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Avery August, PhD

Professor of Immunology

101 Henning Building
University Park, PA 16802

Email: axa45@psu.edu

Phone: (814) 863-3539

Education:

Postdoctoral training, Laboratory of Molecular Oncology, The Rockefeller University, New York (with Dr. Hidesaburo Hanafusa)
Ph.D., Immunology, Cornell University (with Dr. Bo Dupont)
B.S., Medical Technology, California State University , Los Angeles

Biography:

Regulation of immune response by intracellular signaling events.

We are interested in the role of Tyrosine Kinases (TKs) in regulating the immune response, with the goal of using this information to manipulate immune responses. We are specifically interested in the Tec families of nonreceptor TKs.

Regulation of T cell activation and function by Tec family kinases.

Regulation of T cell activation, differentiation and allergic asthma induction by Tec family kinases

Itk is a member of the Tec family of tyrosine kinases. Mice lacking Itk have T-cell defects, including reduced intracellular calcium increases during T cell activation and defective Th2 development. Understanding the specific downstream activities of these kinases is crucial to understanding how they impact lymphoid activation and development.

We have recently shown that the SH3 domain functionally interacts with the Proline Rich region of ITK, regulating both basal and activation induced kinase activity. We have also recently shown that mice lacking ITK a resistant to developing immunological symptoms of allergic asthma, a disease primarily driven by Th2 type T cells. Finally, we have recently shown that Tec kinases regulate the activation of the transcription factor Serum Response Factor (SRF), and that calcium mediated pathways differentially regulate the activation of SRF and the transcription factor NFAT, such that SRF has a lower requirement for calcium, while NFAT is absolutely dependent on calcium increase, regulated by Tec kinases. We are currently pursuing the signaling pathways regulated by Tec family kinases in vitro and in vivo, using the Th2 mediated disease allergic asthma as a model. Our recent data suggest that Itk controls the development of allergic asthma by regulating the development of Th2 responses, but also by regulating the ability of T cells to migrate into the lung.

Regulation of T cell development by Tec family kinases

We have recently shown that in the absence of Itk, a population of CD8 + T cells that have a memory phenotype (CD8 + CD44 + CD122 hi ) predominates. Our analysis of these cells indicate that they develop in the absence of direct signaling by Itk since they are present in transgenic mice carrying a mutant Itk with no kinase domain. We also showed that these cells have intrinsic innate immune function as the carry preformed message for the cytokine IFN gamma , and can this cytokine in response to IL-12/IL-18 stimulation. Our data suggest that these cells allow Itk null mice to effectively respond to infection with L. monocytogenes or exposure to LPS by secretion of IFN gamma . Confirming this, our experiments show that transfer of these cells rescues IFN gamma null mice during Listeria infection. We are continuing to study the function and behavior of this population of memory T cells with innate function.

Regulation of Mast cell activation and function by Tec family kinases

Itk is also expressed in mast cells, and has been shown to be activated when IgE interacts with the receptor for IgE (FcepsilonR) in these cells. Our recent experiments have started to examine the role of Itk in regulating the response of these cells to stimulation via the FcepsilonR. These experiments have implicates for the control of allergic responses, as well as those disease in which mast cells play a critical role.

Regulation of allergic asthma by eosinophils

The presence of eosinophils in patients in asthma has long been recognized. However, their specific role in this disease is unclear. It is even unclear whether they are required for the development of this disease as the evidence is mixed. We are interested in defining the role of these cells in this disease. Using a mouse model of this disease, we have recently shown that eosinophils are required for T cells to enter the lung during the development of allergic asthma. We are continuing our analysis of the role of eosinophils in the development of allergic asthma.

Lab Members

Avery August - Center for Molecular Immunology & Infectious Disease & Dept. of Veterinary & Biomedical Sciences
Chavez Carter – Pathobiology Graduate Student
Ayesha Fraser - Undergraduate Student
Margaret Kensinger - Research Technician
Man Kit Law - Immunology & Infectious Disease Graduate Student
Sonia Mohinta - Pathobiology Graduate Student
Luis Morales - Post-Doc
Meg Potter - Research Technician
Patrick Power - Schreyers Scholar, Undergraduate Student
Qian Qi - Post-Doctoral Fellow
Kindra Stokes - Pathobiology Graduate Student
Weishan Huang - Cell & Developmental Biology Graduate Student
Arun Kumar - Immunology & Infectious Disease Graduate Student
Lina Khong - Schreyers Scholar, Undergraduate Student
Allison Neely - Schreyers Scholar, Undergraduate Student
Tammy Terosky - Research Technician
Adam Winters - Undergraduate Student
Elizabeth Fernandez - Undergraduate Student

