Shannon L. Kelleher, Ph.D. - US grants
Affiliations: | 2002 | University of California, Davis, Davis, CA |
Area:
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High-probability grants
According to our matching algorithm, Shannon L. Kelleher is the likely recipient of the following grants.| Years | Recipients | Code | Title / Keywords | Matching score |
|---|---|---|---|---|
| 2008 — 2012 | Kelleher, Shannon L | R01Activity Code Description: To support a discrete, specified, circumscribed project to be performed by the named investigator(s) in an area representing his or her specific interest and competencies. |
Regulation of Cellular Zn Redistribution: a Role of Znt2 @ Pennsylvania State University-Univ Park [unreadable] DESCRIPTION (provided by applicant): The long-term goal of this application aims to determine how tissues with extraordinary zinc (Zn) requirements, such as mammary gland and prostate, redistribute cellular Zn pools during secretion. Impaired Zn secretion from the mammary gland during lactation results in severe neonatal Zn deficiency. This compromises neuronal and behavioral development, impairs immune function, and increases infant morbidity and/or mortality. Aberrant Zn transport is also implicated in breast cancer. Dysfunctional prostate Zn transport impairs sperm viability and is associated with prostate cancer. These observations underscore the need to understand Zn transport mechanisms in these highly specialized tissues. Zinc transporter-2 (ZnT2) expression is restricted to tissues such as mammary gland and prostate. A mutation in ZnT2 reduces Zn secretion into milk in humans and ZnT2-suppression in mammary epithelial cells reduces Zn secretion in vitro. Discrete ZnT2 isoforms have been identified which are associated with mitochondria (mZnT2) and intracellular vesicles (sZnT2) in mammary epithelial cells. Mitochondrial Zn uptake and Zn concentration parallels mZnT2 abundance, while Zn secretion parallels sZnT2 abundance. Similar to observations in prostate cells, the hormone prolactin shifts Zn distribution in mammary epithelial cells. Prolactin contracts mitochondrial Zn pools while concurrently increasing Zn transport. This redistribution is associated with decreased mZnT2 and increased sZnT2 abundance. We hypothesize that prolactin regulates discrete ZnT2 isoforms to redistribute cellular Zn pools from mitochondria to secretory vesicles to facilitate extraordinary Zn secretion in highly specialized secretory tissues. We propose to use the mammary gland as a representative system to explore potential mechanisms responsible for cellular Zn redistribution using animal and cell models. The four specific aims of this application are to, (1) determine if mitochondrial ZnT2 facilitates expansion of a mitochondrial Zn pool using genomic and proteomic approaches; (2) determine mechanisms by which prolactin redistributes cellular Zn pools through changes in sZnT2 during secretion; (3) develop a transgenic mammary gland mouse model to determine if cellular Zn pools are redistributed by mZnT2 and sZnT2 in vivo; (4) develop a ZnT2-null mouse model to document the biological significance ZnT2 and determine if other Zn transporters participate in Zn pool redistribution in mammary gland and prostate in vivo. Taken together, these studies will identify specific mechanisms which regulate cellular Zn redistribution in highly specialized tissues and are crucial to our understanding of cellular function, Zn metabolism and human health and disease. The mammary and prostate glands are highly specialized secretory tissues that are responsible for extraordinary Zn secretion. Impaired Zn secretion from the mammary gland during lactation results in severe neonatal Zn deficiency which compromises neuronal and behavioral development, impairs immune function, and increases infant morbidity and/or mortality. Aberrant Zn transport is also implicated in breast cancer. Dysfunctional Zn transport in prostate has been implicated in prostate cancer, sperm viability and impaired reproductive function. These observations underscore the need to understand Zn transport mechanisms in these unique tissues. Thus, this application has significance for improving public health outcomes and advancing our understanding of basic cellular mechanisms. PUBLIC HEALTH RELEVANCE: The mammary and prostate glands are highly specialized secretory tissues that are responsible for extraordinary Zn secretion. Impaired Zn secretion from the mammary gland during lactation results in severe neonatal Zn deficiency which compromises neuronal and behavioral development, impairs immune function, and increases infant morbidity and/or mortality. Aberrant Zn transport is also implicated in breast cancer. Dysfunctional Zn transport in prostate has been implicated in prostate cancer, sperm viability and impaired reproductive function. These observations underscore the need to understand Zn transport mechanisms in these unique tissues. Thus, this application has significance for improving public health outcomes and advancing our understanding of basic cellular mechanisms. [unreadable] [unreadable] [unreadable] |
0.933 |
| 2012 | Kelleher, Shannon L Winge, Dennis R. |
R13Activity Code Description: To support recipient sponsored and directed international, national or regional meetings, conferences and workshops. |
Faseb Src 2012 On Trace Elements in Biology and Medicine @ Federation of Amer Soc For Exper Biology DESCRIPTION (provided by applicant): The FASEB Summer Research Conference on Trace Elements in Biology and Medicine will be held in Steamboat Springs, Colorado, June 10 - 15, 2012. This will be the 12th conference in the Trace Element meting series and the conference has become a key cornerstone meeting in the field of metal ions in biology. Trace elements are of vital importance in biology, medicine, and agriculture, and as such have great impact on human health. The 2012 FASEB conference will primarily focus on discussions of research findings from cutting-edge investigations related to metabolism of iron (Fe), zinc (Zn), copper (Cu) and selenium (Se) and their role in human health and disease. Cell signaling by metal ions is a rapidly developing area of trace element research to be addressed. The conference will bring together basic, applied and clinical scientist to share and discuss the most exciting and important breakthroughs in understanding of both basic and applied aspects of trace element homeostasis and metabolism. This conference spans a range of scientific interests from developmental biology, genetics, biochemistry, chemistry, nutrition and clinical medicine. The FASEB conference has been highly successful in fostering fruitful collaborations in this field and integrating molecular, nutritional and biomedical research. The meeting aims to draw together established investigators and trainees to promote communication, mentoring, collaborations and share advances in methodologies. PUBLIC HEALTH RELEVANCE: The FASEB Summer Research Conference on Trace Elements in Biology and Medicine will focus on timely and significant advances in understanding the roles of trace element metal metabolism in biology. Trace elements occupy an important intersection of biology and medicine as illustrated by the wide range of diseases and disorders associated with defects in trace element metabolism. Metal ion biology is important to human health and nutrition in addition to agriculture. The conference has a critical role in bridging basc and applied research in the area of trace element metabolism. |
0.91 |