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Dive into the research topics where Donald E. Ingber is active.

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Featured researches published by Donald E. Ingber.


bioRxiv | 2018

Broad spectrum capture of clinical pathogens using engineered Fc-Mannose-Binding Lectin (FcMBL) enhanced by antibiotic treatment

Benjamin T. Seiler; Mark J. Cartwright; Alexandre L.M. Dinis; Shannon L. Duffy; Patrick Lombardo; David Cartwright; Elana H. Super; Jacqueline Lanzaro; Kristen Dugas; Michael Super; Donald E. Ingber

FcMBL, an engineered version of the blood opsonin mannose-binding lectin (MBL) that contains the carbohydrate recognition domain (CRD) and flexible neck regions of MBL fused to the Fc portion of human IgG1, has been shown to bind various microbes and pathogen-associated molecular patterns (PAMPs). FcMBL also has been used to create an enzyme-linked lectin sorbent assay (ELLecSA) for use as a rapid (< 1 hr) diagnostic of bloodstream infections. Here we extended this work by using the ELLecSA to test FcMBL’s ability to bind to more than 200 different isolates from over 100 different pathogen species. FcMBL bound to 86% of the isolates and 110 of the 122 (90%) different pathogen species tested, including bacteria, fungi, viruses, and parasites. It also bound to PAMPs including, lipopolysaccharide endotoxin (LPS) and lipoteichoic acid (LTA) from Gram-negative and Gram-positive bacteria, as well as lipoarabinomannan (LAM) and phosphatidylinositol mannoside 6 (PIM6) from Mycobacterium tuberculosis. The efficiency of pathogen detection and variation between binding of different strains of the same species also could be improved by treating the bacteria with antibiotics prior to FcMBL capture to reveal previously concealed binding sites within the bacterial cell wall. As FcMBL can bind to pathogens and PAMPs in urine as well as blood, its broad-binding capability could be leveraged to develop a variety of clinically relevant technologies, including infectious disease diagnostics, therapeutics, and vaccines.


Archive | 2012

Integrated human organ-on-chip microphysiological systems

John P. Wikswo; Philip C. Samson; Frank E. Block; Ronald S. Reiserer; Kevin Kit Parker; John A. McLean; Lisa J. McCawley; Dmitry A. Markov; Daniel Levner; Donald E. Ingber; Geraldine A. Hamilton; Josue A. Goss; Robert Cunningham; David E. Cliffel; Jennifer R. McKenzie; Anthony Bahinski; Christopher David Hinojosa


Archive | 2011

AEROSOL DRUG DELIVERY FOR LUNG ON A CHIP

Daniel C. Leslie; Karel Domansky; Geraldine A. Hamilton; Anthony Bahinski; Donald E. Ingber


Archive | 2014

Methods of altering vascular permeability and uses thereof

Donald E. Ingber; Akiko Mammoto


Advanced Biosystems | 2017

Circulating Tumor Cells: An Engineered Human Fc-Mannose-Binding-Lectin Captures Circulating Tumor Cells (Adv. Biosys. 7/2017)

Joo H. Kang; Harry Driscoll; Akiko Mammoto; Alexander L. Watters; Bissrat Melakeberhan; Alexander Diaz; Michael Super; Donald E. Ingber


Archive | 2016

Open-top microfluidic devices and methods for simulating a function of a tissue

Antonio Varone; Norman Wen; Daniel Levner; Richard Novak; Lori Mcpartlin; Donald E. Ingber; Youngjae Choe; Lian Leng; Justin Nguyen


Archive | 2016

Systèmes et procédés de suivi, gestion, et traitement de l'asthme et de l'anaphylaxie

Andy H. Levine; Christoph Matthias Kanzler; Aymeric Guy; Daniel L. Miranda; Joseph Mooney; Adam Zapotok; Samel Berry; Huy Lam; Del Río Jonathan Sabaté; John A. Osborne; Mustafa Karabas; Alan Dunne; James Niemi; Benjamin D. Matthews; Donald E. Ingber; Premananda Pai Indic


Archive | 2016

Automated Membrane Fabrication System

James Coon; Tiama Hamkins-Indik; Donald E. Ingber; Miles Ingram; Daniel Levner; Richard Novak; Jefferson Puerta; Daniel E. Shea; Josiah D. Sliz; Norman Wen


Archive | 2016

Gradient microfluidic devices and uses thereof

Donald E. Ingber; Kyung-Jin Jang; Daniel Levner; Norman Wen


Archive | 2016

Pharmacodynamics Analysis Using Organs-on-Chips

Donald E. Ingber; Daniel Levner; Geraldine A. Hamilton; Anthony Bahinski; Rachelle Prantil-Baun

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Akiko Mammoto

Boston Children's Hospital

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