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huMYOC Mouse
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huMYOC Mouse

Product Name
huMYOC Mouse
Product ID
C001982
Strain Name
C57BL/6JCya-Myoctm1(hMYOC)/Cya
Backgroud
C57BL/6JCya
Status
Live Mouse
When using this mouse strain in a publication, please cite “huMYOC Mouse (Catalog C001982) were purchased from Cyagen.”
HUGO-GT Humanized Models
Small Nucleic Acids
Glaucoma
Product Type
Age
Genotype
Sex
Quantity
The standard delivery applies for a guaranteed minimum of three heterozygous carriers. Breeding services for homozygous carriers and/or specified sex are available.
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HUGO-GT Humanized Models
Small Nucleic Acids
Glaucoma

Basic Information

Related Resource

Basic Information
Gene Name
MYOC
Gene Alias
GPOA, JOAG, TIGR, GLC1A, JOAG1
NCBI ID
4653 (Human)
Chromosome
Chr 1 (Human)
MGI ID
MGI:1202864
Datasheet
Click here to download >>

Strain Description

The MYOC gene encodes a secreted glycoprotein known as myocilin, which is characterized by an N-terminal leucine zipper motif and a C-terminal olfactomedin-like domain [1]. Although myocilin is expressed in various tissues throughout the body—including skeletal muscle, heart, and the lining of the eye—it is most critically labeled and studied in the trabecular meshwork (TM) of the eye, where it is thought to play a role in cytoskeletal organization and cell-matrix interactions [2]. While the precise physiological function of myocilin remains a subject of ongoing research, mutations in the MYOC gene are the most common genetic cause of Primary Open-Angle Glaucoma (POAG) and Juvenile Open-Angle Glaucoma (JOAG). In these disease states, misfolded myocilin proteins fail to be secreted and instead accumulate within the endoplasmic reticulum of TM cells, leading to cellular stress, TM dysfunction, and a subsequent increase in intraocular pressure that can damage the optic nerve [3].
The huMYOC mouse is a humanized model constructed through gene-editing technology, in which the region from upstream to downstream of the mouse Myoc gene was replaced with the region from upstream to downstream of the human MYOC gene. This model can be used for research on glaucoma, as well as for screening, development, and preclinical evaluation of MYOC-targeted therapeutics.
Reference
Sharma R, Grover A. Myocilin-associated Glaucoma: A Historical Perspective and Recent Research Progress. Mol Vis. 2021 Aug 20;27:480-493.
Judge SM, Deyhle MR, Neyroud D, Nosacka RL, D'Lugos AC, Cameron ME, Vohra RS, Smuder AJ, Roberts BM, Callaway CS, Underwood PW, Chrzanowski SM, Batra A, Murphy ME, Heaven JD, Walter GA, Trevino JG, Judge AR. MEF2c-Dependent Downregulation of Myocilin Mediates Cancer-Induced Muscle Wasting and Associates with Cachexia in Patients with Cancer. Cancer Res. 2020 May 1;80(9):1861-1874.
Saccuzzo EG, Youngblood HA, Lieberman RL. Myocilin misfolding and glaucoma: A 20-year update. Prog Retin Eye Res. 2023 Jul;95:101188.

Strain Strategy

The region from upstream to downstream of the mouse Myoc gene was replaced with the region from upstream to downstream of the human MYOC gene.
Figure 1. Gene editing strategy of huMYOC mice.
Figure 1. Gene editing strategy of huMYOC mice.

Application Area

Screening, development, and preclinical evaluation of MYOC-targeted drugs;
Research on the pathogenic mechanism and relevant treatment methods of glaucoma.
Related Resource
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Global Antibody Drug Industry Development BlueBook (Frost & Sullivan)
Key Insights
The industry is undergoing a rapid transformation driven by next-generation modalities, globalized markets, and upstream technological innovations.
  • Market Structural Shift: Monoclonal antibodies drive steady growth, but ADCs and bispecifics are rapidly accelerating, reshaping the market with higher-value innovations.
  • Chinese Market Globalization: China is actively expanding globally, evidenced by a surge in high-value cross-border license-out deals.
  • Technology-Driven Efficiency: Advanced discovery engines—exemplified by Cyagen's HUGO-Ab platform and AI algorithms—are streamlining candidate screening, optimizing molecular design, and localizing the upstream supply chain.
  • Oncology-Focused Innovation: R&D pipelines remain heavily concentrated on high-incidence malignancies like non-small cell lung cancer, utilizing complex modalities to combat clinical resistance.
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