Establishment of a Knock-In Mouse Model with the SLC26A4 c.919-2A>G Mutation and Characterization of Its Pathology

被引:44
作者
Lu, Ying-Chang [1 ,2 ]
Wu, Chen-Chi [2 ,3 ,4 ]
Shen, Wen-Sheng [2 ]
Yang, Ting-Hua [2 ]
Yeh, Te-Huei [2 ]
Chen, Pei-Jer [3 ]
Yu, I-Shing [5 ]
Lin, Shu-Wha [5 ]
Wong, Jau-Min [1 ]
Chang, Qing [6 ]
Lin, Xi [6 ]
Hsu, Chuan-Jen [2 ,7 ]
机构
[1] Natl Taiwan Univ, Inst Biomed Engn, Taipei 10764, Taiwan
[2] Natl Taiwan Univ Hosp, Dept Otolaryngol, Taipei, Taiwan
[3] Natl Taiwan Univ, Coll Med, Grad Inst Clin Med, Taipei 10764, Taiwan
[4] Natl Taiwan Univ Hosp, Dept Med Genet, Taipei, Taiwan
[5] Natl Taiwan Univ, Res Ctr Med Excellence, Div Genom Med, Taipei 10764, Taiwan
[6] Emory Univ Sch Med, Dept Otolaryngol, Atlanta, GA USA
[7] Natl Taiwan Univ, Coll Med, Dept Otolaryngol, Taipei 10764, Taiwan
来源
PLOS ONE | 2011年 / 6卷 / 07期
关键词
ENLARGED VESTIBULAR AQUEDUCT; GENOTYPE-PHENOTYPE CORRELATION; NONSYNDROMIC HEARING-LOSS; PENDRED-SYNDROME; INNER-EAR; MONDINI DYSPLASIA; PDS GENE; UNIQUE SPECTRUM; DEAFNESS; EXPRESSION;
D O I
10.1371/journal.pone.0022150
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Recessive mutations in the SLC26A4 gene are a common cause of hereditary hearing impairment worldwide. Previous studies have demonstrated that different SLC26A4 mutations may have different pathogenetic mechanisms. In the present study, we established a knock-in mouse model (i.e., Slc26a4(tm1Dontuh/tm1Dontuh) mice) homozygous for the c. 919-2A. G mutation, which is a common mutation in East Asians. Mice were then subjected to audiologic assessment, a battery of vestibular evaluations, and inner ear morphological studies. All Slc26a4(tm1Dontuh/tm1Dontuh) mice revealed profound hearing loss, whereas 46% mice demonstrated pronounced head tilting and circling behaviors. There was a significant difference in the vestibular performance between wild-type and Slc26a4(tm1ontuh/tm1Dontuh) mice, especially those exhibiting circling behavior. Inner ear morphological examination of Slc26a4(tm1Dontuh/tm1Dontuh) mice revealed an enlarged endolymphatic duct, vestibular aqueduct and sac, atrophy of stria vascularis, deformity of otoconia in the vestibular organs, consistent degeneration of cochlear hair cells, and variable degeneration of vestibular hair cells. Audiologic and inner ear morphological features of Slc26a4(tm1Dontuh/tm1Dontuh) mice were reminiscent of those observed in humans. These features were also similar to those previously reported in both knock-out Slc26a4(-/-) mice and Slc26a4(loop/loop) mice with the Slc26a4 p.S408F mutation, albeit the severity of vestibular hair cell degeneration appeared different among the three mouse strains.
引用
收藏
页数:10
相关论文
共 35 条
[1]   Genotype-phenotype correlations for SLC26A4-related deafness [J].
Azaiez, Hela ;
Yang, Tao ;
Prasad, Sai ;
Sorensen, Jessica L. ;
Nishimura, Carla J. ;
Kimberling, William J. ;
Smith, Richard J. H. .
HUMAN GENETICS, 2007, 122 (05) :451-457
[2]  
Belyantseva IA, 2000, J NEUROSCI, V20, part. no.
