ASCC1 structures and bioinformatics reveal a novel helix-clasp-helix RNA-binding motif linked to a two-histidine phosphodiesterase

Naga babu Chinnam; Roopa Thapar; Andrew S. Arvai; Altaf H. Sarker; Jennifer M. Soll; Tanmoy Paul; Aleem Syed; Daniel J. Rosenberg; Michal Hammel; Albino Bacolla; Panagiotis Katsonis; Abhishek Asthana; Miaw Sheue Tsai; Ivaylo Ivanov; Olivier Lichtarge; Robert H. Silverman; Nima Mosammaparast; Susan E. Tsutakawa; John A. Tainer

doi:10.1016/j.jbc.2024.107368

ASCC1 structures and bioinformatics reveal a novel helix-clasp-helix RNA-binding motif linked to a two-histidine phosphodiesterase

Naga babu Chinnam, Roopa Thapar, Andrew S. Arvai, Altaf H. Sarker, Jennifer M. Soll, Tanmoy Paul, Aleem Syed, Daniel J. Rosenberg, Michal Hammel, Albino Bacolla, Panagiotis Katsonis, Abhishek Asthana, Miaw Sheue Tsai, Ivaylo Ivanov, Olivier Lichtarge, Robert H. Silverman, Nima Mosammaparast, Susan E. Tsutakawa, John A. Tainer

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

1 Scopus citations

Abstract

Activating signal co-integrator complex 1 (ASCC1) acts with ASCC-ALKBH3 complex in alkylation damage responses. ASCC1 uniquely combines two evolutionarily ancient domains: nucleotide-binding K-Homology (KH) (associated with regulating splicing, transcriptional, and translation) and two-histidine phosphodiesterase (PDE; associated with hydrolysis of cyclic nucleotide phosphate bonds). Germline mutations link loss of ASCC1 function to spinal muscular atrophy with congenital bone fractures 2 (SMABF2). Herein analysis of The Cancer Genome Atlas (TCGA) suggests ASCC1 RNA overexpression in certain tumors correlates with poor survival, Signatures 29 and 3 mutations, and genetic instability markers. We determined crystal structures of Alvinella pompejana (Ap) ASCC1 and Human (Hs) PDE domain revealing high-resolution details and features conserved over 500 million years of evolution. Extending our understanding of the KH domain Gly-X-X-Gly sequence motif, we define a novel structural Helix-Clasp-Helix (HCH) nucleotide binding motif and show ASCC1 sequence-specific binding to CGCG-containing RNA. The V-shaped PDE nucleotide binding channel has two His-Φ-Ser/Thr-Φ (HXT) motifs (Φ being hydrophobic) positioned to initiate cyclic phosphate bond hydrolysis. A conserved atypical active-site histidine torsion angle implies a novel PDE substrate. Flexible active site loop and arginine-rich domain linker appear regulatory. Small-angle X-ray scattering (SAXS) revealed aligned KH-PDE RNA binding sites with limited flexibility in solution. Quantitative evolutionary bioinformatic analyses of disease and cancer-associated mutations support implied functional roles for RNA binding, phosphodiesterase activity, and regulation. Collective results inform ASCC1's roles in transactivation and alkylation damage responses, its targeting by structure-based inhibitors, and how ASCC1 mutations may impact inherited disease and cancer.

Original language	English (US)
Article number	107368
Journal	Journal of Biological Chemistry
Volume	300
Issue number	6
DOIs	https://doi.org/10.1016/j.jbc.2024.107368
State	Published - Jun 2024

Keywords

DNA repair
RNA
binding protein
conformational change
crystallography
genomics
inhibition mechanism
phosphodiesterase: cancer
small angle X-ray scattering (SAXS)
structural biology

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Cell Biology

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10.1016/j.jbc.2024.107368

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Chinnam, N. B., Thapar, R., Arvai, A. S., Sarker, A. H., Soll, J. M., Paul, T., Syed, A., Rosenberg, D. J., Hammel, M., Bacolla, A., Katsonis, P., Asthana, A., Tsai, M. S., Ivanov, I., Lichtarge, O., Silverman, R. H., Mosammaparast, N., Tsutakawa, S. E., & Tainer, J. A. (2024). ASCC1 structures and bioinformatics reveal a novel helix-clasp-helix RNA-binding motif linked to a two-histidine phosphodiesterase. Journal of Biological Chemistry, 300(6), Article 107368. https://doi.org/10.1016/j.jbc.2024.107368

