Partial Rescue of Ocular Pigment Cells and Structure by Inducible Ectopic Expression of Mitf-M in MITF-Deficient Mice

Michael, Helen; Graff-Cherry, Cari; Chin, Sung; Rauck, Corinne; Habtemichael, Amelework D; Bunda, Patricia; Smith, Tunde; Campos, Maria M; Bharti, Kapil; Arnheiter, Heinz; Merlino, Glenn; Day, Chi-Ping

doi:10.1167/iovs.18-25186

Cited by 4 publications

(4 citation statements)

References 26 publications

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“…This study reviewed the changes of Mitf-M mutation on gene expression in the cochlea. Mitf has many subtypes [38], in which type M is specifically expressed in melanocytes [39], by direct association with related pigmentases such as tyrosinase (Tyr), dopachrome tautomerase (Dct), endothelin receptor type B (Ednrb), and solute carrier family 45 member 2 (Slc45a2), regulating the survival, migration, and differentiation of melanocytes [40]. Among them, Mitf-M gene [38,39] plays a key role in regulating tyrosine metabolic pathway and melanin production, mainly regulating downstream pigment-related enzymes such as Tyr, Dct, and Tyrp1.…”

Section: Discussionmentioning

confidence: 99%

Transcript Profiles of Stria Vascularis in Models of Waardenburg Syndrome

et al. 2020

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Background. Waardenburg syndrome is an uncommon genetic condition characterized by at least some degree of congenital hearing loss and pigmentation deficiencies. However, the genetic pathway affecting the development of stria vascularis is not fully illustrated. Methods. The transcript profile of stria vascularis of Waardenburg syndrome was studied using Mitf-M mutant pig and mice models. Therefore, GO analysis was performed to identify the differential gene expression caused by Mitf-M mutation. Results. There were 113 genes in tyrosine metabolism, melanin formation, and ion transportations showed significant changes in pig models and 191 genes in mice models. In addition, there were some spice’s specific gene changes in the stria vascularis in the mouse and porcine models. The expression of tight junction-associated genes, including Cadm1, Cldn11, Pcdh1, Pcdh19, and Cdh24 genes, were significantly higher in porcine models compared to mouse models. Vascular-related and ion channel-related genes in the stria vascularis were also shown significantly difference between the two species. The expression of Col2a1, Col3a1, Col11a1, and Col11a2 genes were higher, and the expression of Col8a2, Cd34, and Ncam genes were lower in the porcine models compared to mouse models. Conclusions. Our data suggests that there is a significant difference on the gene expression and function between these two models.

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Section: Discussionmentioning

confidence: 99%

Transcript Profiles of Stria Vascularis in Models of Waardenburg Syndrome

et al. 2020

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“…In this study, we have generated a specific Mitf‐M knockout mouse and demonstrated that the loss of MITF‐M results in the loss of iris stromal and choroidal melanocytes. Our findings also demonstrate that while Mitf‐M may be expressed in the adult RPE (Maruotti, Thein, Zack, & Esumi, ) and can rescue the loss of pigmentation in Mitf vga9 mice (Michael et al, ), it is not required for pigmentation of the RPE. Additionally, the loss of Mitf‐M increased the size of the kidneys (Figure ), indicating that the loss of a single isoform affects distinct tissues differently, further highlighting the utility of the isoform‐specific knockout reagents generated in this study.…”

Section: Discussionmentioning

confidence: 99%

“…(b) examination of the expression pattern of isoforms in target tissues of wild-type and Mitf mutant animals to infer their function during development (Bharti et al, 2008); (c) isoform-specific overexpression studies to determine the function of individual isoforms (Michael et al, 2018); or (d) isoform-specific knockouts as previously performed (Bharti et al, 2012;Phelep et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

“…Although mice with mutations in the promoter regions of Mitf have been identified (Steingrímsson, Copeland, & Jenkins, ), the mutant alleles involve the loss of multiple isoforms, so it is still unclear how specific isoforms of MITF regulate pigmentation. Established methods for studying the role of Mitf isoforms rely on (a) mutant alleles that affect multiple isoforms (Steingrímsson et al, ); (b) examination of the expression pattern of isoforms in target tissues of wild‐type and Mitf mutant animals to infer their function during development (Bharti et al, ); (c) isoform‐specific overexpression studies to determine the function of individual isoforms (Michael et al, ); or (d) isoform‐specific knockouts as previously performed (Bharti et al, ; Phelep et al, ). More precise knockout models are needed to deconvolute the role of individual isoforms in tissue development and disease.…”

Section: Introductionmentioning

confidence: 99%

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Delineating the role of MITF isoforms in pigmentation and tissue homeostasis

Flesher

Paterson‐Coleman

Vasudeva

et al. 2019

Pigment Cell Melanoma Res

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MITF, a gene that is mutated in familial melanoma and Waardenburg syndrome, encodes multiple isoforms expressed from alternative promoters that share common coding exons but have unique amino termini. It is not completely understood how these isoforms influence pigmentation in different tissues and how the expression of these independent isoforms of MITF is regulated. Here, we show that melanocytes express two isoforms of MITF, MITF‐A and MITF‐M. The expression of MITF‐A is partially regulated by a newly identified retinoid enhancer element located upstream of the MITF‐A promoter. Mitf‐A knockout mice have only subtle changes in melanin accumulation in the hair and reduced Tyr expression in the eye. In contrast, Mitf‐M‐null mice have enlarged kidneys, lack neural crest‐derived melanocytes in the skin, choroid, and iris stroma, yet maintain pigmentation within the retinal pigment epithelium and iris pigment epithelium of the eye. Taken together, these studies identify a critical role for MITF‐M in melanocytes, a minor role for MITF‐A in regulating pigmentation in the hair and Tyr expression in the eye, and a novel role for MITF‐M in size control of the kidney.

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The transcription factor MITF in RPE function and dysfunction

Chen

et al. 2019

Progress in Retinal and Eye Research

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Partial Rescue of Ocular Pigment Cells and Structure by Inducible Ectopic Expression of Mitf-M in MITF-Deficient Mice

Cited by 4 publications

References 26 publications

Transcript Profiles of Stria Vascularis in Models of Waardenburg Syndrome

Transcript Profiles of Stria Vascularis in Models of Waardenburg Syndrome

Delineating the role of MITF isoforms in pigmentation and tissue homeostasis

The transcription factor MITF in RPE function and dysfunction

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