Abstract

. Mucolipidosis type IV (MLIV) is a lysosomal storage disorder caused by mutations in the gene coding for a lysosomal ion channel Mucolipin 1 (TRPML1). MLIV causes severe developmental delays, psychomotor retardation, cognitive disabilities, corneal cloudiness and degeneration of the retina. At the cellular level, accumulation of phospholipids and gangliosides is detected, and virtually all patients'cells contain enfolded membranous structures of unknown origin. Since TRPML1 localizes in lysosomes and its downregulation causes severe lysosomal storage phenotype, TRPML1 was suggested to regulate lysosomal function. At present, there is no complete model that explains TRPML1 function in the lysosomes. TRPML1 was suggested to directly regulate intracellular membrane traffic by modulating fusion and/or fission of the organelles within the lower portions of the endocytic pathway. An alternative model suggests that TRPML1 affects lysosomal hydrolysis by regulating lysosomal acidification. The present project aims to directly answer the two main question in MLIV pathogenesis: whether TRPML1 directly regulates membrane traffic in the endocytic pathway and which aspect of TRPML1 permeability makes it indispensable for the proper function of the endocytic pathway. This will be accomplished by a combination of molecular, biochemical and physiological techniques. Specifically, an siRNA driven TRPML1 downregulation system will be used to establish the direct and immediate effects of TRPML1 downregulation on membrane traffic and lysosomal lipid hydrolysis. A structure function analysis of ion permeation through TRPML1 and its close relative TRPML3 will be performed to identify the structural determinants of the unique aspects of TRPML1 ion permeation. The ion permeation through TRPML1 will be specifically modulated in order to establish the aspects of TRPML1 permeability that make TRPML1 indispensable for the proper function of the endocytic pathway. The experiments planned in this proposal will establish the direction for the search for MLIV treatments, identify the new roles for intracellular ion channels in regulation of membrane traffic, lysosomal metabolism and organellar ion homeostasis and provide novel structural information regarding the basic mechanisms of ion channel permeation, rectification and block.

Public Health Relevance

. Finding whether MLIV is a result of membrane traffic delays or inefficient lipid hydrolysis in lysosomes is key to formulating strategies for MLIV treatment as it defines whether the enzyme replacement therapies will be effective as an MLIV treatment. If TRPML1 loss affects lysosomal ion homeostasis and causes inactivation of lysosomal enzymes, then the future MLIV therapies may focus on enzyme replacement using enzymes modified to work in MLIV specific lysosomal ionic environment. Furthermore, pharmacological strategies can be formulated to specifically change lysosomal ionic environment to compensate the TRPML1 loss.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
1R01HD058577-01A1
Application #
7651968
Study Section
Developmental Brain Disorders Study Section (DBD)
Program Officer
Oster-Granite, Mary Lou
Project Start
2009-09-30
Project End
2011-08-31
Budget Start
2009-09-30
Budget End
2010-08-31
Support Year
1
Fiscal Year
2009
Total Cost
$249,323
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Kiselyov, Kirill; Muallem, Shmuel (2016) ROS and intracellular ion channels. Cell Calcium 60:108-14
Ravi, Sreeram; Peña, Karina A; Chu, Charleen T et al. (2016) Biphasic regulation of lysosomal exocytosis by oxidative stress. Cell Calcium 60:356-362
Grishchuk, Yulia; Peña, Karina A; Coblentz, Jessica et al. (2015) Impaired myelination and reduced brain ferric iron in the mouse model of mucolipidosis IV. Dis Model Mech 8:1591-601
Bouron, Alexandre; Kiselyov, Kirill; Oberwinkler, Johannes (2015) Permeation, regulation and control of expression of TRP channels by trace metal ions. Pflugers Arch 467:1143-64
Peña, Karina A; Kiselyov, Kirill (2015) Transition metals activate TFEB in overexpressing cells. Biochem J 470:65-76
Morgan, Alwena H; Hammond, Victoria J; Sakoh-Nakatogawa, Machiko et al. (2015) A novel role for 12/15-lipoxygenase in regulating autophagy. Redox Biol 4:40-7
Peña, Karina; Coblenz, Jessica; Kiselyov, Kirill (2015) Brief exposure to copper activates lysosomal exocytosis. Cell Calcium 57:257-62
Kukic, Ira; Kelleher, Shannon L; Kiselyov, Kirill (2014) Zn2+ efflux through lysosomal exocytosis prevents Zn2+-induced toxicity. J Cell Sci 127:3094-103
Coblentz, Jessica; St Croix, Claudette; Kiselyov, Kirill (2014) Loss of TRPML1 promotes production of reactive oxygen species: is oxidative damage a factor in mucolipidosis type IV? Biochem J 457:361-8
Cherra 3rd, Salvatore J; Steer, Erin; Gusdon, Aaron M et al. (2013) Mutant LRRK2 elicits calcium imbalance and depletion of dendritic mitochondria in neurons. Am J Pathol 182:474-84

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