ImmunoX Faculty Directory

The Faculty Directory lists faculty members and associates associated with the Bakar ImmunoX Initiative, showing their name, title, and a link to view their profile.

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Elena Nedelcu
Associate Professor
Elena Nedelcu
Associate Professor
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Stephen Nishimura
Professor
Stephen Nishimura
Professor
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Philip Norris
Professor
Philip Norris
Professor
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Melanie Ott
Professor
Melanie Ott
Professor
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Karin Pelka
Assistant Professor
Karin Pelka
Assistant Professor
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Tien Peng
Associate Professor
Tien Peng
Associate Professor
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Rushika Perera
Associate Professor
Rushika Perera
Associate Professor
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B. Matija Peterlin
Professor Emeritus
B. Matija Peterlin
Professor Emeritus
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Angela Phillips
Assistant Professor
Angela Phillips
Assistant Professor
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Joanna Phillips
Professor
Joanna Phillips
Professor
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Xianhua Piao
Professsor
Xianhua Piao
Professsor
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Satish Pillai
Professor
Satish Pillai
Professor
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Samuel Pleasure
samuel-pleasure

The Pleasure lab studies autoantibody associated meningoencephalitis. We use a coordinated approach to identify novel autoantibodies and also we study the pathophysiology of known autoantibodies in neurologic disease.

Arun Prakash
arun-prakash

The Prakash Lab studies the immunobiology of lung injury - both sterile and infectious - and investigates lung cellular and molecular signaling contributions as well as the immuno-metabolic influence of the microbiome on the lung.

Aric Prather
aric-prather

The Prather Lab focuses on the influence of psychological and behavioral factors on immune function in humans. Much of this work has focused on the impact of acute and chronic psychological stress on markers of immunological aging and the effect of insufficient sleep (measured in lab using sleep deprivation protocols and in the field) on inflammatory functioning and susceptibility to infectious illness.

Jennifer Puck
jennifer-puck

The Puck Lab focuses on genetic and genomic technology as well as cellular immunology to study human immune disorders and models of lymphocyte development. These studies have resulted in discoveries of new gene defects, including BCL11B, CORO1A and others. Noting the better outcomes for infants with severe combined immunodeficiency (SCID) after diagnosis early in life, Dr. Puck conceived and developed newborn screening for SCID in DNA extracted from infant dried blood spots. This test, now part of standard newborn screening in all 50 states, uses PCR to quantitate T cell receptor excision circles (TRECs), byproducts of T cell receptor rearrangement in the thymus. Absent or low TRECs identify SCID, and also other conditions with T cell insufficiency. Dr. Puck is also advancing new therapies for SCID, with a clinical trial of lentivirus gene therapy for X-linked and a first-in-human Phase I/II study of lentiviral gene therapy for Artemis deficient SCID.

Robert Raffai
robert-raffai

The Raffai Lab investigates the biology of atherosclerosis. Through our studies, we strive to develop a more profound understanding of the immune system's participation in vascular wall inflammation and atherosclerosis. Our long-term goal is to develop approaches to control the immune systems participation in atherosclerosis initiation and progression. Furthermore, we seek to harness anti������ inflammatory and tissue-remodeling properties of the immune system to promote atheroma stabilization and its regression as new treatments for cardiov

Rajalingam Raja
rajalingam-raja

Dr. Raja is the Director of the UCSF Immunogenetics and Transplantation Laboratory (UCSF-ITL). The ITL laboratory is a core HLA typing lab for Immune Tolerance Network, a research cooperative focused on the development of therapeutic approached for asthma and allergy, autoimmune diseases, type 1 diabetes and solid organ transplantation that lead to immune tolerance. Our current research centers on three themes: 1) to understand the basis of alloimmuneresponse in clinical transplantation to identify acceptable mismatches and tolerable donor-specific HLA antibodies, which will help designing functional histocompatibility matching for better transplant outcomes; 2) to understand the functional polymorphism of immunity related genes (HLA, KIR, KLR, FCGR) in human populations and impact on infections, tumor transformation, autoimmune diseases, pregnancy success and allogeneic transplantation; 3) to understand the complex relationship between polymorphic Natural Killer cell receptors (KIR receptors) and HLA class I ligands and the influence on human disease and transplant outcomes.