[3]   Two missense mutations in SLC26A4 gene: a molecular and functional study [J].
Ben Rebeh, I. ;
Yoshimi, N. ;
Hadj-Kacem, H. ;
Yanohco, S. ;
Hammami, B. ;
Mnif, M. ;
Araki, M. ;
Ghorbel, A. ;
Ayadi, H. ;
Masmoudi, S. ;
Miyazaki, H. .
CLINICAL GENETICS, 2010, 78 (01) :74-80
[4]   Expression of pendrin and the Pendred Syndrome (PDS) gene in human thyroid tissues [J].
Bidart, JM ;
Mian, C ;
Lazar, V ;
Russo, D ;
Filetti, S ;
Caillou, B ;
Schlumberger, M .
JOURNAL OF CLINICAL ENDOCRINOLOGY & METABOLISM, 2000, 85 (05) :2028-2033
[5]   Hypo-Functional SLC26A4 Variants Associated with Nonsyndromic Hearing Loss and Enlargement of the Vestibular Aqueduct: Genotype-Phenotype Correlation or Coincidental Polymorphisms? [J].
Choi, Byung Yoon ;
Stewart, Andrew K. ;
Madeo, Anne C. ;
Pryor, Shannon P. ;
Lenhard, Suzanne ;
Kittles, Rick ;
Eisenman, David ;
Kim, H. Jeffrey ;
Niparko, John ;
Thomsen, James ;
Arnos, Kathleen S. ;
Nance, Walter E. ;
King, Kelly A. ;
Zalewski, Christopher K. ;
Brewer, Carmen C. ;
Shawker, Thomas ;
Reynolds, James C. ;
Butman, John A. ;
Karniski, Lawrence P. ;
Alper, Seth L. ;
Griffith, Andrew J. .
HUMAN MUTATION, 2009, 30 (04) :599-608
[6]   Calcium Oxalate Stone Formation in the Inner Ear as a Result of an Slc26a4 Mutation [J].
Dror, Amiel A. ;
Politi, Yael ;
Shahin, Hashem ;
Lenz, Danielle R. ;
Dossena, Silvia ;
Nofziger, Charity ;
Fuchs, Helmut ;
de Angelis, Martin Hrabe ;
Paulmichl, Markus ;
Weiner, Steve ;
Avraham, Karen B. .
JOURNAL OF BIOLOGICAL CHEMISTRY, 2010, 285 (28) :21724-21735
[7]   Pendred syndrome is caused by mutations in a putative sulphate transporter gene (PDS) [J].
Everett, LA ;
Glaser, B ;
Beck, JC ;
Idol, JR ;
Buchs, A ;
Heyman, M ;
Adawi, F ;
Hazani, E ;
Nassir, E ;
Baxevanis, AD ;
Sheffield, VC ;
Green, ED .
NATURE GENETICS, 1997, 17 (04) :411-422
[8]   Targeted disruption of mouse Pds provides insight about the inner-ear defects encountered in Pendred syndrome [J].
Everett, LA ;
Belyantseva, IA ;
Noben-Trauth, K ;
Cantos, R ;
Chen, A ;
Thakkar, SI ;
Hoogstraten-Miller, SL ;
Kachar, B ;
Wu, DK ;
Green, ED .
HUMAN MOLECULAR GENETICS, 2001, 10 (02) :153-161
[9]   Expression pattern of the mouse ortholog of the Pendred's syndrome gene (Pds) suggests a key role for pendrin in the inner ear [J].
Everett, LA ;
Morsli, H ;
Wu, DK ;
Green, ED .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1999, 96 (17) :9727-9732
[10]   Forty-six genes causing nonsyndromic hearing impairment: Which ones should be analyzed in DNA diagnostics? [J].
Hilgert, Nele ;
Smith, Richard J. H. ;
Van Camp, Guy .
MUTATION RESEARCH-REVIEWS IN MUTATION RESEARCH, 2009, 681 (2-3) :189-196
1234