SPECC1L regulates palate development downstream of IRF6

Everett G. Hall; Luke W. Wenger; Nathan R. Wilson; Sraavya S. Undurty-Akella; Jennifer Standley; Eno Abasi Augustine-Akpan; Youssef A. Kousa; Diana S. Acevedo; Jeremy P. Goering; Lenore Pitstick; Nagato Natsume; Shahnawaz M. Paroya; Tamara D. Busch; Masaaki Ito; Akihiro Mori; Hideto Imura; Laura E. Schultz-Rogers; Eric W. Klee; Dusica Babovic-Vuksanovic; Sarah A. Kroc; Wasiu L. Adeyemo; Mekonen A. Eshete; Bryan C. Bjork; Satoshi Suzuki; Jeffrey C. Murray; Brian C. Schutte; Azeez Butali; Irfan Saadi

doi:10.1093/hmg/ddaa002

SPECC1L regulates palate development downstream of IRF6

Everett G. Hall, Luke W. Wenger, Nathan R. Wilson, Sraavya S. Undurty-Akella, Jennifer Standley, Eno Abasi Augustine-Akpan, Youssef A. Kousa, Diana S. Acevedo, Jeremy P. Goering, Lenore Pitstick, Nagato Natsume, Shahnawaz M. Paroya, Tamara D. Busch, Masaaki Ito, Akihiro Mori, Hideto Imura, Laura E. Schultz-Rogers, Eric W. Klee, Dusica Babovic-Vuksanovic, Sarah A. KrocWasiu L. Adeyemo, Mekonen A. Eshete, Bryan C. Bjork, Satoshi Suzuki, Jeffrey C. Murray, Brian C. Schutte, Azeez Butali, Irfan Saadi

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

3 Scopus citations

Abstract

SPECC1L mutations have been identified in patients with rare atypical orofacial clefts and with syndromic cleft lip and/or palate (CL/P). These mutations cluster in the second coiled-coil and calponin homology domains of SPECC1L and severely affect the ability of SPECC1L to associate with microtubules. We previously showed that gene-trap knockout of Specc1l in mouse results in early embryonic lethality. We now present a truncation mutant mouse allele, Specc1lΔC510, that results in perinatal lethality. Specc1lΔC510/ΔC510 homozygotes showed abnormal palate rugae but did not show cleft palate. However, when crossed with a gene-trap allele, Specc1lcGT/ΔC510 compound heterozygotes showed a palate elevation delay with incompletely penetrant cleft palate. Specc1lcGT/ΔC510 embryos exhibit transient oral epithelial adhesions at E13.5, which may delay shelf elevation. Consistent with oral adhesions, we show periderm layer abnormalities, including ectopic apical expression of adherens junction markers, similar to Irf6 hypomorphic mutants and Arhgap29 heterozygotes. Indeed, SPECC1L expression is drastically reduced in Irf6 mutant palatal shelves. Finally, we wanted to determine if SPECC1L deficiency also contributed to non-syndromic (ns) CL/P. We sequenced 62 Caucasian, 89 Filipino, 90 Ethiopian, 90 Nigerian and 95 Japanese patients with nsCL/P and identified three rare coding variants (p.Ala86Thr, p.Met91Iso and p.Arg546Gln) in six individuals. These variants reside outside of SPECC1L coiled-coil domains and result in milder functional defects than variants associated with syndromic clefting. Together, our data indicate that palate elevation is sensitive to deficiency of SPECC1L dosage and function and that SPECC1L cytoskeletal protein functions downstream of IRF6 in palatogenesis.

