TREX tetramer disruption alters RNA processing necessary for corticogenesis in THOC6 Intellectual Disability Syndrome

Elizabeth A. Werren; Geneva R. LaForce; Anshika Srivastava; Delia R. Perillo; Shaokun Li; Katherine Johnson; Safa Baris; Brandon Berger; Samantha L. Regan; Christian D. Pfennig; Sonja de Munnik; Rolph Pfundt; Malavika Hebbar; Raúl Jimenez-Heredia; Elif Karakoc-Aydiner; Ahmet Ozen; Jasmin Dmytrus; Ana Krolo; Ken Corning; E. J. Prijoles; Raymond J. Louie; Robert Roger Lebel; Thuy Linh Le; Jeanne Amiel; Christopher T. Gordon; Kaan Boztug; Katta M. Girisha; Anju Shukla; Stephanie L. Bielas; Ashleigh E. Schaffer

doi:10.1038/s41467-024-45948-y

TREX tetramer disruption alters RNA processing necessary for corticogenesis in THOC6 Intellectual Disability Syndrome

Elizabeth A. Werren, Geneva R. LaForce, Anshika Srivastava, Delia R. Perillo, Shaokun Li, Katherine Johnson, Safa Baris, Brandon Berger, Samantha L. Regan, Christian D. Pfennig, Sonja de Munnik, Rolph Pfundt, Malavika Hebbar, Raúl Jimenez-Heredia, Elif Karakoc-Aydiner, Ahmet Ozen, Jasmin Dmytrus, Ana Krolo, Ken Corning, E. J. PrijolesRaymond J. Louie, Robert Roger Lebel, Thuy Linh Le, Jeanne Amiel, Christopher T. Gordon, Kaan Boztug, Katta M. Girisha, Anju Shukla, Stephanie L. Bielas^*, Ashleigh E. Schaffer^*

^*المؤلف المقابل لهذا العمل

Genetics

نتاج البحث: المساهمة في مجلة › Article › مراجعة النظراء

ملخص

THOC6 variants are the genetic basis of autosomal recessive THOC6 Intellectual Disability Syndrome (TIDS). THOC6 is critical for mammalian Transcription Export complex (TREX) tetramer formation, which is composed of four six-subunit THO monomers. The TREX tetramer facilitates mammalian RNA processing, in addition to the nuclear mRNA export functions of the TREX dimer conserved through yeast. Human and mouse TIDS model systems revealed novel THOC6-dependent, species-specific TREX tetramer functions. Germline biallelic Thoc6 loss-of-function (LOF) variants result in mouse embryonic lethality. Biallelic THOC6 LOF variants reduce the binding affinity of ALYREF to THOC5 without affecting the protein expression of TREX members, implicating impaired TREX tetramer formation. Defects in RNA nuclear export functions were not detected in biallelic THOC6 LOF human neural cells. Instead, mis-splicing was detected in human and mouse neural tissue, revealing novel THOC6-mediated TREX coordination of mRNA processing. We demonstrate that THOC6 is required for key signaling pathways known to regulate the transition from proliferative to neurogenic divisions during human corticogenesis. Together, these findings implicate altered RNA processing in the developmental biology of TIDS neuropathology.

اللغة الأصلية	English
رقم المقال	1640
دورية	Nature Communications
مستوى الصوت	15
رقم الإصدار	1
المعرِّفات الرقمية للأشياء	https://doi.org/10.1038/s41467-024-45948-y
حالة النشر	Published - فبراير 22 2024

ASJC Scopus subject areas

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الوصول إلى المستند

10.1038/s41467-024-45948-y

الملفات والروابط الأخرى

قم بذكر هذا

Werren, E. A., LaForce, G. R., Srivastava, A., Perillo, D. R., Li, S., Johnson, K., Baris, S., Berger, B., Regan, S. L., Pfennig, C. D., de Munnik, S., Pfundt, R., Hebbar, M., Jimenez-Heredia, R., Karakoc-Aydiner, E., Ozen, A., Dmytrus, J., Krolo, A., Corning, K., ... Schaffer, A. E. (2024). TREX tetramer disruption alters RNA processing necessary for corticogenesis in THOC6 Intellectual Disability Syndrome. Nature Communications, 15(1), المقال 1640. https://doi.org/10.1038/s41467-024-45948-y

TREX tetramer disruption alters RNA processing necessary for corticogenesis in THOC6 Intellectual Disability Syndrome. / Werren, Elizabeth A.; LaForce, Geneva R.; Srivastava, Anshika وآخرون.
في: Nature Communications, المجلد 15, رقم 1, 1640, ٢٢.٠٢.٢٠٢٤.

