Functional analysis of BMP4 mutations identified in pediatric CAKUT patients

Mansoureh Tabatabaeifar; Karl Peter Schlingmann; Mieczyslaw Litwin; Sevinc Emre; Aysin Bakkaloglu; Otto Mehls; Corinne Antignac; Franz Schaefer; Stefanie Weber; A. Anarat; F. Ozaltin; A. Peco-Antic; U. Querfeld; J. Gellermann; P. Sallay; D. Drozdz; K. E. Bonzel; A. M. Wingen; A. Zurowska; I. Balasz; F. Perfumo; A. Canepa; D. E. Müller-Wiefel; K. Zepf; G. Offner; B. Enke; E. Wühl; C. Hadtstein; U. Berg; G. Celsi; A. Sirin; I. Bilge; S. Çaliskan; S. Mir; E. Serdaroglu; C. Greiner; H. Eichstädt; S. Wygoda; K. Hohbach-Hohenfellner; N. Jeck; G. Klaus; A. Appiani; G. Ardissino; S. Testa; G. Montini; P. Niaudet; M. Charbit; J. Dusek; A. Caldas-Afonso; A. Teixeira; S. Picca; C. Matteucci; M. Wigger; M. Fischbach; J. Terzic; J. Fydryk; T. Urasinski; R. Coppo; L. Peruzzi; A. Jankauskiene; M. Abuauba; R. Grenda; K. Arbeiter; T. J. Neuhaus

doi:10.1007/s00467-009-1287-6

Functional analysis of BMP4 mutations identified in pediatric CAKUT patients

Mansoureh Tabatabaeifar
, Karl Peter Schlingmann
, Mieczyslaw Litwin
, Sevinc Emre
, Aysin Bakkaloglu
, Otto Mehls
, Corinne Antignac
, Franz Schaefer
, Stefanie Weber
, A. Anarat
, F. Ozaltin
, A. Peco-Antic
, U. Querfeld
, J. Gellermann
, P. Sallay
, D. Drozdz
, K. E. Bonzel
, A. M. Wingen
, A. Zurowska
, I. Balasz

F. Perfumo, A. Canepa, D. E. Müller-Wiefel, K. Zepf, G. Offner, B. Enke, E. Wühl, C. Hadtstein, U. Berg, G. Celsi, A. Sirin, I. Bilge, S. Çaliskan, S. Mir, E. Serdaroglu, C. Greiner, H. Eichstädt, S. Wygoda, K. Hohbach-Hohenfellner, N. Jeck, G. Klaus, A. Appiani, G. Ardissino, S. Testa, G. Montini, P. Niaudet, M. Charbit, J. Dusek, A. Caldas-Afonso, A. Teixeira, S. Picca, C. Matteucci, M. Wigger, M. Fischbach, J. Terzic, J. Fydryk, T. Urasinski, R. Coppo, L. Peruzzi, A. Jankauskiene, M. Abuauba, R. Grenda, K. Arbeiter, T. J. Neuhaus

Araştırma sonucu: Dergiye katkı › Makale › bilirkişi

42 Alıntılar (Scopus)

Özet

Human congenital anomalies of the kidney and urinary tract (CAKUT) represent the major causes of chronic renal failure (CRF) in children. This set of disorders comprises renal agenesis, hypoplasia, dysplastic or double kidneys, and/or malformations of the ureter. It has recently been shown that mutations in several genes, among them BMP4, are associated with hereditary renal developmental diseases. In BMP4, we formerly identified three missense mutations (S91C, T116S, N150K) in five pediatric CAKUT patients. These BMP4 mutations were subsequently studied in a cellular expression system, and here we present functional data demonstrating a lower level of messenger RNA (mRNA) abundance in Bmp4 mutants that indicates a possible negative feedback of the mutants on their own mRNA expression and/or stability. Furthermore, we describe the formation of alternative protein complexes induced by the S91C-BMP4mutation, which results in perinuclear endoplasmic reticulum (ER) accumulation and enhanced lysosomal degradation of Bmp4. This work further supports the role of mutations in BMP4for abnormalities of human kidney development.

Orijinal dil	İngilizce
Sayfa (başlangıç-bitiş)	2361-2368
Sayfa sayısı	8
Dergi	Pediatric Nephrology
Hacim	24
Basın numarası	12
DOI'lar	https://doi.org/10.1007/s00467-009-1287-6
Yayın durumu	Yayınlandı - 2009

BM SKH

Bu sonuç, aşağıdaki Sürdürülebilir Kalkınma Hedefine/Hedeflerine katkıda bulunur

SKH 3 Sağlık ve Kaliteli Yaşam

Belgeye Erişim

10.1007/s00467-009-1287-6

Diger dosyalar ve linkler

Link to publication in Scopus

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Tabatabaeifar, M., Schlingmann, K. P., Litwin, M., Emre, S., Bakkaloglu, A., Mehls, O., Antignac, C., Schaefer, F., Weber, S., Anarat, A., Ozaltin, F., Peco-Antic, A., Querfeld, U., Gellermann, J., Sallay, P., Drozdz, D., Bonzel, K. E., Wingen, A. M., Zurowska, A., ... Neuhaus, T. J. (2009). Functional analysis of BMP4 mutations identified in pediatric CAKUT patients. Pediatric Nephrology, 24(12), 2361-2368. https://doi.org/10.1007/s00467-009-1287-6

