Abstract

Identification of """"""""molecular determinants"""""""" that regulate bladder cancer (BCa) progression could improve treatment and recurrence monitoring for BCa patients. Hyaluronic acid (HA) is a glycosaminoglycan that promotes tumor metastasis. Hyaluronidase (HAase) is an enzyme that degrades HA into angiogenic fragments. HYAL1 is the major HAase expressed in bladder tumor (BT) cells. It regulates BCa growth and invasion both in vitro and in BT xenografts. While HYAL1 wild type (wt) is enzymatically active and is exclusively expressed in high-grade BCa, 5 HYAL1 variants are enzymatically inactive and expressed in normal and low-grade BCa tissues. In BT tissues, both tumor cells and the stroma produce HA, however, HAS1 type HA-synthase is exclusively expressed in BT cells. The measurement of urinary HA and HAase levels (HA-HAase test) has high accuracy in detecting BCa. This proposal is designed to investigate the therapeutic and prognostic potentials of HYAL1, HYAL1 splice variants, and HAS1 in BCa progression. Furthermore, in a multi-center trial whether the HA-HAase test, either alone or in combination with other urine tests, can be used for monitoring BCa recurrence will be evaluated. To define HYAL1 function(s) in BCa growth and progression, the efficacy of anti-HAase therapy will be tested in BT xenografts, following delivery of HYAL1-antisense cDNA using a viral system or by treatment with a HAase inhibitor. The mechanism of HYAL1 action will be examined by analyzing alterations in cell cycle regulators, matrix degrading enzymes, and angiogenic factors (Aim 1). A possible neutralizing effect of HYAL1 variants on BCa growth and invasion will be examined by cDNA transfection of HYAL1wt expressing BT cells with HYAL1 splice variant cDNAs. Differential expression of HYAL1 variants in BT tissues will be correlated with BT prognosis (Aim 2). HAS1 function in BT growth and progression will be evaluated by transfecting BCa cells which either express or are blocked in HYAL1 production, using HAS1-sense and HAS1-antisense constructs. Expression of HAS1 and its variant (HAS1v) in BT tissues will be correlated with BCa prognosis (Aim 3). In a multi-center trial, the utility of the HA-HAase test, urine cytology, BTA-Stat, NMP22 tests, individually and in combination, will be examined for precision to monitor tumor recurrence in 100 to 150 BCa patients. The results will be compared to clinical findings (Aim 4). The proposed study will reveal the function, therapeutic and/or prognostic potentials of the HA, HYAL1 and related molecules in BT progression. Furthermore, it will establish whether the HA-HAase test or its combination with other tests can precisely monitor BCa recurrence.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA072821-08
Application #
6895254
Study Section
Special Emphasis Panel (ZRG1-CAMP (01))
Program Officer
Tricoli, James
Project Start
1997-01-01
Project End
2007-05-31
Budget Start
2005-06-01
Budget End
2006-05-31
Support Year
8
Fiscal Year
2005
Total Cost
$268,524
Indirect Cost

  Institution

Name
University of Miami School of Medicine
Department
Urology
Type
Schools of Medicine
DUNS #
052780918
City
Miami
State
FL
Country
United States
Zip Code
33146

  Publications

Jordan, Andre R; Lokeshwar, Soum D; Lopez, Luis E et al. (2017) Antitumor activity of sulfated hyaluronic acid fragments in pre-clinical models of bladder cancer. Oncotarget 8:24262-24274
Morera, Daley S; Hennig, Martin S; Talukder, Asif et al. (2017) Hyaluronic acid family in bladder cancer: potential prognostic biomarkers and therapeutic targets. Br J Cancer 117:1507-1517
Yates, Travis J; Lopez, Luis E; Lokeshwar, Soum D et al. (2015) Dietary supplement 4-methylumbelliferone: an effective chemopreventive and therapeutic agent for prostate cancer. J Natl Cancer Inst 107:
Gosalbez, Miguel; Hupe, Marie C; Lokeshwar, Soum D et al. (2014) Differential expression of SDF-1 isoforms in bladder cancer. J Urol 191:1899-1905
Lokeshwar, Vinata B; Mirza, Summan; Jordan, Andre (2014) Targeting hyaluronic acid family for cancer chemoprevention and therapy. Adv Cancer Res 123:35-65
Garcia-Roig, Michael; Ortiz, Nicolas; Lokeshwar, Vinata (2014) Molecular marker for predicting treatment response in advanced renal cell carcinoma: does the promise fulfill clinical need? Curr Urol Rep 15:375
Yates, Travis J; Knapp, Judith; Gosalbez, Miguel et al. (2013) C-X-C chemokine receptor 7: a functionally associated molecular marker for bladder cancer. Cancer 119:61-71
Benitez, Anaid; Yates, Travis J; Shamaldevi, N et al. (2013) Dietary supplement hymecromone and sorafenib: a novel combination for the control of renal cell carcinoma. J Urol 190:285-90
Chi, Andrew; Shirodkar, Samir P; Escudero, Diogo O et al. (2012) Molecular characterization of kidney cancer: association of hyaluronic acid family with histological subtypes and metastasis. Cancer 118:2394-402
Gahan, Jeffrey C; Gosalbez, Miguel; Yates, Travis et al. (2012) Chemokine and chemokine receptor expression in kidney tumors: molecular profiling of histological subtypes and association with metastasis. J Urol 187:827-33

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