Liver-specific Knockout of GRP94 in Mice Disrupts Cell Adhesion, Activates Liver Progenitor Cells, and Accelerates Liver Tumorigenesis

Documenti analoghi

• GRP78 as a regulator of liver steatosis and cancer progression mediated by loss of the tumor suppressor PTEN
  di: Chen, Wan-Ting, et al.
  Pubblicazione: (2013)
• Deficiency of GRP94 in the Hematopoietic System Alters Proliferation Regulators in Hematopoietic Stem Cells
  di: Luo, Biquan, et al.
  Pubblicazione: (2013)
• Targeted Deletion of ER Chaperone GRP94 in the Liver Results in Injury, Repopulation of GRP94-Positive Hepatocytes, and Spontaneous Hepatocellular Carcinoma Development in Aged Mice
  di: Chen, Wan-Ting, et al.
  Pubblicazione: (2014)
• Targeted Mutation of the Mouse Grp94 Gene Disrupts Development and Perturbs Endoplasmic Reticulum Stress Signaling
  di: Mao, Changhui, et al.
  Pubblicazione: (2010)
• The critical role of GRP78 in physiologic and pathologic stress
  di: Pfaffenbach, Kyle T., et al.
  Pubblicazione: (2010)