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PIGO variants in a boy with features of Mabry syndrome who also exhibits Fryns syndrome with peripheral neuropathy

We report a 2‐year‐old boy with left congenital diaphragmatic defect (CDH), pulmonary hypoplasia, and polyhydramnios who harbors compound heterozygous mutations, c.1109A>G and c.2497_2498del, in the PIGO gene. The facial appearance was characterized by cloudy cornea, broad and flat nasal bridge,...

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Published in:	American journal of medical genetics. Part A 2021-03, Vol.185 (3), p.845-849
Main Authors:	Okuda, Taro, Yonekawa, Takahiro, Murakami, Yoshiko, Kinoshita, Taroh, Ito, Takahiro, Matsushita, Kohei, Koike, Yuhki, Inoue, Mikihiro, Uchida, Keiichi, Yodoya, Noriko, Ohashi, Hiroyuki, Sawada, Hirofumi, Iwamoto, Shotaro, Mitani, Yoshihide, Hirayama, Masahiro
Format:	Article
Language:	English
Subjects:	Alkaline phosphatase CD16 antigen CD59 antigen Cell surface Cornea Cryptorchidism Demyelination Electrophysiology Ethanolamine Fryns syndrome Glycosylphosphatidylinositol glycosylphosphatidylinositol (GPI) Hirschsprung's disease Hyperphosphatasia Hypoplasia Immunoglobulin D inherited GPI deficiency (IGD) Leukocytes (granulocytic) Mutation Peripheral neuropathy PIGO
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container_title	American journal of medical genetics. Part A
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creator	Okuda, Taro Yonekawa, Takahiro Murakami, Yoshiko Kinoshita, Taroh Ito, Takahiro Matsushita, Kohei Koike, Yuhki Inoue, Mikihiro Uchida, Keiichi Yodoya, Noriko Ohashi, Hiroyuki Sawada, Hirofumi Iwamoto, Shotaro Mitani, Yoshihide Hirayama, Masahiro
description	We report a 2‐year‐old boy with left congenital diaphragmatic defect (CDH), pulmonary hypoplasia, and polyhydramnios who harbors compound heterozygous mutations, c.1109A>G and c.2497_2498del, in the PIGO gene. The facial appearance was characterized by cloudy cornea, broad and flat nasal bridge, long philtrum, low‐set ears, and micrognathia. Serum alkaline phosphatase level was consistently elevated, suggesting that he meets the criteria for Mabry syndrome. However, the observation of other anomalies including micropenis, cryptorchidism, and Hirschsprung disease suggests clinical features compatible with Fryns syndrome (FS). Left CDH and Hirschsprung disease were surgically repaired at 1 week and 3 months of age, respectively. He also exhibited multiple joint contractures and markedly decreased voluntary movement. Craw hands were seen but pes cavus was absent. Electrophysiology studies showed diffuse axonal demyelinating neuropathy. The cell surface expression of CD16, CD24, and CD59 on blood granulocytes was significantly reduced. The PIGO gene encodes ethanolamine phosphate transferase 3 in the glycosylphosphatidylinositol (GPI) biosynthesis pathway. Mutations in the gene are known to cause Mabry syndrome, an inherited GPI deficiency (IGD) characterized by hyperphosphatasia. IGDs show clinical heterogeneity and overlap with other syndromes and diseases. A severe end of the phenotypic spectrum can be recognized as FS. This is the first report of PIGO gene mutations in a Mabry syndrome patient who also meets the criteria for FS.
doi_str_mv	10.1002/ajmg.a.62005
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The facial appearance was characterized by cloudy cornea, broad and flat nasal bridge, long philtrum, low‐set ears, and micrognathia. Serum alkaline phosphatase level was consistently elevated, suggesting that he meets the criteria for Mabry syndrome. However, the observation of other anomalies including micropenis, cryptorchidism, and Hirschsprung disease suggests clinical features compatible with Fryns syndrome (FS). Left CDH and Hirschsprung disease were surgically repaired at 1 week and 3 months of age, respectively. He also exhibited multiple joint contractures and markedly decreased voluntary movement. Craw hands were seen but pes cavus was absent. Electrophysiology studies showed diffuse axonal demyelinating neuropathy. The cell surface expression of CD16, CD24, and CD59 on blood granulocytes was significantly reduced. The PIGO gene encodes ethanolamine phosphate transferase 3 in the glycosylphosphatidylinositol (GPI) biosynthesis pathway. Mutations in the gene are known to cause Mabry syndrome, an inherited GPI deficiency (IGD) characterized by hyperphosphatasia. IGDs show clinical heterogeneity and overlap with other syndromes and diseases. A severe end of the phenotypic spectrum can be recognized as FS. This is the first report of PIGO gene mutations in a Mabry syndrome patient who also meets the criteria for FS.