@article{8d8fb1eb382e45f4b02b923b435f158d,

title = "Functional analysis of BMP4 mutations identified in pediatric CAKUT patients",

abstract = "Human congenital anomalies of the kidney and urinary tract (CAKUT) represent the major causes of chronic renal failure (CRF) in children. This set of disorders comprises renal agenesis, hypoplasia, dysplastic or double kidneys, and/or malformations of the ureter. It has recently been shown that mutations in several genes, among them BMP4, are associated with hereditary renal developmental diseases. In BMP4, we formerly identified three missense mutations (S91C, T116S, N150K) in five pediatric CAKUT patients. These BMP4 mutations were subsequently studied in a cellular expression system, and here we present functional data demonstrating a lower level of messenger RNA (mRNA) abundance in Bmp4 mutants that indicates a possible negative feedback of the mutants on their own mRNA expression and/or stability. Furthermore, we describe the formation of alternative protein complexes induced by the S91C-BMP4mutation, which results in perinuclear endoplasmic reticulum (ER) accumulation and enhanced lysosomal degradation of Bmp4. This work further supports the role of mutations in BMP4for abnormalities of human kidney development.",

keywords = "Abnormal protein complex, Bone morphogenetic protein 4, CAKUT, Kidney development, Subcellular localization",

author = "Mansoureh Tabatabaeifar and Schlingmann, \{Karl Peter\} and Mieczyslaw Litwin and Sevinc Emre and Aysin Bakkaloglu and Otto Mehls and Corinne Antignac and Franz Schaefer and Stefanie Weber and A. Anarat and F. Ozaltin and A. Peco-Antic and U. Querfeld and J. Gellermann and P. Sallay and D. Drozdz and Bonzel, \{K. E.\} and Wingen, \{A. M.\} and A. Zurowska and I. Balasz and F. Perfumo and A. Canepa and M{\"u}ller-Wiefel, \{D. E.\} and K. Zepf and G. Offner and B. Enke and E. W{\"u}hl and C. Hadtstein and U. Berg and G. Celsi and A. Sirin and I. Bilge and S. {\c C}aliskan and S. Mir and E. Serdaroglu and C. Greiner and H. Eichst{\"a}dt and S. Wygoda and K. Hohbach-Hohenfellner and N. Jeck and G. Klaus and A. Appiani and G. Ardissino and S. Testa and G. Montini and P. Niaudet and M. Charbit and J. Dusek and A. Caldas-Afonso and A. Teixeira and S. Picca and C. Matteucci and M. Wigger and M. Fischbach and J. Terzic and J. Fydryk and T. Urasinski and R. Coppo and L. Peruzzi and A. Jankauskiene and M. Abuauba and R. Grenda and K. Arbeiter and Neuhaus, \{T. J.\}",

year = "2009",

doi = "10.1007/s00467-009-1287-6",

language = "English",

volume = "24",

pages = "2361--2368",

journal = "Pediatric Nephrology",

issn = "0931-041X",

publisher = "Springer Science and Business Media Deutschland GmbH",

number = "12",

}

Tabatabaeifar, M, Schlingmann, KP, Litwin, M, Emre, S, Bakkaloglu, A, Mehls, O, Antignac, C, Schaefer, F, Weber, S, Anarat, A, Ozaltin, F, Peco-Antic, A, Querfeld, U, Gellermann, J, Sallay, P, Drozdz, D, Bonzel, KE, Wingen, AM, Zurowska, A, Balasz, I, Perfumo, F, Canepa, A, Müller-Wiefel, DE, Zepf, K, Offner, G, Enke, B, Wühl, E, Hadtstein, C, Berg, U, Celsi, G, Sirin, A, Bilge, I, Çaliskan, S, Mir, S, Serdaroglu, E, Greiner, C, Eichstädt, H, Wygoda, S, Hohbach-Hohenfellner, K, Jeck, N, Klaus, G, Appiani, A, Ardissino, G, Testa, S, Montini, G, Niaudet, P, Charbit, M, Dusek, J, Caldas-Afonso, A, Teixeira, A, Picca, S, Matteucci, C, Wigger, M, Fischbach, M, Terzic, J, Fydryk, J, Urasinski, T, Coppo, R, Peruzzi, L, Jankauskiene, A, Abuauba, M, Grenda, R, Arbeiter, K & Neuhaus, TJ 2009, 'Functional analysis of BMP4 mutations identified in pediatric CAKUT patients', Pediatric Nephrology, hac. 24, no. 12, pp. 2361-2368. https://doi.org/10.1007/s00467-009-1287-6

TY - JOUR

T1 - Functional analysis of BMP4 mutations identified in pediatric CAKUT patients

AU - Tabatabaeifar, Mansoureh

AU - Schlingmann, Karl Peter

AU - Litwin, Mieczyslaw

AU - Emre, Sevinc

AU - Bakkaloglu, Aysin

AU - Mehls, Otto

AU - Antignac, Corinne

AU - Schaefer, Franz

AU - Weber, Stefanie

AU - Anarat, A.