نتاج البحث: المساهمة في مجلة › Article › مراجعة النظراء

Werren, EA, LaForce, GR, Srivastava, A, Perillo, DR, Li, S, Johnson, K, Baris, S, Berger, B, Regan, SL, Pfennig, CD, de Munnik, S, Pfundt, R, Hebbar, M, Jimenez-Heredia, R, Karakoc-Aydiner, E, Ozen, A, Dmytrus, J, Krolo, A, Corning, K, Prijoles, EJ, Louie, RJ, Lebel, RR, Le, TL, Amiel, J, Gordon, CT, Boztug, K, Girisha, KM, Shukla, A, Bielas, SL & Schaffer, AE 2024, 'TREX tetramer disruption alters RNA processing necessary for corticogenesis in THOC6 Intellectual Disability Syndrome', Nature Communications, المجلد 15, رقم 1, 1640. https://doi.org/10.1038/s41467-024-45948-y

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title = "TREX tetramer disruption alters RNA processing necessary for corticogenesis in THOC6 Intellectual Disability Syndrome",

abstract = "THOC6 variants are the genetic basis of autosomal recessive THOC6 Intellectual Disability Syndrome (TIDS). THOC6 is critical for mammalian Transcription Export complex (TREX) tetramer formation, which is composed of four six-subunit THO monomers. The TREX tetramer facilitates mammalian RNA processing, in addition to the nuclear mRNA export functions of the TREX dimer conserved through yeast. Human and mouse TIDS model systems revealed novel THOC6-dependent, species-specific TREX tetramer functions. Germline biallelic Thoc6 loss-of-function (LOF) variants result in mouse embryonic lethality. Biallelic THOC6 LOF variants reduce the binding affinity of ALYREF to THOC5 without affecting the protein expression of TREX members, implicating impaired TREX tetramer formation. Defects in RNA nuclear export functions were not detected in biallelic THOC6 LOF human neural cells. Instead, mis-splicing was detected in human and mouse neural tissue, revealing novel THOC6-mediated TREX coordination of mRNA processing. We demonstrate that THOC6 is required for key signaling pathways known to regulate the transition from proliferative to neurogenic divisions during human corticogenesis. Together, these findings implicate altered RNA processing in the developmental biology of TIDS neuropathology.",

keywords = "Humans, Animals, Mice, RNA/metabolism, Intellectual Disability/genetics, RNA, Messenger/genetics, RNA Processing, Post-Transcriptional, RNA Transport, Mammals/genetics, Nuclear Proteins/metabolism, RNA-Binding Proteins/genetics, Stilbenes, Sulfonic Acids",

author = "Werren, {Elizabeth A.} and LaForce, {Geneva R.} and Anshika Srivastava and Perillo, {Delia R.} and Shaokun Li and Katherine Johnson and Safa Baris and Brandon Berger and Regan, {Samantha L.} and Pfennig, {Christian D.} and {de Munnik}, Sonja and Rolph Pfundt and Malavika Hebbar and Ra{\'u}l Jimenez-Heredia and Elif Karakoc-Aydiner and Ahmet Ozen and Jasmin Dmytrus and Ana Krolo and Ken Corning and Prijoles, {E. J.} and Louie, {Raymond J.} and Lebel, {Robert Roger} and Le, {Thuy Linh} and Jeanne Amiel and Gordon, {Christopher T.} and Kaan Boztug and Girisha, {Katta M.} and Anju Shukla and Bielas, {Stephanie L.} and Schaffer, {Ashleigh E.}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2024",

month = feb,

day = "22",

doi = "10.1038/s41467-024-45948-y",

language = "English",

volume = "15",

journal = "Nature Communications",

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T1 - TREX tetramer disruption alters RNA processing necessary for corticogenesis in THOC6 Intellectual Disability Syndrome

AU - Werren, Elizabeth A.

