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Dive into the research topics where David M. Kranz is active.

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Featured researches published by David M. Kranz.


Journal of Biological Chemistry | 2003

Dissecting Cooperative and Additive Binding Energetics in the Affinity Maturation Pathway of a Protein-Protein Interface

Jianying Yang; Chittoor P. Swaminathan; Yuping Huang; Rongjin Guan; Sangwoo Cho; Michele C. Kieke; David M. Kranz; Roy A. Mariuzza; Eric J. Sundberg

When two proteins associate they form a molecular interface that is a structural and energetic mosaic. Within such interfaces, individual amino acid residues contribute distinct binding energies to the complex. In combination, these energies are not necessarily additive, and significant positive or negative cooperative effects often exist. The basis of reliable algorithms to predict the specificities and energies of protein-protein interactions depends critically on a quantitative understanding of this cooperativity. We have used a model protein-protein system defined by an affinity maturation pathway, comprising variants of a T cell receptor Vβ domain that exhibit an overall affinity range of ∼1500-fold for binding to the superantigen staphylococcal enterotoxin C3, in order to dissect the cooperative and additive energetic contributions of residues within an interface. This molecular interaction has been well characterized previously both structurally, by x-ray crystallographic analysis, and energetically, by scanning alanine mutagenesis. Through analysis of group and individual maturation and reversion mutations using surface plasmon resonance spectroscopy, we have identified energetically important interfacial residues, determined their cooperative and additive energetic properties, and elucidated the kinetic and thermodynamic bases for molecular evolution in this system. The summation of the binding free energy changes associated with the individual mutations that define this affinity maturation pathway is greater than that of the fully matured variant, even though the affinity gap between the end point variants is relatively large. Two mutations in particular, both located in the complementarity determining region 2 loop of the Vβ domain, exhibit negative cooperativity.


Archive | 2000

Proteines des recepteurs de leucocytes t (tcr) a affinite elevee et procedes correspondants

David M. Kranz; K. Dane Wittrup; Phillip D. Holler


Archive | 2000

High affinity t-cell receptor proteins and methods

David M. Kranz; K. Dane Wittrup; Phillip D. Holler


Archive | 2000

Hochaffine t-zellrezeptorproteine und verfahren High affinity T cell receptor proteins and methods

David M. Kranz; K. Dane Wittrup; Phillip D. Holler


Archive | 1999

Presenting proteins on the surface of yeast cells and their uses

K. Dane Wittrup; Michele C. Kieke; David M. Kranz; Eric V. Shusta; Eric T. Boder


Archive | 1999

Hefezellen-oberflächenprotein-display und dessen verwendung

K. Dane Wittrup; Michele C. Kieke; David M. Kranz; Eric V. Shusta; Eric T. Boder


Archive | 1999

Hefezellen-Oberflächen-Display von Proteinen sowie Verwendungen diesbezüglich

Dane K. Wittrup; Michele C. Kieke; David M. Kranz; Eric V. Shusta; Eric T. Boder


Archive | 1999

Hefezellenoberflächen-Display von Proteinen und Verwendungen diesbezüglich

Dane K. Wittrup; Michele C. Kieke; David M. Kranz; Eric V. Shusta; Eric T. Boder


Archive | 1999

Proteines pour la presentation de la surface d'une cellule de levure et leurs utilisations

K. Dane Wittrup; Michele C. Kieke; David M. Kranz; Eric V. Shusta; Eric T. Boder


Archive | 1999

Yeast cell surface of proteins having enhanced properties

K. Dane Wittrup; Michele C. Kieke; David M. Kranz; Eric V. Shusta; Eric T. Boder

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Eric V. Shusta

University of Wisconsin-Madison

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K. Dane Wittrup

Massachusetts Institute of Technology

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Chittoor P. Swaminathan

University of Maryland Biotechnology Institute

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Eric J. Sundberg

Boston Biomedical Research Institute

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Rongjin Guan

University of Maryland Biotechnology Institute

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Sangwoo Cho

University of Maryland Biotechnology Institute

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