Nebraska Mesothelioma Fact Sheet
While mesothelioma is a problem in all states, the specific incident rate for Nebraska is 1 / 100,000. This is below the average rate of 1.1 / 100,000. Click on the tabs below to find mesothelioma and asbestos research in NE, recent NE mesothelioma-related court cases, mesothelioma specialists in NE and potential asbestos hotspots in Nebraska.
Nebraska Mesothelioma Info
By clicking on the above tabs, you will find information on mesothelioma specific to the state of Nebraska
Nebraska Research and Clinical Trials
This is a partial list of scientific or medical grants in your state for research into mesothelioma and related illnesses.
Nebraska Doctors and Hospitals
This is a partial list of hospitals and physicians that reportedly treat mesothelioma patients in your state.
Nebraska Cases
This is a partial list of relevant court cases on mesothelioma in your state.
Disclaimer: Inclusion on this directory does not constitute endorsement by Cancer Monthly, Inc. All physicians who appear in this section do so based on their own expression of interest in the fields of mesothelioma treatment. Cancer Monthly, Inc. has not verified the competence, professional credentials, business practices or validity of the expressed interests of these physicians. Cancer Monthly makes no recommendation of any physician on this list and makes no suggestion that any such physician will cure or prevent any disease. Those consulting a physician on this list should approach the consultation exactly as they would with any other unknown physician.
This is a partial list of scientific or medical grants in your state for research into mesothelioma and related illnesses.
Nebraska Doctors and Hospitals
This is a partial list of hospitals and physicians that reportedly treat mesothelioma patients in your state.
Nebraska Cases
This is a partial list of relevant court cases on mesothelioma in your state.
Disclaimer: Inclusion on this directory does not constitute endorsement by Cancer Monthly, Inc. All physicians who appear in this section do so based on their own expression of interest in the fields of mesothelioma treatment. Cancer Monthly, Inc. has not verified the competence, professional credentials, business practices or validity of the expressed interests of these physicians. Cancer Monthly makes no recommendation of any physician on this list and makes no suggestion that any such physician will cure or prevent any disease. Those consulting a physician on this list should approach the consultation exactly as they would with any other unknown physician.
Olivotto v. DeMarco Bros. Co.
No. S-05-1526., SUPREME COURT OF NEBRASKA, June 1, 2007, Filed
No. S-05-1526., SUPREME COURT OF NEBRASKA, June 1, 2007, Filed
Morris v. Neb. Health Sys.
No. S-01-1194. , SUPREME COURT OF NEBRASKA, July 11, 2003, Filed
No. S-01-1194. , SUPREME COURT OF NEBRASKA, July 11, 2003, Filed
Hospitals and Cancer Centers
Creighton University Medical Center: Cancer Center-Suite 2321
601 N. 30th Street
Omaha, NE
402.280.5009
Creighton University Medical Center: Cancer Center-Suite 2321
601 N. 30th Street
Omaha, NE
402.280.5009
| City | Site |
| Auburn |
Cooper Nuclera Power Plant Gerald Gentleman Power Plant |
| Beatrice |
Phillips Chemical Plant |
| Brownsville |
Nuclear Plant |
| Grand Island |
Municipal Power Plant |
| Lincoln |
Yeargin Construction |
| Nebraska City |
Nebraska Power Station |
| Omaha |
AAA Appliances Asarco Boys Home Woodmen Tower Bldg |
| Pine Bluff |
Atlas Missile Site |
Research
Wang, Zhao-yi Regulation Of Cell Growth By The Wilms Tumor Gene
Grant: 7R29CA076632-06
Grant: 7R29CA076632-06
Abstract: DESCRIPTION: (Adapted from investigator's abstract) The Wilms' tumor
suppressor gene, wt1, encodes a zinc finger transcription factor, WT1. A
number of mutations to the wt1 gene have been identified in subsets of Wilms
tumor, mesothelioma, ovarian tumor and acute myeloid leukemia, suggesting
that dysfunction of WT1 may be important in many tumors. However,
effectively nothing is known about the endogenous genes regulated by WT1,
and thus the signaling pathways triggered by WT1 and how mutated WT1
influences these pathways to result in Wilms' tumor remain to be discovered.