Chinnam, NB, Thapar, R, Arvai, AS, Sarker, AH, Soll, JM, Paul, T, Syed, A, Rosenberg, DJ, Hammel, M, Bacolla, A, Katsonis, P, Asthana, A, Tsai, MS, Ivanov, I, Lichtarge, O, Silverman, RH, Mosammaparast, N, Tsutakawa, SE & Tainer, JA 2024, 'ASCC1 structures and bioinformatics reveal a novel helix-clasp-helix RNA-binding motif linked to a two-histidine phosphodiesterase', Journal of Biological Chemistry, vol. 300, no. 6, 107368. https://doi.org/10.1016/j.jbc.2024.107368

@article{1b3d1c6dfeda4ea7a8bcf3954f7b5a5c,

title = "ASCC1 structures and bioinformatics reveal a novel helix-clasp-helix RNA-binding motif linked to a two-histidine phosphodiesterase",

abstract = "Activating signal co-integrator complex 1 (ASCC1) acts with ASCC-ALKBH3 complex in alkylation damage responses. ASCC1 uniquely combines two evolutionarily ancient domains: nucleotide-binding K-Homology (KH) (associated with regulating splicing, transcriptional, and translation) and two-histidine phosphodiesterase (PDE; associated with hydrolysis of cyclic nucleotide phosphate bonds). Germline mutations link loss of ASCC1 function to spinal muscular atrophy with congenital bone fractures 2 (SMABF2). Herein analysis of The Cancer Genome Atlas (TCGA) suggests ASCC1 RNA overexpression in certain tumors correlates with poor survival, Signatures 29 and 3 mutations, and genetic instability markers. We determined crystal structures of Alvinella pompejana (Ap) ASCC1 and Human (Hs) PDE domain revealing high-resolution details and features conserved over 500 million years of evolution. Extending our understanding of the KH domain Gly-X-X-Gly sequence motif, we define a novel structural Helix-Clasp-Helix (HCH) nucleotide binding motif and show ASCC1 sequence-specific binding to CGCG-containing RNA. The V-shaped PDE nucleotide binding channel has two His-Φ-Ser/Thr-Φ (HXT) motifs (Φ being hydrophobic) positioned to initiate cyclic phosphate bond hydrolysis. A conserved atypical active-site histidine torsion angle implies a novel PDE substrate. Flexible active site loop and arginine-rich domain linker appear regulatory. Small-angle X-ray scattering (SAXS) revealed aligned KH-PDE RNA binding sites with limited flexibility in solution. Quantitative evolutionary bioinformatic analyses of disease and cancer-associated mutations support implied functional roles for RNA binding, phosphodiesterase activity, and regulation. Collective results inform ASCC1's roles in transactivation and alkylation damage responses, its targeting by structure-based inhibitors, and how ASCC1 mutations may impact inherited disease and cancer.",

keywords = "DNA repair, RNA, binding protein, conformational change, crystallography, genomics, inhibition mechanism, phosphodiesterase: cancer, small angle X-ray scattering (SAXS), structural biology",

author = "Chinnam, {Naga babu} and Roopa Thapar and Arvai, {Andrew S.} and Sarker, {Altaf H.} and Soll, {Jennifer M.} and Tanmoy Paul and Aleem Syed and Rosenberg, {Daniel J.} and Michal Hammel and Albino Bacolla and Panagiotis Katsonis and Abhishek Asthana and Tsai, {Miaw Sheue} and Ivaylo Ivanov and Olivier Lichtarge and Silverman, {Robert H.} and Nima Mosammaparast and Tsutakawa, {Susan E.} and Tainer, {John A.}",

note = "Publisher Copyright: {\textcopyright} 2024 The Authors",

year = "2024",

month = jun,

doi = "10.1016/j.jbc.2024.107368",

language = "English (US)",

volume = "300",

journal = "Journal of Biological Chemistry",

issn = "0021-9258",

publisher = "American Society for Biochemistry and Molecular Biology Inc.",

number = "6",

}

TY - JOUR

T1 - ASCC1 structures and bioinformatics reveal a novel helix-clasp-helix RNA-binding motif linked to a two-histidine phosphodiesterase

AU - Chinnam, Naga babu

AU - Thapar, Roopa

AU - Arvai, Andrew S.

AU - Sarker, Altaf H.

AU - Soll, Jennifer M.

AU - Paul, Tanmoy

AU - Syed, Aleem

AU - Rosenberg, Daniel J.

AU - Hammel, Michal

AU - Bacolla, Albino

AU - Katsonis, Panagiotis

AU - Asthana, Abhishek

AU - Tsai, Miaw Sheue

AU - Ivanov, Ivaylo

AU - Lichtarge, Olivier

AU - Silverman, Robert H.

AU - Mosammaparast, Nima

AU - Tsutakawa, Susan E.

AU - Tainer, John A.

