Abstract

Central to the retinal pigment epithelial cells'(RPE)1 role as professional phagocytes is the regulated biogenesis and maturation of lysosomes which serves as the major degrading compartment, containing over 50 acid-dependent hydrolytic enzymes (1). In RPE cells the daily phagocytic challenge produces not only a high degradative load but since these cells are post-mitotic, over the long-term, virtually continuous phagocytosis produces additional metabolic stress on the RPE. Incomplete digestion of internalized OSs leads to the accumulation of autofluorescent aggregates called lipofuscin within the membrane bound lysosomes. We have identified a novel putative regulator of lysosome function, called melanoregulin (MREG). In the Mreg- /- mouse, loss of MREG results in diminished lysosomal hydrolase activity and deregulation of Cathepsin-D processing. This has deleterious consequences to the RPE resulting in delayed phagosome degradation, accumulation of opsin positive phagolysosomes and in aging animals, enhanced production of toxic photoproducts. Our studies are focused on understanding the molecular mechanism by which MREG regulates lysosomogenesis. We will test the hypothesis that MREG is necessary in the dynamic regulation of lysosome function. We plan to use an integrated approach involving in vivo studies using Mreg-/- and age-matched control Mreg+/+ mice in combination with in vitro Mregdsu gene silencing techniques to assess the consequences of abnormal lysosome maturation on human RPE health.
In specific aim 1, we will delineate how MREG contributes to lysosome maturation and how defects in maturation lead to diminished lysosomal hydrolase function. The cumulative, long-term effect of lysosomal dysfunction will be addressed by quantifying the levels of A2E in the RPE. In the second specific aim we will focus on the effect of lysosomal dysfunction on the processing of Cat-D and establish the relationship between Cat-D sorting and, missorting due to loss of MREG, and phagocytosis. We predict that loss of MREG contributes to RPE dysfunction leading to long-term pathologic changes in RPE, Bruch's membrane (BM), and choroid. This proposal expands previous RPE intracellular trafficking studies in a new direction and represents a unique approach to advance our understanding of how lysosomal enzymes are trafficked and what effect the collective loss of several hydrolases has on RPE health. These studies provide the underpinnings for future studies directed at the development of MREG as therapeutic agent.

Public Health Relevance

The accumulation of debris in the retina contributes to pathologic changes associated with retinal degenerative disease as well as normal human aging. Essential for the efficient degradation of ingested material are lysosomes. They play a particularly crucial role in the degradation of ingested photoreceptor material by the retinal pigment epithelia (RPE). Defective maturation of essential lysosomal enzymes and missorting of lysosomal proteases are hallmarks of the RPE's response to oxidative stress, as well as age- associated changes in the RPE. In these studies we will evaluate a novel regulator of lysosome function called melanoregulin. Understanding how melanoregulin contributed to lysosome function will allow us to develop therapeutic approaches to enhancing lysosome function during normal human aging.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Exploratory/Developmental Grants (R21)
Project #
5R21EY018705-02
Application #
7892466
Study Section
Special Emphasis Panel (ZRG1-CB-G (90))
Program Officer
Mariani, Andrew P
Project Start
2009-08-01
Project End
2012-07-31
Budget Start
2010-08-01
Budget End
2012-07-31
Support Year
2
Fiscal Year
2010
Total Cost
$198,000
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Biochemistry
Type
Schools of Dentistry
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Frost, Laura S; Lopes, Vanda S; Bragin, Alvina et al. (2015) The Contribution of Melanoregulin to Microtubule-Associated Protein 1 Light Chain 3 (LC3) Associated Phagocytosis in Retinal Pigment Epithelium. Mol Neurobiol 52:1135-1151
Frost, Laura S; Mitchell, Claire H; Boesze-Battaglia, Kathleen (2014) Autophagy in the eye: implications for ocular cell health. Exp Eye Res 124:56-66
Brown, Angela C; Balashova, Nataliya V; Epand, Richard M et al. (2013) Aggregatibacter actinomycetemcomitans leukotoxin utilizes a cholesterol recognition/amino acid consensus site for membrane association. J Biol Chem 288:23607-21
Frost, Laura S; Lopes, Vanda S; Stefano, Frank P et al. (2013) Loss of melanoregulin (MREG) enhances cathepsin-D secretion by the retinal pigment epithelium. Vis Neurosci 30:55-64
Brown, Angela C; Boesze-Battaglia, Kathleen; Du, Yurong et al. (2012) Aggregatibacter actinomycetemcomitans leukotoxin cytotoxicity occurs through bilayer destabilization. Cell Microbiol 14:869-81
Kuznetsova, Tatyana; Iwabe, Simone; Boesze-Battaglia, Kathleen et al. (2012) Exclusion of RPGRIP1 ins44 from primary causal association with early-onset cone-rod dystrophy in dogs. Invest Ophthalmol Vis Sci 53:5486-501
Moore, David T; Nygren, Patrik; Jo, Hyunil et al. (2012) Affinity of talin-1 for the ?3-integrin cytosolic domain is modulated by its phospholipid bilayer environment. Proc Natl Acad Sci U S A 109:793-8
Baltazar, Gabriel C; Guha, Sonia; Lu, Wennan et al. (2012) Acidic nanoparticles are trafficked to lysosomes and restore an acidic lysosomal pH and degradative function to compromised ARPE-19 cells. PLoS One 7:e49635
Guha, Sonia; Baltazar, Gabriel C; Tu, Leigh-Anne et al. (2012) Stimulation of the D5 dopamine receptor acidifies the lysosomal pH of retinal pigmented epithelial cells and decreases accumulation of autofluorescent photoreceptor debris. J Neurochem 122:823-33
Rachel, Rivka A; Nagashima, Kunio; O'Sullivan, T Norene et al. (2012) Melanoregulin, product of the dsu locus, links the BLOC-pathway and OA1 in organelle biogenesis. PLoS One 7:e42446

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