Research Database

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Therapeutics Award
Lynne Regan, PhD
Yale University, New Haven, CT
Funded equally by LUNGevity Foundation and Joan's Legacy

Cancer-causing proteins called heat shock proteins (HSPs) protect cancer cells from the effects of chemotherapy. Dr. Regan is testing how inhibiting the protein chaperon HSP90 affects the growth of different lung cancer cells.

Therapeutics Award
Hildegard M. Schuller, DVM, PhD
University of Tennessee, Knoxville, TN
Funded equally by LUNGevity Foundation and the National Lung Cancer Partnership

NNK is a powerful nicotine-derived carcinogen. Dr. Schuller is determining the exact role of estrogen in tumors caused by NNK. This understanding will provide new targets for the early diagnosis, prevention, and therapy of lung cancer in women.

Therapeutics Award
Sreenath Sharma, PhD
Massachusetts General Hospital, Boston, MA
Jeffery Settleman, MD, PhD
Massachusetts General Hospital, Boston, MA
Funded by LUNGevity Foundation, A Breath of Hope Foundation, and Partnership for Cures

Patients with EGFR mutations are treated with EGFR drugs such as gefitinib (Iressa) and erlotinib (Tarceva). However, the cancer cells eventually develop resistance to these drugs. Dr. Sharma is  aiming to understand the processes by which non-small cell lung cancer cells develop resistance to gefitinib and erlotinib as well as  how these processes can be targeted to develop new therapeutic strategies for patients in whom gefitinib and erlotinib have failed.

Early Detection Award
Scott L. Shofer, MD
Durham VA Medical Center Pulmonary Service, Durham, NC
Funded by LUNGevity Foundation and The CHEST Foundation

Dr. Shofer’s research builds on work of earlier investigators who developed a lung cancer risk signature based on genetic changes in lung cells in smokers. Dr. Shofer hypothesizes that the lung cancer risk signature model is an indicator of how lung cells change during the process of cancer development. Should his hypothesis be correct, the lung cancer risk signature could be established as a sensitive biomarker capable of diagnosing patients with lung cancer by checking cells taken from the throat using a swab.

Early Detection Award
Christopher G. Slatore, MD, MS
University of Washington School of Medicine, Seattle, WA
Funded by LUNGevity Foundation and The CHEST Foundation

Previously conducted clinical trials have suggested an increased risk of lung cancer from hormone replacement therapy (HRT). Dr. Slatore is studying women who have both undergone HRT and smoked  to determine whether there is a relationship between HRT, tobacco use, and lung cancer.

Early Detection Award
Michael Tainsky, PhD
Wayne State University, Karmanos Cancer Institute, Detroit, MI
Funded equally by LUNGevity Foundation and the American Lung Association

Dr. Tainsky has developed a technology that takes advantage of the responses of the human immune system to identify cancer-associated proteins that bind to antibodies present in the blood of cancer patients but not in the blood of healthy subjects or those with benign diseases. Dr. Tainsky is working to develop a non-invasive screening test for the early detection of lung cancer by using cancer-associated antigens as biomarkers.

Therapeutics Award
Jane Yanagawa, MD
University of California, Los Angeles, Los Angeles, CA
Funded equally by LUNGevity Foundation and the Thoracic Surgery Foundation

When cancer cells start spreading to other parts of the body, their shape changes through a process called EMT (epithelial-to-mesenchymal transition). The process of EMT in non-small cell lung cancer cells is mediated by the Snail protein. Dr. Yanagawa is studying how the Snail protein controls the EMT process through a protein called MMP2.

Therapeutics Award
Randolph Hastings, MD, PhD
Veterans Medical Research Foundation, San Diego, CA
Funded equally by LUNGevity Foundation and the American Lung Association

Dr. Hastings is establishing how parathyroid hormone-related protein (PTHrP) slows lung cancer growth, evaluating why lung cancers in men are less sensitive to PTHrP, and testing whether changes in hormone levels can affect the growth of lung cancer cells. His research may also determine whether changing the levels of male hormones makes it possible to improve the response to PTHrP.

Therapeutics Award
John Heymach, MD, PhD
MD Anderson Cancer Center, Houston, TX
Funded equally by LUNGevity Foundation and Joan's Legacy

The role of the hormone estrogen in the development of lung cancer has been established. Dr. Heymach is studying how estrogen affects signaling by the EGFR gene and secretion of proteins that fuel the development of new blood vessels necessary to sustain the growth of the cancer.

Therapeutics Award
Carla Kim, PhD
Children's Hospital, Boston, MA
Funded equally by LUNGevity Foundation and Joan's Legacy

Dr. Kim’s hypothesis is that bronchioloalveolar carcinomas, a subtype of non-small cell lung cancer, are maintained by a small population of cells often referred to as cancer stem cells. Dr. Kim is identifying these stem cells and drugs that inhibit them.