The long-term objective of the investigator's research is to characterize
the normal functions of WT1 during development and the dysfunctions of
mutated WT1 that lead to the genesis of Wilms' tumor. The investigators
recently cloned a gene whose expression is over tenfold greater in cells
expressing WT1 than in cells with undetectable levels of WT1. The gene was
identified as retinoblastoma (Rb) suppressor associated protein (AP)
(RbAp46), a nuclear protein that physically interacts with Rb. The
investigators have recently cloned and expressed the full-length cDNA of
RbAp46, and analyzed its effect on tumor cells. Remarkably, expression of
exogenous RbAp46 suppressed growth in four out of four tumor cell lines,
suggesting that RbAp46 itself has growth inhibitory activity. The
investigators now plan to establish the positive correlation between the
levels of WT1 and RbAp46 expression in different tumor cells and in mouse
tissues from different stages of development using Northern and in situ
hybridization analysis. They plan to analyze the promoter region of RbAp46
to determine whether WT1 directly regulates the expression of RbAp46. They
plan to explore the possible roles of RbAp46 as a mediator of WT1 function
by expressing exogenous RbAp46 or by down-regulating RbAp46 in cells. The
investigators plan to probe the mechanisms by which RbAp46 functions as a
growth inhibitor by analyzing its impact on the cell cycle and its influence
on the ras signaling pathway. The investigators plan to perform structure
and function analysis to identify the domain(s) of RbAp46 required for its
function. The investigators plan to identify the proteins which interact
with RbAp46 by co-immunoprecipitation and an in vivo GST capture assay and,
if necessary, by a yeast two-hybrid strategy. It is hoped that these
studies will lay the foundation of therapeutic intervention for the Wilms'
tumor and other tumors as well.
Tags: Wilms' Tumor, Cell Growth Regulation, Gene Expression, Neoplasm /cancer Genetics, Retinoblastoma Protein, Transcription Factor, Tumor Suppressor Gene, Tumor Suppressor Protein Cell Differentiation, Developmental Genetics, Gene Interaction, Genetic Promoter Element, Growth Inhibitor, Neoplastic Transformation, Protein Structure Function, Regulatory Gene 3t3 Cell, Athymic Mouse, Cell Line, Immunoprecipitation, In Situ Hybridization, Neoplastic Cell, Northern Blotting
Tags: Wilms' Tumor, Cell Growth Regulation, Gene Expression, Neoplasm /cancer Genetics, Retinoblastoma Protein, Transcription Factor, Tumor Suppressor Gene, Tumor Suppressor Protein Cell Differentiation, Developmental Genetics, Gene Interaction, Genetic Promoter Element, Growth Inhibitor, Neoplastic Transformation, Protein Structure Function, Regulatory Gene 3t3 Cell, Athymic Mouse, Cell Line, Immunoprecipitation, In Situ Hybridization, Neoplastic Cell, Northern Blotting
Clinical Trials
Condition: Malignant Mesothelioma
Intervention: Drug: pazopanib hydrochloride; Other: laboratory biomarker analysis
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Intervention: Drug: pazopanib hydrochloride; Other: laboratory biomarker analysis
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Condition: Malignant Mesothelioma
Intervention: Drug: doxorubicin hydrochloride; Drug: ranpirnase
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Intervention: Drug: doxorubicin hydrochloride; Drug: ranpirnase
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Active, not recruiting Dasatinib in Treating Patients With Previously Treated Malignant Mesothelioma
Condition: Malignant Mesothelioma
Intervention: Drug: dasatinib; Other: immunoenzyme technique; Other: immunohistochemistry staining method; Other: laboratory biomarker analysis
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Intervention: Drug: dasatinib; Other: immunoenzyme technique; Other: immunohistochemistry staining method; Other: laboratory biomarker analysis
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Condition: Malignant Mesothelioma
Intervention: Drug: epirubicin hydrochloride; Drug: gemcitabine hydrochloride
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Intervention: Drug: epirubicin hydrochloride; Drug: gemcitabine hydrochloride
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