PY - 2024/6

Y1 - 2024/6

N2 - Activating signal co-integrator complex 1 (ASCC1) acts with ASCC-ALKBH3 complex in alkylation damage responses. ASCC1 uniquely combines two evolutionarily ancient domains: nucleotide-binding K-Homology (KH) (associated with regulating splicing, transcriptional, and translation) and two-histidine phosphodiesterase (PDE; associated with hydrolysis of cyclic nucleotide phosphate bonds). Germline mutations link loss of ASCC1 function to spinal muscular atrophy with congenital bone fractures 2 (SMABF2). Herein analysis of The Cancer Genome Atlas (TCGA) suggests ASCC1 RNA overexpression in certain tumors correlates with poor survival, Signatures 29 and 3 mutations, and genetic instability markers. We determined crystal structures of Alvinella pompejana (Ap) ASCC1 and Human (Hs) PDE domain revealing high-resolution details and features conserved over 500 million years of evolution. Extending our understanding of the KH domain Gly-X-X-Gly sequence motif, we define a novel structural Helix-Clasp-Helix (HCH) nucleotide binding motif and show ASCC1 sequence-specific binding to CGCG-containing RNA. The V-shaped PDE nucleotide binding channel has two His-Φ-Ser/Thr-Φ (HXT) motifs (Φ being hydrophobic) positioned to initiate cyclic phosphate bond hydrolysis. A conserved atypical active-site histidine torsion angle implies a novel PDE substrate. Flexible active site loop and arginine-rich domain linker appear regulatory. Small-angle X-ray scattering (SAXS) revealed aligned KH-PDE RNA binding sites with limited flexibility in solution. Quantitative evolutionary bioinformatic analyses of disease and cancer-associated mutations support implied functional roles for RNA binding, phosphodiesterase activity, and regulation. Collective results inform ASCC1's roles in transactivation and alkylation damage responses, its targeting by structure-based inhibitors, and how ASCC1 mutations may impact inherited disease and cancer.

AB - Activating signal co-integrator complex 1 (ASCC1) acts with ASCC-ALKBH3 complex in alkylation damage responses. ASCC1 uniquely combines two evolutionarily ancient domains: nucleotide-binding K-Homology (KH) (associated with regulating splicing, transcriptional, and translation) and two-histidine phosphodiesterase (PDE; associated with hydrolysis of cyclic nucleotide phosphate bonds). Germline mutations link loss of ASCC1 function to spinal muscular atrophy with congenital bone fractures 2 (SMABF2). Herein analysis of The Cancer Genome Atlas (TCGA) suggests ASCC1 RNA overexpression in certain tumors correlates with poor survival, Signatures 29 and 3 mutations, and genetic instability markers. We determined crystal structures of Alvinella pompejana (Ap) ASCC1 and Human (Hs) PDE domain revealing high-resolution details and features conserved over 500 million years of evolution. Extending our understanding of the KH domain Gly-X-X-Gly sequence motif, we define a novel structural Helix-Clasp-Helix (HCH) nucleotide binding motif and show ASCC1 sequence-specific binding to CGCG-containing RNA. The V-shaped PDE nucleotide binding channel has two His-Φ-Ser/Thr-Φ (HXT) motifs (Φ being hydrophobic) positioned to initiate cyclic phosphate bond hydrolysis. A conserved atypical active-site histidine torsion angle implies a novel PDE substrate. Flexible active site loop and arginine-rich domain linker appear regulatory. Small-angle X-ray scattering (SAXS) revealed aligned KH-PDE RNA binding sites with limited flexibility in solution. Quantitative evolutionary bioinformatic analyses of disease and cancer-associated mutations support implied functional roles for RNA binding, phosphodiesterase activity, and regulation. Collective results inform ASCC1's roles in transactivation and alkylation damage responses, its targeting by structure-based inhibitors, and how ASCC1 mutations may impact inherited disease and cancer.

KW - DNA repair

KW - RNA

KW - binding protein

KW - conformational change

KW - crystallography

KW - genomics

KW - inhibition mechanism

KW - phosphodiesterase: cancer

KW - small angle X-ray scattering (SAXS)

KW - structural biology

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UR - http://www.scopus.com/inward/citedby.url?scp=85195036545&partnerID=8YFLogxK

U2 - 10.1016/j.jbc.2024.107368

DO - 10.1016/j.jbc.2024.107368

M3 - Article

C2 - 38750793

AN - SCOPUS:85195036545

SN - 0021-9258

VL - 300

JO - Journal of Biological Chemistry

JF - Journal of Biological Chemistry

IS - 6

M1 - 107368

ER -

ASCC1 structures and bioinformatics reveal a novel helix-clasp-helix RNA-binding motif linked to a two-histidine phosphodiesterase

Abstract

Keywords

ASJC Scopus subject areas

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