Original language	English (US)
Pages (from-to)	845-858
Number of pages	14
Journal	Human molecular genetics
Volume	29
Issue number	5
DOIs	https://doi.org/10.1093/hmg/ddaa002
State	Published - Mar 1 2020

ASJC Scopus subject areas

Molecular Biology
Genetics
Genetics(clinical)

Access to Document

10.1093/hmg/ddaa002

Cite this

Hall, E. G., Wenger, L. W., Wilson, N. R., Undurty-Akella, S. S., Standley, J., Augustine-Akpan, E. A., Kousa, Y. A., Acevedo, D. S., Goering, J. P., Pitstick, L., Natsume, N., Paroya, S. M., Busch, T. D., Ito, M., Mori, A., Imura, H., Schultz-Rogers, L. E., Klee, E. W., Babovic-Vuksanovic, D., ... Saadi, I. (2020). SPECC1L regulates palate development downstream of IRF6. Human molecular genetics, 29(5), 845-858. https://doi.org/10.1093/hmg/ddaa002

Hall, EG, Wenger, LW, Wilson, NR, Undurty-Akella, SS, Standley, J, Augustine-Akpan, EA, Kousa, YA, Acevedo, DS, Goering, JP, Pitstick, L, Natsume, N, Paroya, SM, Busch, TD, Ito, M, Mori, A, Imura, H, Schultz-Rogers, LE, Klee, EW , Babovic-Vuksanovic, D, Kroc, SA, Adeyemo, WL, Eshete, MA, Bjork, BC, Suzuki, S, Murray, JC, Schutte, BC, Butali, A & Saadi, I 2020, 'SPECC1L regulates palate development downstream of IRF6', Human molecular genetics, vol. 29, no. 5, pp. 845-858. https://doi.org/10.1093/hmg/ddaa002

@article{4b1c010c7d9f4a63b767aaca9be90928,

title = "SPECC1L regulates palate development downstream of IRF6",

abstract = "SPECC1L mutations have been identified in patients with rare atypical orofacial clefts and with syndromic cleft lip and/or palate (CL/P). These mutations cluster in the second coiled-coil and calponin homology domains of SPECC1L and severely affect the ability of SPECC1L to associate with microtubules. We previously showed that gene-trap knockout of Specc1l in mouse results in early embryonic lethality. We now present a truncation mutant mouse allele, Specc1lΔC510, that results in perinatal lethality. Specc1lΔC510/ΔC510 homozygotes showed abnormal palate rugae but did not show cleft palate. However, when crossed with a gene-trap allele, Specc1lcGT/ΔC510 compound heterozygotes showed a palate elevation delay with incompletely penetrant cleft palate. Specc1lcGT/ΔC510 embryos exhibit transient oral epithelial adhesions at E13.5, which may delay shelf elevation. Consistent with oral adhesions, we show periderm layer abnormalities, including ectopic apical expression of adherens junction markers, similar to Irf6 hypomorphic mutants and Arhgap29 heterozygotes. Indeed, SPECC1L expression is drastically reduced in Irf6 mutant palatal shelves. Finally, we wanted to determine if SPECC1L deficiency also contributed to non-syndromic (ns) CL/P. We sequenced 62 Caucasian, 89 Filipino, 90 Ethiopian, 90 Nigerian and 95 Japanese patients with nsCL/P and identified three rare coding variants (p.Ala86Thr, p.Met91Iso and p.Arg546Gln) in six individuals. These variants reside outside of SPECC1L coiled-coil domains and result in milder functional defects than variants associated with syndromic clefting. Together, our data indicate that palate elevation is sensitive to deficiency of SPECC1L dosage and function and that SPECC1L cytoskeletal protein functions downstream of IRF6 in palatogenesis.",

author = "Hall, {Everett G.} and Wenger, {Luke W.} and Wilson, {Nathan R.} and Undurty-Akella, {Sraavya S.} and Jennifer Standley and Augustine-Akpan, {Eno Abasi} and Kousa, {Youssef A.} and Acevedo, {Diana S.} and Goering, {Jeremy P.} and Lenore Pitstick and Nagato Natsume and Paroya, {Shahnawaz M.} and Busch, {Tamara D.} and Masaaki Ito and Akihiro Mori and Hideto Imura and Schultz-Rogers, {Laura E.} and Klee, {Eric W.} and Dusica Babovic-Vuksanovic and Kroc, {Sarah A.} and Adeyemo, {Wasiu L.} and Eshete, {Mekonen A.} and Bjork, {Bryan C.} and Satoshi Suzuki and Murray, {Jeffrey C.} and Schutte, {Brian C.} and Azeez Butali and Irfan Saadi",

