapiro.Virginia1@mayo.edu ORCIDs: 0000-0003-0037-0848 (M.J.S.); 0000-0003-1142-7790 (A.D.S.); 0000-0001-9978-341X (V.S.S.). 1Equal contributions. This work was supported by National Institutes of Health Grant R01 AI083279 to V.S.S. B.D. designed experiments, analyzed data and wrote and edited the manuscript, M.J.S. generated the lines of mice and edited the manuscript. P.T. designed experiments, performed experiments and analyzed data, S.R.A., J.-Y.C., A.D.S., S.A.M., and M.J.R. maintained the mouse colony and genotyped the mice. V.S.S. oversaw the study, designed experiments and edited the manuscript. Abbreviations used in this article: ANA, anti-nuclear Ab; cKO, conditional knockout; DP, double positive; gMFI, geometric mean fluorescence intensity; HDAC3, histone deacetylase 3; HSC, hematopoietic stem cell; iNKT, invariant NKT; M1, mature 1; M2, mature 2; RTE, recent thymic emigrant; SM, semimature; SP, single positive; Treg, regulatory T cell; WT, wild type. The online version of this article contains supplemental material. This article is distributed under the terms of the CC BY-NC-ND 4.0 Unported license. Copyright © 2019 The Authors Publisher Copyright: Copyright © 2019 The Authors.

PY - 2019/8/1

Y1 - 2019/8/1

N2 - NKAP and HDAC3 are critical for T cell maturation. NKAP and HDAC3 physically associate, and a point mutation in NKAP, NKAP(Y352A), abrogates this interaction. To evaluate the significance of NKAP and HDAC3 association in T cell maturation, transgenic mice were engineered for cre-mediated endogenous NKAP gene deletion coupled to induction of NKAP(Y352A) or a wild type (WT) control transgene, NKAP(WT), in double positive thymocytes or regulatory T cells (Tregs). T cell maturation was normal in mice with endogenous NKAP deletion coupled to NKAP(WT) induction. However, severe defects occurred in T cell and Treg maturation and in iNKT cell development when NKAP(Y352A) was induced, recapitulating NKAP deficiency. Conventional T cells expressing NKAP(Y352A) failed to enter the long-term T cell pool, did not produce cytokines, and remained complement susceptible, whereas Tregs expressing NKAP(Y352A) were eliminated as recent thymic emigrants leading to lethal autoimmunity. Overall, these results demonstrate the significance of NKAP–HDAC3 association in T cells.

AB - NKAP and HDAC3 are critical for T cell maturation. NKAP and HDAC3 physically associate, and a point mutation in NKAP, NKAP(Y352A), abrogates this interaction. To evaluate the significance of NKAP and HDAC3 association in T cell maturation, transgenic mice were engineered for cre-mediated endogenous NKAP gene deletion coupled to induction of NKAP(Y352A) or a wild type (WT) control transgene, NKAP(WT), in double positive thymocytes or regulatory T cells (Tregs). T cell maturation was normal in mice with endogenous NKAP deletion coupled to NKAP(WT) induction. However, severe defects occurred in T cell and Treg maturation and in iNKT cell development when NKAP(Y352A) was induced, recapitulating NKAP deficiency. Conventional T cells expressing NKAP(Y352A) failed to enter the long-term T cell pool, did not produce cytokines, and remained complement susceptible, whereas Tregs expressing NKAP(Y352A) were eliminated as recent thymic emigrants leading to lethal autoimmunity. Overall, these results demonstrate the significance of NKAP–HDAC3 association in T cells.

UR - http://www.scopus.com/inward/record.url?scp=85106330642&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85106330642&partnerID=8YFLogxK

U2 - 10.4049/immunohorizons.1900052

DO - 10.4049/immunohorizons.1900052

M3 - Article

C2 - 31387873

AN - SCOPUS:85106330642

SN - 2573-7732

VL - 3

SP - 352

EP - 367

JO - ImmunoHorizons

JF - ImmunoHorizons

IS - 8

ER -

The Interaction between NKAP and HDAC3 Is Critical for T Cell Maturation

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this