Aleksandar Rajkovic
aleksandar-rajkovic

The Rajkovic Lab investigates the genetic underpinnings of the formation and differentiation of gametes and reproductive tract, their role of these genes in human disease, embryo lethality and origin of heritable human disorders. More specicifally, their lab studies transcriptional regulation of ovarian follicle activation and oocyte survival and how these processes are essential to produce healthy egg. Whole genome human studies in their laboratory discovered that DNA damage repair genes such as MCM8 and MCM9 are mutated in women with infertility and the lab is exploring the link bettheyen DNA damage repair genes with infertility phenotypes and accelerated overall aging, as theyll as the effect of these genes on the overall health of offspring and genesis of structural birth defects. These and other studies indicate that many of the reproductive disorders are developmental in origin.

Roberto Ricardo-Gonzalez
roberto-ricardo-gonzalez

The Ricardo-Gonzalez lab's overarching goal is to understand how tissue-resident immune cells respond to physiologic and pathologic stimuli and how they can influence changes across multiple cell lineages in barrier tissues.

Nadia Roan
nadia-roan

The Roan Lab studies how intracellular and extracellular factors in the tissue microenvironment can affect infection by HIV, mucosal immunity, and reproductive health. They have demonstrated that genital and rectal fibroblasts, amongst the most abundant cells of the mucosa, potently increase HIV infection of T cells through at least two distinct mechanisms: promoting viral entry, and altering the cellular state of T cells to render them more permissive to viral replication. To characterize the molecular basis of how intrinsic and extrinsic perturbations can render some subsets of CD4+ T cells more susceptible than others to HIV infection, they are using a variety of global gene expression analysis approaches, including CyTOF and RNA-seq. These approaches are also being used to characterize the HIV latent reservoir and the nature of viral rebound upon antiretroviral treatment interruption. Another research interest in the lab is to understand how factors in seminal plasma affect reproductive health and susceptibility to sexually transmitted diseases.

Jeroen Roose
jeroen-roose

Jeroen Roose is a tenured Principal Investigator and Vice Chair of Anatomy at the University of California, San Francisco. He is also a co-founder of UCSF's Bakar ImmunoX Immunology Program and co-lead of UCSF's AutoIPI (AutoImmunoProfiler). The Roose lab focuses on understanding cell fate decisions driven by cell-cell interactions and signaling pathways, in the context of cancer and autoimmune diseases. Dr. Roose also runs an Organoid disease to biology unit connected to UCSF's CoLabs. There is a rich training environment for staff, students, postdocs, and fellows in the established infrastructure of the Roose lab and the programs it is connected to.

Steven Rosen
steven-rosen

The Rosen Lab is interested in glycobiology and biological sulfation. The origin of this interest began 30 years ago with our investigation of molecular mechanisms involved in lymphocyte homing to lymph nodes. Over the past 12 years, we have been focusing on the role of the SULFs in cancer, triggered by our finding that one or both SULFs are commonly overexpressed in cancers. Following our initial studies of the SULFs in breast cancer and pancreatic cancer, we have focused on the study of these enzymes in non-small cell lung cancer (NSCLC). Our studies have documented widespread overexpression of SULF2 protein in human NSCLC tumors. Employing a series of tumorigenic lung cancer cell lines, we showed that SULF2 promotes the malignant properties of these cells in both in vitro and vivo assays, including the formation of xenograft tumors in nude mice. We have developed a very sensitive ELISA for SULF2 and have detected the enzyme in human blood. Current studies are directed at determining whether the SULFs could serve as cancer biomarkers in blood or other body fluids.

Michael Rosenblum
michael-rosenblum

The Rosenblum Lab's central focus is to understand how the immune system is regulated or controlled in peripheral tissues and how this knowledge can be exploited for therapeutic benefit. To this end, we currently have two areas of active investigation: 1) Understanding how regulatory T cells (Tregs) control immune responses outside of lymphoid organs and 2) Understanding the 'alternative' functions of Tregs in peripheral tissues. Because of its complex immunological properties, its accessibility, and potential for clinical translation, the skin is the model peripheral tissue that we primarily focus on. Approximately 50% of our research employs a reductionist approach, utilizing transgenic animal models to ask fundamental questions of how the immune system functions in skin (and other peripheral tissues) at both the cellular and molecular levels. The other half of our work focuses on doing functional immunology with human tissue, human blood and humanized mice.