note = "Funding Information: National Institutes of Health (DE026172 to I.S., DE022378 to A.B., GM102801 to A.C., F31DE027284 to E.H.); Robert Wood Johnson Foundation (72429); JSPS KAKENHI (JP24249092, JP26861757, JP17K11863); Center of Biomedical Research Excellence (COBRE) (National Institute of General Medical Sciences P20 GM104936); Kansas IDeA Network for Biomedical Research Excellence (National Institute of General Medical Sciences P20 GM103418); Kansas Intellectual and Developmental Disabilities Research Center (KIDDRC) (U54 Eunice Kennedy Shriver National Institute of Child Health and Human Development, HD 090216); the Confocal Imaging Facility, the Integrated Imaging Core, and the Transgenic and Gene Targeting Institutional Facility at the University of Kansas Medical Center are supported, in part, by NIH/NIGMS COBRE (P30GM122731) and by NIH/NICHD KIDDRC (U54HD090216). Publisher Copyright: {\textcopyright} 2020 The Author(s) 2020.",

year = "2020",

month = mar,

day = "1",

doi = "10.1093/hmg/ddaa002",

language = "English (US)",

volume = "29",

pages = "845--858",

journal = "Human molecular genetics",

issn = "0964-6906",

publisher = "Oxford University Press",

number = "5",

}

TY - JOUR

T1 - SPECC1L regulates palate development downstream of IRF6

AU - Hall, Everett G.

AU - Wenger, Luke W.

AU - Wilson, Nathan R.

AU - Undurty-Akella, Sraavya S.

AU - Standley, Jennifer

AU - Augustine-Akpan, Eno Abasi

AU - Kousa, Youssef A.

AU - Acevedo, Diana S.

AU - Goering, Jeremy P.

AU - Pitstick, Lenore

AU - Natsume, Nagato

AU - Paroya, Shahnawaz M.

AU - Busch, Tamara D.

AU - Ito, Masaaki

AU - Mori, Akihiro

AU - Imura, Hideto

AU - Schultz-Rogers, Laura E.

AU - Klee, Eric W.

AU - Babovic-Vuksanovic, Dusica

AU - Kroc, Sarah A.

AU - Adeyemo, Wasiu L.

AU - Eshete, Mekonen A.

AU - Bjork, Bryan C.

AU - Suzuki, Satoshi

AU - Murray, Jeffrey C.

AU - Schutte, Brian C.

AU - Butali, Azeez

AU - Saadi, Irfan

N1 - Funding Information: National Institutes of Health (DE026172 to I.S., DE022378 to A.B., GM102801 to A.C., F31DE027284 to E.H.); Robert Wood Johnson Foundation (72429); JSPS KAKENHI (JP24249092, JP26861757, JP17K11863); Center of Biomedical Research Excellence (COBRE) (National Institute of General Medical Sciences P20 GM104936); Kansas IDeA Network for Biomedical Research Excellence (National Institute of General Medical Sciences P20 GM103418); Kansas Intellectual and Developmental Disabilities Research Center (KIDDRC) (U54 Eunice Kennedy Shriver National Institute of Child Health and Human Development, HD 090216); the Confocal Imaging Facility, the Integrated Imaging Core, and the Transgenic and Gene Targeting Institutional Facility at the University of Kansas Medical Center are supported, in part, by NIH/NIGMS COBRE (P30GM122731) and by NIH/NICHD KIDDRC (U54HD090216). Publisher Copyright: © 2020 The Author(s) 2020.

