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Dive into the research topics where Jackson Dean Harvey is active.

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Featured researches published by Jackson Dean Harvey.


Nature Biomedical Engineering | 2017

A carbon nanotube reporter of microRNA hybridization events in vivo

Jackson Dean Harvey; Prakrit V. Jena; Hanan A. Baker; Gül H. Zerze; Ryan M. Williams; Thomas Vito Galassi; Daniel Roxbury; Jeetain Mittal; Daniel A. Heller

MicroRNAs and other small oligonucleotides in biofluids are promising disease biomarkers, yet conventional assays require complex processing steps that are unsuitable for point-of-care testing or for implantable or wearable sensors. Single-walled carbon nanotubes are an ideal material for implantable sensors, owing to their emission in the near-infrared spectral region, photostability and exquisite sensitivity. Here, we report an engineered carbon-nanotube-based sensor capable of real-time optical quantification of hybridization events of microRNA and other oligonucleotides. The mechanism of the sensor arises from competitive effects between displacement of both oligonucleotide charge groups and water from the nanotube surface, which result in a solvatochromism-like response. The sensor, which allows for detection via single-molecule sensor elements and for multiplexing by using multiple nanotube chiralities, can monitor toehold-based strand-displacement events, which reverse the sensor response and regenerate the sensor complex. We also show that the sensor functions in whole urine and serum, and can non-invasively measure DNA and microRNA after implantation in live mice.


ACS Nano | 2017

A Carbon Nanotube Optical Reporter Maps Endolysosomal Lipid Flux

Prakrit V. Jena; Daniel Roxbury; Thomas Vito Galassi; Leila Akkari; Christopher Peter Horoszko; David B. Iaea; Januka Budhathoki-Uprety; Nina H. Pipalia; Abigail S. Haka; Jackson Dean Harvey; Jeetain Mittal; Frederick R. Maxfield; Johanna A. Joyce; Daniel A. Heller

Lipid accumulation within the lumen of endolysosomal vesicles is observed in various pathologies including atherosclerosis, liver disease, neurological disorders, lysosomal storage disorders, and cancer. Current methods cannot measure lipid flux specifically within the lysosomal lumen of live cells. We developed an optical reporter, composed of a photoluminescent carbon nanotube of a single chirality, that responds to lipid accumulation via modulation of the nanotube’s optical band gap. The engineered nanomaterial, composed of short, single-stranded DNA and a single nanotube chirality, localizes exclusively to the lumen of endolysosomal organelles without adversely affecting cell viability or proliferation or organelle morphology, integrity, or function. The emission wavelength of the reporter can be spatially resolved from within the endolysosomal lumen to generate quantitative maps of lipid content in live cells. Endolysosomal lipid accumulation in cell lines, an example of drug-induced phospholipidosis, was observed for multiple drugs in macrophages, and measurements of patient-derived Niemann–Pick type C fibroblasts identified lipid accumulation and phenotypic reversal of this lysosomal storage disease. Single-cell measurements using the reporter discerned subcellular differences in equilibrium lipid content, illuminating significant intracellular heterogeneity among endolysosomal organelles of differentiating bone-marrow-derived monocytes. Single-cell kinetics of lipoprotein-derived cholesterol accumulation within macrophages revealed rates that differed among cells by an order of magnitude. This carbon nanotube optical reporter of endolysosomal lipid content in live cells confers additional capabilities for drug development processes and the investigation of lipid-linked diseases.


Science Advances | 2018

Noninvasive ovarian cancer biomarker detection via an optical nanosensor implant

Ryan M. Williams; Christopher Lee; Thomas Vito Galassi; Jackson Dean Harvey; Rachel Leicher; Maria Sirenko; Madeline A. Dorso; Janki Shah; Narciso Olvera; Fanny Dao; Douglas A. Levine; Daniel A. Heller

Ovarian cancer biomarker detection using a novel nanosensor implant in live mice. Patients with high-grade serous ovarian carcinoma (HGSC) exhibit poor 5-year survival rates, which may be significantly improved by early-stage detection. The U.S. Food and Drug Administration–approved biomarkers for HGSC—CA-125 (cancer antigen 125) and HE4 (human epididymis protein 4)—do not generally appear at detectable levels in the serum until advanced stages of the disease. An implantable device placed proximal to disease sites, such as in or near the fallopian tube, ovary, uterine cavity, or peritoneal cavity, may constitute a feasible strategy to improve detection of HGSC. We engineered a prototype optical sensor composed of an antibody-functionalized carbon nanotube complex, which responds quantitatively to HE4 via modulation of the nanotube optical bandgap. The complexes measured HE4 with nanomolar sensitivity to differentiate disease from benign patient biofluids. The sensors were implanted into four models of ovarian cancer, within a semipermeable membrane, enabling the optical detection of HE4 within the live animals. We present the first in vivo optical nanosensor capable of noninvasive cancer biomarker detection in orthotopic models of disease.


