The mutational spectrum in Waardenburg syndrome

Tassabehji, Mayada; Newton, Valerie; Liu, Xue Zhong; Brady, Angela; Donnai, Dian; Krajewska‐Walasek, M; Murday, Victoria; Norman, Andrew; Obersztyn, Ewa; Reardon, William; Rice, John C; Trembath, Richard; Wieacker, P.; Whiteford, Margo; Winter, R M; Read, Andrew P.

doi:10.1093/hmg/4.11.2131

Cited by 193 publications

(149 citation statements)

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“…Along these lines, serine 298 of MITF, a GSK3b phosphoacceptor site, was found to be mutated to proline in a WS type 2 patient (Tassabehji et al, 1995;Takeda et al, 2000a). Absence of this serine abrogated DNA binding and transcriptional activity of MITF on the tyrosinase model promoter in vitro.…”

Section: Signaling and Mitf: Regulation By Post-translational Modificmentioning

confidence: 98%

Microphthalamia-associated transcription factor: a critical regulator of pigment cell development and survival

2003

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The microphthalamia-associated transcription factor (MITF) is an integral transcriptional regulator in melanocyte, the lineage from which melanoma cells originate. This basic-helix-loop-helix-leucine-zipper (bHLHzip) protein is critical for melanocyte cell-fate choice during commitment from pluripotent precursor cells in the neural crest. Its role in differentiation pathways has been highlighted by its potent transcriptional and lineage-specific regulation of the three major pigment enzymes: tyrosinase, Tyrp1, and Dct as well as other pigmentation factors. However, the cellular functions of MITF seem to be wider than differentiation and cell-fate pathways alone, since melanocytes and melanoma cells appear to require an expression of this factor. Here, we discuss the transcriptional networks in which MITF is thought to reside and describe signaling pathways in the cell which impinge on MITF. Accumulating evidence supports the notion that MITF is involved in survival pathways during normal development as well as during neoplastic growth of melanoma.

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Section: Signaling and Mitf: Regulation By Post-translational Modificmentioning

confidence: 98%

Microphthalamia-associated transcription factor: a critical regulator of pigment cell development and survival

2003

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“…Specific mutations within a number of PAX/ Pax (human/mouse) genes lead to a range of developmental abnormalities in both human beings and mouse. Many studies proved that PAX3 loss of function mutations are involved in either type 1 or type 3 Waardenburg syndrome [59][60][61][62][63][64][65]. PAX3/Pax3 (human/mouse) mutations are associated with limb muscle hypoplasia in Waardenburg syndrome patients and Splotch phenotype mice, respectively [54,55].…”

Section: Pax3 and Its Role In Development And Diseasesmentioning

confidence: 99%

“…Interestingly, PAX3 mutations were typically not found in families with other neurocristopathies [64]. Mutations that partially abolish the activity of PAX2, PAX3, and PAX6 were known to cause dysmorphic syndromes with developmental abnormalities [66][67][68][69][70].…”

Section: Pax3 and Its Role In Development And Diseasesmentioning

confidence: 99%

PAX3: A Molecule with Oncogenic or Tumor Suppressor Function Is Involved in Cancer

Arasu

Murugan

Essa

et al. 2018

BioMed Research International

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Metastasis is the most deadly aspect of cancer and results from acquired gene regulation abnormalities in tumor cells. Transcriptional regulation is an essential component of controlling of gene function and its failure could contribute to tumor progression and metastasis. During cancer progression, deregulation of oncogenic or tumor suppressive transcription factors, as well as master cell fate regulators, collectively influences multiple steps of the metastasis cascade, including local invasion and dissemination of the tumor to distant organs. Transcription factor PAX3/Pax3, which contributes to diverse cell lineages during embryonic development, plays a major role in tumorigenesis. Mutations in this gene can cause neurodevelopmental disease and the existing literature supports that there is a potential link between aberrant expression of PAX3 genes in adult tissues and a wide variety of cancers. PAX3 function is tissue-specific and could contribute to tumorigenesis either directly as oncogene or as a tumor suppressor by losing its function. In this review, we discuss comprehensively the differential role played by PAX3 in various tissues and how its aberrant expression is implicated in disease development. This review particularly highlights the oncogenic and tumor suppressor role played by PAX3 in different cancers and underlines the importance of precisely identifying tissue-specific role of PAX3 in order to determine its exact role in development of cancer.

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“…Particularly vulnerable to haploinsufficiency are regulatory genes working close to threshold levels in specific tissues. Examples include PAX3, which is responsible for Waardenburg syndrome Type 1 (Tassabehji et al 1995), and SOX9, a cause of campomelic dysplasia (Sock et al 2001). Based on our data, EYA1 and EYA4 can be added to this list.…”

Section: Discussionmentioning

confidence: 99%

A Comparative Study of Eya1 and Eya4 Protein Function and Its Implication in Branchio-oto-renal Syndrome and DFNA10

Zhang

Knosp

Maconochie

et al. 2004

JARO

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Allele variants of EYA1 and EYA4, two members of the vertebrate Eya gene family, underlie two types of inherited human deafness, branchio-oto-renal (BOR) syndrome and DFNA10, respectively. To clarify how mutations in these two genes and their encoded proteins impact the normal biology of hearing, we completed a number of functional studies using the yeast-two-hybrid system. We verified that bait constructs of the homologous region (Eya1HR and Eya4HR) interact with Six1 prey constructs, although no interaction with Dach1 prey was demonstrable. To compare interaction affinities, we evaluated a-galactosidase activity after cotransformation of Eya1HR/ Six1 and Eya4HR/Six1 and found that the latter interaction was weaker. By immunofluorescence staining, we showed Eya4HR localization to the cytoplasm. After coexpression of Six1, Eya4HR was translocated to the nucleus. Results with Eya1HR were similar. Translation of mutant constructs (Eya4HR R564X and Eya1HR R539X ) could not be demonstrated. Using dual Eya-containing constructs (with two wild-type alleles or wild-type and mutant alleles), we confirmed no translation of the mutant allele, even if the mutation was nontruncating. These results are consistent with clinical data and implicate haploinsufficiency as the cause of BOR syndrome and DFNA10.

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The mutational spectrum in Waardenburg syndrome

Cited by 193 publications

References 0 publications

Microphthalamia-associated transcription factor: a critical regulator of pigment cell development and survival

Microphthalamia-associated transcription factor: a critical regulator of pigment cell development and survival

PAX3: A Molecule with Oncogenic or Tumor Suppressor Function Is Involved in Cancer

A Comparative Study of Eya1 and Eya4 Protein Function and Its Implication in Branchio-oto-renal Syndrome and DFNA10

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