PY - 2020/3/1

Y1 - 2020/3/1

N2 - SPECC1L mutations have been identified in patients with rare atypical orofacial clefts and with syndromic cleft lip and/or palate (CL/P). These mutations cluster in the second coiled-coil and calponin homology domains of SPECC1L and severely affect the ability of SPECC1L to associate with microtubules. We previously showed that gene-trap knockout of Specc1l in mouse results in early embryonic lethality. We now present a truncation mutant mouse allele, Specc1lΔC510, that results in perinatal lethality. Specc1lΔC510/ΔC510 homozygotes showed abnormal palate rugae but did not show cleft palate. However, when crossed with a gene-trap allele, Specc1lcGT/ΔC510 compound heterozygotes showed a palate elevation delay with incompletely penetrant cleft palate. Specc1lcGT/ΔC510 embryos exhibit transient oral epithelial adhesions at E13.5, which may delay shelf elevation. Consistent with oral adhesions, we show periderm layer abnormalities, including ectopic apical expression of adherens junction markers, similar to Irf6 hypomorphic mutants and Arhgap29 heterozygotes. Indeed, SPECC1L expression is drastically reduced in Irf6 mutant palatal shelves. Finally, we wanted to determine if SPECC1L deficiency also contributed to non-syndromic (ns) CL/P. We sequenced 62 Caucasian, 89 Filipino, 90 Ethiopian, 90 Nigerian and 95 Japanese patients with nsCL/P and identified three rare coding variants (p.Ala86Thr, p.Met91Iso and p.Arg546Gln) in six individuals. These variants reside outside of SPECC1L coiled-coil domains and result in milder functional defects than variants associated with syndromic clefting. Together, our data indicate that palate elevation is sensitive to deficiency of SPECC1L dosage and function and that SPECC1L cytoskeletal protein functions downstream of IRF6 in palatogenesis.

AB - SPECC1L mutations have been identified in patients with rare atypical orofacial clefts and with syndromic cleft lip and/or palate (CL/P). These mutations cluster in the second coiled-coil and calponin homology domains of SPECC1L and severely affect the ability of SPECC1L to associate with microtubules. We previously showed that gene-trap knockout of Specc1l in mouse results in early embryonic lethality. We now present a truncation mutant mouse allele, Specc1lΔC510, that results in perinatal lethality. Specc1lΔC510/ΔC510 homozygotes showed abnormal palate rugae but did not show cleft palate. However, when crossed with a gene-trap allele, Specc1lcGT/ΔC510 compound heterozygotes showed a palate elevation delay with incompletely penetrant cleft palate. Specc1lcGT/ΔC510 embryos exhibit transient oral epithelial adhesions at E13.5, which may delay shelf elevation. Consistent with oral adhesions, we show periderm layer abnormalities, including ectopic apical expression of adherens junction markers, similar to Irf6 hypomorphic mutants and Arhgap29 heterozygotes. Indeed, SPECC1L expression is drastically reduced in Irf6 mutant palatal shelves. Finally, we wanted to determine if SPECC1L deficiency also contributed to non-syndromic (ns) CL/P. We sequenced 62 Caucasian, 89 Filipino, 90 Ethiopian, 90 Nigerian and 95 Japanese patients with nsCL/P and identified three rare coding variants (p.Ala86Thr, p.Met91Iso and p.Arg546Gln) in six individuals. These variants reside outside of SPECC1L coiled-coil domains and result in milder functional defects than variants associated with syndromic clefting. Together, our data indicate that palate elevation is sensitive to deficiency of SPECC1L dosage and function and that SPECC1L cytoskeletal protein functions downstream of IRF6 in palatogenesis.

UR - http://www.scopus.com/inward/record.url?scp=85082563462&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85082563462&partnerID=8YFLogxK

U2 - 10.1093/hmg/ddaa002

DO - 10.1093/hmg/ddaa002

M3 - Article

C2 - 31943082

AN - SCOPUS:85082563462

SN - 0964-6906

VL - 29

SP - 845

EP - 858

JO - Human molecular genetics

JF - Human molecular genetics

IS - 5

ER -

SPECC1L regulates palate development downstream of IRF6

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this