Therapeutics Award
LOGIC (Lung Oncology Group in Chicago)
, Chicago, IL
2007 Melissa Lumberg Zagon Award

The landscape of lung cancer treatment has changed with the initial discovery of an EGFR mutation in 2004. Now, drugs that block specific driver mutations are being considered for the treatment of non-small cell lung cancer (NSCLC). The LOGIC group (Lung Oncology Group in Chicago) is studying the correlative effects of agents used in conjunction with targeted therapies in the treatment of lung cancer.

Therapeutics Award
Hayley McDaid, PhD
Albert Einstein College of Medicine, New York, NY
Funded equally by LUNGevity Foundation and Joan's Legacy

Two commonly mutated genes in non-small cell lung cancer are KRAS and BRAF. Dr. McDaid is studying how these two genes control the synthesis of proteins in lung cancer cells. She is also testing how targeting the LKB1 mutation that often co-occurs with KRAS mutations can neutralize the effects of the KRAS mutation.

Early Detection Award
Milliman Consulting Services Agreement (CSA)
, , IL
Funded equally by LUNGevity Foundation, Lung Cancer Alliance (LCA), American Legacy Foundation, Prevent Cancer Foundation, Joan's Legacy Foundation, Thomas G. Labrecque Foundation, and the Bonnie J. Addario Lung Cancer Foundation

Lung cancer screening is not established as a public health practice, yet the results of a large randomized controlled trial among a high-risk population showed that screening with low-dose spiral computed tomography reduces lung cancer mortality. Milliman Consulting Company is conducting a cost-benefit analysis to demonstrate whether improved health outcomes (by catching the lung cancer early so that it can be treated) correlate with increased cost savings among this population.

Early Detection Award
S. Patrick Nana-Sinkam, MD
The Ohio State University, Columbus, OH
Funded by LUNGevity Foundation and The CHEST Foundation

Dr. Nana-Sinkam is delineating the role of microRNA expression profiling in the diagnosis, management, and prognosis of lung cancer. He is testing whether microRNA expression profiles are detectable in the  blood of lung cancer patients. He will compare individuals with lung cancer with current and former smokers without lung cancer.

Therapeutics Award
David J. Robbins, PhD
Dartmouth University Medical School, Hanover, NH
Funded equally by LUNGevity Foundation and the American Lung Association

The Hedgehog (Hh) signaling pathway is active in both small cell and non-small cell lung cancer and provides a “don’t stop growing” signal to cancer cells. Dr. Robbins is working to identify and validate a panel of biomarkers that can be used to determine whether the lung cancer is sensitive to drugs that stop Hh signaling.

Therapeutics Award
Dwight Seferos, PhD
Northwestern University Department of Chemistry, Chicago, IL
Funded equally by LUNGevity Foundation and the Illinois Chapter of the American Cancer Society

Dr. Seferos is developing new nanoparticle-based agents that are 13 nanometers in diameter to treat lung cancer. Unlike traditional chemotherapy, these particles can target the cancer cells directly and so reduce the side effects that are commonly associated with chemotherapy.

Therapeutics Award
Timothy K. Starr, PhD
University of Minnesota Department of Genetics, Cell Biology and Development, Minneapolis, MN
Funded equally by LUNGevity Foundation and the Illinois Chapter of the American Cancer Society

In order to identify mutated genes that cause lung cancer, Dr. Starr has developed a system that is capable of randomly mutating genes within cells, resulting in tumor formation. The genes mutated by this method can easily be identified using standard molecular biology techniques. He can then test their role in lung cancer formation. 

Therapeutics Award
Steven P. Zielske, PhD
University of Michigan Department of Radiation Oncology, Ann Arbor, MI
Funded equally by LUNGevity Foundation and the Illinois Chapter of the American Cancer Society

Human mesenchymal stem cells (MSCs) selectively migrate to tumors of the brain or the lung. MSCs are specialized cells found in the bone marrow. They can form bone, cartilage, fat, and possibly other tissues. Dr. Zielske is researching how to make use of this property of MSCs. He is working on how to deliver locally high concentrations of chemotherapy drugs to the tumor microenvironment while avoiding the side effects associated with chemotherapy, which flows through the bloodstream to most parts of the body.

Therapeutics Award
Michele Cote, PhD
Wayne State University, Karmanos Cancer Institute, Detroit, MI
Funded equally by LUNGevity Foundation and the National Lung Cancer Partnership

Dr. Cote is examining the role of estrogen-related tumor characteristics in predicting differences in survival between men and women after a lung cancer diagnosis. The identification of molecular and genetic profiles associated with survival will help target treatment advances and customize treatment for male and female lung cancer patients.

Therapeutics Award
Alan Patrick Fields, PhD
Mayo Clinic Jacksonville, Jacksonville, FL
Funded equally by LUNGevity Foundation and American Lung Association National Office

Dr. Fields is generating pre-clinical data to support a clinical trial of a novel compound, autothiomalate (ATM), for the treatment of lung cancer. ATM, which is FDA-approved for rheumatoid arthritis, exhibits anti-cancer activity against non-small cell lung cancer (NSCLC) in preclinical studies.