عنوان
پدید آورنده
موضوع
رده
کتابخانه
محل استقرار
شماره کتابشناسی ملی
شماره
TL9782h91g
زبان اثر
زبان متن نوشتاري يا گفتاري و مانند آن
انگلیسی
عنوان و نام پديدآور
عنوان اصلي
Structure-function effects of mutations in domains of Inducible Tyrosine Kinase
نام عام مواد
[Thesis]
نام نخستين پديدآور
Levytskyy, Roman Myroslavovych
وضعیت نشر و پخش و غیره
تاریخ نشرو بخش و غیره
2012
یادداشتهای مربوط به پایان نامه ها
امتياز متن
2012
یادداشتهای مربوط به خلاصه یا چکیده
متن يادداشت
The dissertation is studying structural mutants of various domains of the Inducible Tyrosine Kinase (Itk), and their relation to functionality of this protein in immune cells. Using cell lines as well as primary cells from Itk-/- mice, and employing systematic functional study approach this work is exploring effects of several mutations (Y511F, BtkSH3, FYF) on immediate, and far downstream signaling of Itk under conditions of TCR induced stimulation. Structural (FRET), as well as biochemical and molecular biology techniques were used (western blotting, flow cytometry, ELISA). It was shown that Itk does not exhibit noticeable differences neither in structure, nor in localization in resting cells, but changes conformation and localization patterns under stimulation in T-cell-APC system. This event is pronounced in statistically significant manner in wild type Itk, but is disrupted to different extent in mutants. PH domain mutant FYF is the only one from those explored that has disrupted localization pattern, and surprisingly, nonfunctional activation residue mutant Y511F preserves intact localization. However, all mutants show disruption in structural pattern when compared to wild type Itk. Another novel finding is related to Itk-SLP-76 interaction, which proved to be disrupted in BtkSH3 mutant that lacks noncanonical SH3 domain interactions, pointing on important role of noncanonical SH3 interactions in signaling of Itk in complex with SLP-76, and as a result in activation of Itk. All mutants show some extent of disruption in Y511 phosphorylation, which has a direct effect on downstream events as assessed by PLC[Gamma] phosphorylation, and reflects defects in structure and localization patterns, with mutants being significantly deficient comparing to wild type. This results in even more pronounced effect in Th2 cytokine production, and this dissertation provides the first evidence of the influence of these mutants on Th2 cytokines, which are the signature cytokines of Itk. The dissertation proposes explanations of the mentioned phenomena, underlines an importance of different parts of Itk molecule in its functionality, and makes possible to apply the data acquired here to further understand the role of Itk in deeper detail with possible clinical implications in the future
نام شخص به منزله سر شناسه - (مسئولیت معنوی درجه اول )
مستند نام اشخاص تاييد نشده
Saulnier, Eric Scott
نام شخص - ( مسئولیت معنوی درجه دوم )
مستند نام اشخاص تاييد نشده
Levytskyy, Roman Myroslavovych
شناسه افزوده (تنالگان)
مستند نام تنالگان تاييد نشده
UC San Diego
دسترسی و محل الکترونیکی
نام الکترونيکي
مطالعه متن کتاب وضعیت انتشار
فرمت انتشار
p
اطلاعات رکورد کتابشناسی
نوع ماده
[Thesis]
کد کاربرگه
276903
اطلاعات دسترسی رکورد
سطح دسترسي
a
تكميل شده
Y