Journal of Materials Chemistry B | 2017

Polymer cloaking modulates the carbon nanotube protein corona and delivery into cancer cells

Januka Budhathoki-Uprety; Jackson Dean Harvey; Elizabeth Isaac; Ryan M. Williams; Thomas Vito Galassi; Rachel E Langenbacher; Daniel A. Heller

Carbon nanotube-based molecular probes, imaging agents, and biosensors in cells and in vivo continue to garner interest as investigational tools and clinical devices due to their unique photophysical properties. Surface chemistry modulation of nanotubes plays a critical role in determining stability and interaction with biological systems both in vitro and in vivo. Among the many parameters that influence the biological fate of nanomaterials, surface charge is particularly influential due to direct electrostatic interactions with components of the cell membrane as well as proteins in the serum, which coat the nanoparticle surface in a protein corona and alter nanoparticle-cell interactions. Here, we modulated functional moieties on a helical polycarbodiimide polymer backbone that non-covalently suspended the nanotubes in aqueous media. By derivatizing the polymer with either primary amine or carboxylic acid side chains, we obtained nanotube complexes that present net surface charges of opposite polarity at physiological pH. Using these materials, we found that the uptake of carbon nanotubes in these cells is highly dependent on charge, with cationic nanotubes efficiently internalized into cells compared to the anionic nanotubes. Furthermore, we found that serum proteins drastically influenced cell uptake of the anionic nanotubes, while the effect was not prominent for the cationic nanotubes. Our findings have implications for improved engineering of drug delivery devices, molecular probes, and biosensors.


ACS Applied Materials & Interfaces | 2017

Control of Carbon Nanotube Solvatochromic Response to Chemotherapeutic Agents

Jackson Dean Harvey; Hanan A. Baker; Elizabeth Mercer; Januka Budhathoki-Uprety; Daniel A. Heller

Alkylating agents such as cisplatin play an essential role in chemotherapy regimens, but initial and acquired resistance in many cancer types often dampen therapeutic response. The poor understanding of the mechanisms of resistance highlight the need for quantitative measurements of alkylating agent distribution at both the tissue and subcellular levels. Sensors for use in live animals and cells would allow for more effective study of drug action and resistance. Toward this end, single-walled carbon nanotubes suspended with single-stranded DNA have suitable optical properties for in vivo sensors, such as near-infrared emission and sensitivity to the local environment via solvatochromic responses. Currently, solvatochromic changes of such sensors have been limited by the chemical nature of the analyte, making it impossible to control the direction of energy emission changes. Here, we describe a new approach to control the direction and magnitude of solvatochromic responses of carbon nanotubes. We found that the alkylation of DNA on the nanotube surface can result in small changes in DNA conformation that allow the adsorption of amphiphiles to produce large differences (>14 nm) in response to different drugs. The technique surprisingly revealed differences among drugs upon alkylation. The ability to control carbon nanotube solvatochromism as desired may potentially expand the application of nanotube-based optical sensors for new classes of analytes.


Journal of Physical Chemistry C | 2018

Electrostatic Screening Modulates Analyte Binding and Emission of Carbon Nanotubes

Jackson Dean Harvey; Gül H. Zerze; Kathryn M. Tully; Jeetain Mittal; Daniel A. Heller


Cancer Research | 2017

Abstract LB-222: A nanoscale optical reporter implant for miRNA biomarkersin vivo

Daniel A. Heller; Jackson Dean Harvey; Prakrit V. Jena; Ryan M. Williams; Thomas Vito Galassi; Hanan A. Baker; Daniel Roxbury; Gül H. Zerze; Jeetain Mittal


231st ECS Meeting (May 28 - June 1, 2017) | 2017

Single-Walled Carbon Nanotubes for the Quantification of Active Chemotherapy Drugs

Jackson Dean Harvey; Hanan A. Baker; Thomas Vito Galassi; Ryan M. Williams; Daniel A. Heller


231st ECS Meeting (May 28 - June 1, 2017) | 2017

Invited) Developments in Modulating Carbon Nanotube Photoluminescence

Daniel A. Heller; Januka Budhathoki-Uprety; Thomas Vito Galassi; Jackson Dean Harvey; Christopher Peter Horoszko; Prakrit V. Jena; Rachel E Langenbacher; Daniel Roxbury; Ryan M. Williams


231st ECS Meeting (May 28 - June 1, 2017) | 2017

Toward Single-Color Carbon Nanotube Fluorescence Microscopy

Rachel E Langenbacher; Januka Budhathoki-Uprety; Daniel A. Heller; Prakrit V. Jena; Daniel Roxbury; Ming Zheng; Jackson Dean Harvey

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Prakrit V. Jena

Memorial Sloan Kettering Cancer Center

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Ryan M. Williams

Memorial Sloan Kettering Cancer Center

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Daniel Roxbury

Memorial Sloan Kettering Cancer Center

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Januka Budhathoki-Uprety

Memorial Sloan Kettering Cancer Center

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Janki Shah

Memorial Sloan Kettering Cancer Center

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Hanan A. Baker

Memorial Sloan Kettering Cancer Center

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