Lab Alumni

Shengli Hao......California Institute of Technology
Angela Fischer...... Johns Hopkins University School of Medicine
Nawel Mahrour......Stowers Institute for Medical Research
Jason Mercer......National Institute for Environmental Health Sciences, NIH<
Melanie Ragin... Director, Graduate Program in Public Health, Fort valley State university, GA
Jianfang Hu..... Scripps Research Institute
Elizabeth Walsh....NIAID, NIH
Nisibeta Sahu.....Mass. Gen. Hosp/Harvard Medical School
Selected Publications (by research area):

T helper cell differentiation and Allergic Asthma:

Sahu N, Venegas AM, Jankovic D, Mitzner W, Gomez-Rodriguez J, Cannons JL, Sommers C, Love P, Sher A, Schwartzberg PL, August A. "Selective expression rather than specific function of Txk and Itk regulate Th1 and Th2 responses." J Immunol. 2008 181:6125-31.

Sahu N, Mueller C, Fischer A, August A. “Differential sensitivity to Itk kinase signals for T helper 2 cytokine production and chemokine-mediated migration.” J Immunol. 2008 180:3833-8. Erratum in: J Immunol. 2008 180:7047-8.

Mueller C, August A. "Attenuation of immunological symptoms of allergic asthma in mice lacking the tyrosine kinase ITK.". J Immunol. 170:5056-63, (2003)

Role of Itk in Mast cell function:

Iyer AS, August A. “The Tec family kinase, IL-2-inducible T cell kinase, differentially controls mast cell responses.” J Immunol. 2008 180:7869-77.

Role of Eosinophils in development of Allergic Asthma:

Walsh ER, Sahu N, Kearley J, Benjamin E, Kang BH, Humbles A, August A. “Strain-specific requirement for eosinophils in the recruitment of T cells to the lung during the development of allergic asthma.” J Exp Med. 2008 205:1285-92.

Role of Itk in the development of “naïve” and “innate memory-phenotype T cells”:

Hu J, August A.”Naive and innate memory phenotype CD4+ T cells have different requirements for active Itk for their development.” J Immunol. 2008 180:6544-52.

Hu J, Sahu N, Walsh E, August A.” Memory phenotype CD8+ T cells with innate function selectively develop in the absence of active Itk.” Eur J Immunol. 2007 37:2892-9.

Role of Itk in regulation of HIV replication:

Readinger JA, Schiralli GM, Jiang JK, Thomas CJ, August A, Henderson AJ, Schwartzberg PL. “Selective targeting of ITK blocks multiple steps of HIV replication.” Proc Natl Acad Sci U S A. 2008 105:6684-9.

Cook JA, Albacker L, August A, Henderson AJ."CD28-dependent HIV-1 transcription is associated with Vav, Rac, and NF-kappa B activation.” J. Biol. Chem 2003 278:35812-8.

Cook JA, August A, Henderson A” Recruitment of phosphatidylinositol 3-kinase to CD28 inhibits HIV transcription by a Tat-dependent mechanism.” J. Immunol. 2002 169:254-60.

Role of Tec kinases in antigen receptor signaling:

Qi Q and August A. "Keeping the (kinase) party going: SLP-76 and ITK dance to the beat." Science STKE. 396:pe39. (2007).

Qi Q, Sahu N and August A . "Tec kinase Itk forms membrane clusters specifically in the vicinity of recruiting receptors." J. Biol. Chem 281, 38529-38534 (2006).

Hao S, Qi Q, Hu J and August A . "A kinase independent function for Tec kinase ITK in regulating antigen receptor induced serum response factor activation." Febs. Letts. 580:2691-2697 (2006).

Hao S and August A. "Actin depolymerization transduces the strength of B-cell receptor stimulation.". Mol. Biol. Cell 16:2275-2284, (2005).

Hao S, Kurosaki T, August A. "Differential regulation of NFAT and SRF by the B cell receptor via a PLCgamma-Ca(2+)-dependent pathway." EMBO J. 22:4166-77, (2003)

Woods ML, Kivens WJ, Adelsman MA, Qiu Y, August A, Shimizu Y. A novel function for the Tec family tyrosine kinase Itk in activation of beta 1 integrins by the T-cell receptor. EMBO J. 20:1232-44, (2001)

Misc:

Boonyarattanakalin S, Hu J, Dykstra-Rummel SA, August A and Peterson BR. "Endocytic delivery of vancomycin mediated by a synthetic cell surface receptor: rescue of bacterially infected Mammalian cells and tissue targeting in vivo." J. Amer. Chem. Soc. 129, 268-9 (2007).

Ragin MJ, Sahu N and August A. "Differential regulation of cytokine production by CD1d-restricted NKT cells in response to superantigen staphylococcal enterotoxin B exposure." Infec. & Imm. 74:282-8 (2006).

Fischer AM, Mercer JC, Iyer A, Ragin MJ, August A. "Regulation of CXC chemokine receptor 4-mediated migration by the Tec family tyrosine kinase ITK". J Biol Chem. 279:29816-20, (2004)