AU - Ozaltin, F.

AU - Peco-Antic, A.

AU - Querfeld, U.

AU - Gellermann, J.

AU - Sallay, P.

AU - Drozdz, D.

AU - Bonzel, K. E.

AU - Wingen, A. M.

AU - Zurowska, A.

AU - Balasz, I.

AU - Perfumo, F.

AU - Canepa, A.

AU - Müller-Wiefel, D. E.

AU - Zepf, K.

AU - Offner, G.

AU - Enke, B.

AU - Wühl, E.

AU - Hadtstein, C.

AU - Berg, U.

AU - Celsi, G.

AU - Sirin, A.

AU - Bilge, I.

AU - Çaliskan, S.

AU - Mir, S.

AU - Serdaroglu, E.

AU - Greiner, C.

AU - Eichstädt, H.

AU - Wygoda, S.

AU - Hohbach-Hohenfellner, K.

AU - Jeck, N.

AU - Klaus, G.

AU - Appiani, A.

AU - Ardissino, G.

AU - Testa, S.

AU - Montini, G.

AU - Niaudet, P.

AU - Charbit, M.

AU - Dusek, J.

AU - Caldas-Afonso, A.

AU - Teixeira, A.

AU - Picca, S.

AU - Matteucci, C.

AU - Wigger, M.

AU - Fischbach, M.

AU - Terzic, J.

AU - Fydryk, J.

AU - Urasinski, T.

AU - Coppo, R.

AU - Peruzzi, L.

AU - Jankauskiene, A.

AU - Abuauba, M.

AU - Grenda, R.

AU - Arbeiter, K.

AU - Neuhaus, T. J.

PY - 2009

Y1 - 2009

N2 - Human congenital anomalies of the kidney and urinary tract (CAKUT) represent the major causes of chronic renal failure (CRF) in children. This set of disorders comprises renal agenesis, hypoplasia, dysplastic or double kidneys, and/or malformations of the ureter. It has recently been shown that mutations in several genes, among them BMP4, are associated with hereditary renal developmental diseases. In BMP4, we formerly identified three missense mutations (S91C, T116S, N150K) in five pediatric CAKUT patients. These BMP4 mutations were subsequently studied in a cellular expression system, and here we present functional data demonstrating a lower level of messenger RNA (mRNA) abundance in Bmp4 mutants that indicates a possible negative feedback of the mutants on their own mRNA expression and/or stability. Furthermore, we describe the formation of alternative protein complexes induced by the S91C-BMP4mutation, which results in perinuclear endoplasmic reticulum (ER) accumulation and enhanced lysosomal degradation of Bmp4. This work further supports the role of mutations in BMP4for abnormalities of human kidney development.

AB - Human congenital anomalies of the kidney and urinary tract (CAKUT) represent the major causes of chronic renal failure (CRF) in children. This set of disorders comprises renal agenesis, hypoplasia, dysplastic or double kidneys, and/or malformations of the ureter. It has recently been shown that mutations in several genes, among them BMP4, are associated with hereditary renal developmental diseases. In BMP4, we formerly identified three missense mutations (S91C, T116S, N150K) in five pediatric CAKUT patients. These BMP4 mutations were subsequently studied in a cellular expression system, and here we present functional data demonstrating a lower level of messenger RNA (mRNA) abundance in Bmp4 mutants that indicates a possible negative feedback of the mutants on their own mRNA expression and/or stability. Furthermore, we describe the formation of alternative protein complexes induced by the S91C-BMP4mutation, which results in perinuclear endoplasmic reticulum (ER) accumulation and enhanced lysosomal degradation of Bmp4. This work further supports the role of mutations in BMP4for abnormalities of human kidney development.

KW - Abnormal protein complex

KW - Bone morphogenetic protein 4

KW - CAKUT

KW - Kidney development

KW - Subcellular localization

UR - https://www.scopus.com/pages/publications/70350692080

U2 - 10.1007/s00467-009-1287-6

DO - 10.1007/s00467-009-1287-6

M3 - Article

C2 - 19685083

AN - SCOPUS:70350692080

SN - 0931-041X

VL - 24

SP - 2361

EP - 2368

JO - Pediatric Nephrology

JF - Pediatric Nephrology

IS - 12

ER -

Functional analysis of BMP4 mutations identified in pediatric CAKUT patients

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