</description><identifier>ISSN: 1552-4825</identifier><identifier>EISSN: 1552-4833</identifier><identifier>DOI: 10.1002/ajmg.a.62005</identifier><language>eng</language><publisher>Hoboken, USA: John Wiley & Sons, Inc</publisher><subject>Alkaline phosphatase ; CD16 antigen ; CD59 antigen ; Cell surface ; Cornea ; Cryptorchidism ; Demyelination ; Electrophysiology ; Ethanolamine ; Fryns syndrome ; Glycosylphosphatidylinositol ; glycosylphosphatidylinositol (GPI) ; Hirschsprung's disease ; Hyperphosphatasia ; Hypoplasia ; Immunoglobulin D ; inherited GPI deficiency (IGD) ; Leukocytes (granulocytic) ; Mutation ; Peripheral neuropathy ; PIGO</subject><ispartof>American journal of medical genetics. 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The cell surface expression of CD16, CD24, and CD59 on blood granulocytes was significantly reduced. The PIGO gene encodes ethanolamine phosphate transferase 3 in the glycosylphosphatidylinositol (GPI) biosynthesis pathway. Mutations in the gene are known to cause Mabry syndrome, an inherited GPI deficiency (IGD) characterized by hyperphosphatasia. IGDs show clinical heterogeneity and overlap with other syndromes and diseases. A severe end of the phenotypic spectrum can be recognized as FS. This is the first report of PIGO gene mutations in a Mabry syndrome patient who also meets the criteria for FS.</description><subject>Alkaline phosphatase</subject><subject>CD16 antigen</subject><subject>CD59 antigen</subject><subject>Cell surface</subject><subject>Cornea</subject><subject>Cryptorchidism</subject><subject>Demyelination</subject><subject>Electrophysiology</subject><subject>Ethanolamine</subject><subject>Fryns syndrome</subject><subject>Glycosylphosphatidylinositol</subject><subject>glycosylphosphatidylinositol (GPI)</subject><subject>Hirschsprung's disease</subject><subject>Hyperphosphatasia</subject><subject>Hypoplasia</subject><subject>Immunoglobulin D</subject><subject>inherited GPI deficiency (IGD)</subject><subject>Leukocytes (granulocytic)</subject><subject>Mutation</subject><subject>Peripheral neuropathy</subject><subject>PIGO</subject><issn>1552-4825</issn><issn>1552-4833</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2021</creationdate><recordtype>article</recordtype><recordid>eNp9kLFOwzAQhi0EEqWw8QCWWEmxnThOx6qipaioDDBb58Qhrto42AnFb09KEGJiutPp-_-TPoSuKZlQQtgdbPdvE5ikjBB-gkaUcxYlWRyf_u6Mn6ML77eExISLdITc82q5wR_gDNStx6bGgJUN-GDaCpca2s5pj22Jn0C5gH2oC2f3Gh8qi2HnLdaflVGmjy5cqP0f4FjQaGeaSjvY4Vp3zjbQVuESnZV9VF_9zDF6Xdy_zB-i9Wa5ms_WUc5SziOmWQKQ5ypNYh1nVDBQJeP9WdGClYUqRF7mhGeKTpnQmkxzRokoEs5BxEkRj9HN0Ns4-95p38qt7Vzdv5QsyQQTRFDWU7cDlTvrvdOlbJzZgwuSEnm0Ko9WJchvqz2eDPjB7HT4l5Wzx6flbIh9Ae2VfTk</recordid><startdate>202103</startdate><enddate>202103</enddate><creator>Okuda, Taro</creator><creator>Yonekawa, Takahiro</creator><creator>Murakami, Yoshiko</creator><creator>Kinoshita, Taroh</creator><creator>Ito, Takahiro</creator><creator>Matsushita, Kohei</creator><creator>Koike, Yuhki</creator><creator>Inoue, Mikihiro</creator><creator>Uchida, Keiichi</creator><creator>Yodoya, Noriko</creator><creator>Ohashi, Hiroyuki</creator><creator>Sawada, Hirofumi</creator><creator>Iwamoto, Shotaro</creator><creator>Mitani, Yoshihide</creator><creator>Hirayama, Masahiro</creator><general>John Wiley & Sons, Inc</general><general>Wiley Subscription Services, Inc</general><scope>AAYXX</scope><scope>CITATION</scope><scope>7QP</scope><scope>7TK</scope><scope>8FD</scope><scope>FR3</scope><scope>K9.</scope><scope>P64</scope><scope>RC3</scope><orcidid>https://orcid.org/0000-0001-7663-5668</orcidid></search><sort><creationdate>202103</creationdate><title>PIGO variants in a boy with features of Mabry syndrome who also exhibits Fryns syndrome with peripheral neuropathy</title><author>Okuda, Taro ; 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He also exhibited multiple joint contractures and markedly decreased voluntary movement. Craw hands were seen but pes cavus was absent. Electrophysiology studies showed diffuse axonal demyelinating neuropathy. The cell surface expression of CD16, CD24, and CD59 on blood granulocytes was significantly reduced. The PIGO gene encodes ethanolamine phosphate transferase 3 in the glycosylphosphatidylinositol (GPI) biosynthesis pathway. Mutations in the gene are known to cause Mabry syndrome, an inherited GPI deficiency (IGD) characterized by hyperphosphatasia. IGDs show clinical heterogeneity and overlap with other syndromes and diseases. A severe end of the phenotypic spectrum can be recognized as FS. 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subjects	Alkaline phosphatase CD16 antigen CD59 antigen Cell surface Cornea Cryptorchidism Demyelination Electrophysiology Ethanolamine Fryns syndrome Glycosylphosphatidylinositol glycosylphosphatidylinositol (GPI) Hirschsprung's disease Hyperphosphatasia Hypoplasia Immunoglobulin D inherited GPI deficiency (IGD) Leukocytes (granulocytic) Mutation Peripheral neuropathy PIGO
title	PIGO variants in a boy with features of Mabry syndrome who also exhibits Fryns syndrome with peripheral neuropathy
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