AU - LaForce, Geneva R.

AU - Srivastava, Anshika

AU - Perillo, Delia R.

AU - Li, Shaokun

AU - Johnson, Katherine

AU - Baris, Safa

AU - Berger, Brandon

AU - Regan, Samantha L.

AU - Pfennig, Christian D.

AU - de Munnik, Sonja

AU - Pfundt, Rolph

AU - Hebbar, Malavika

AU - Jimenez-Heredia, Raúl

AU - Karakoc-Aydiner, Elif

AU - Ozen, Ahmet

AU - Dmytrus, Jasmin

AU - Krolo, Ana

AU - Corning, Ken

AU - Prijoles, E. J.

AU - Louie, Raymond J.

AU - Lebel, Robert Roger

AU - Le, Thuy Linh

AU - Amiel, Jeanne

AU - Gordon, Christopher T.

AU - Boztug, Kaan

AU - Girisha, Katta M.

AU - Shukla, Anju

AU - Bielas, Stephanie L.

AU - Schaffer, Ashleigh E.

N1 - Publisher Copyright: © The Author(s) 2024.

PY - 2024/2/22

Y1 - 2024/2/22

N2 - THOC6 variants are the genetic basis of autosomal recessive THOC6 Intellectual Disability Syndrome (TIDS). THOC6 is critical for mammalian Transcription Export complex (TREX) tetramer formation, which is composed of four six-subunit THO monomers. The TREX tetramer facilitates mammalian RNA processing, in addition to the nuclear mRNA export functions of the TREX dimer conserved through yeast. Human and mouse TIDS model systems revealed novel THOC6-dependent, species-specific TREX tetramer functions. Germline biallelic Thoc6 loss-of-function (LOF) variants result in mouse embryonic lethality. Biallelic THOC6 LOF variants reduce the binding affinity of ALYREF to THOC5 without affecting the protein expression of TREX members, implicating impaired TREX tetramer formation. Defects in RNA nuclear export functions were not detected in biallelic THOC6 LOF human neural cells. Instead, mis-splicing was detected in human and mouse neural tissue, revealing novel THOC6-mediated TREX coordination of mRNA processing. We demonstrate that THOC6 is required for key signaling pathways known to regulate the transition from proliferative to neurogenic divisions during human corticogenesis. Together, these findings implicate altered RNA processing in the developmental biology of TIDS neuropathology.

AB - THOC6 variants are the genetic basis of autosomal recessive THOC6 Intellectual Disability Syndrome (TIDS). THOC6 is critical for mammalian Transcription Export complex (TREX) tetramer formation, which is composed of four six-subunit THO monomers. The TREX tetramer facilitates mammalian RNA processing, in addition to the nuclear mRNA export functions of the TREX dimer conserved through yeast. Human and mouse TIDS model systems revealed novel THOC6-dependent, species-specific TREX tetramer functions. Germline biallelic Thoc6 loss-of-function (LOF) variants result in mouse embryonic lethality. Biallelic THOC6 LOF variants reduce the binding affinity of ALYREF to THOC5 without affecting the protein expression of TREX members, implicating impaired TREX tetramer formation. Defects in RNA nuclear export functions were not detected in biallelic THOC6 LOF human neural cells. Instead, mis-splicing was detected in human and mouse neural tissue, revealing novel THOC6-mediated TREX coordination of mRNA processing. We demonstrate that THOC6 is required for key signaling pathways known to regulate the transition from proliferative to neurogenic divisions during human corticogenesis. Together, these findings implicate altered RNA processing in the developmental biology of TIDS neuropathology.

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KW - Animals

KW - Mice

KW - RNA/metabolism

KW - Intellectual Disability/genetics

KW - RNA, Messenger/genetics

KW - RNA Processing, Post-Transcriptional

KW - RNA Transport

KW - Mammals/genetics

KW - Nuclear Proteins/metabolism

KW - RNA-Binding Proteins/genetics

KW - Stilbenes

KW - Sulfonic Acids

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