Publications by authors named "Jordan Lo"

Background: Patients with sepsis-induced AKI can be classified into two distinct sub-phenotypes (AKI-SP1, AKI-SP2) that differ in clinical outcomes and response to treatment. The biologic mechanisms underlying these sub-phenotypes remains unknown. Our objective was to understand the underlying biology that differentiates AKI sub-phenotypes and associations with kidney outcomes.

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Purpose: Previous work has identified two AKI sub-phenotypes (SP1 and SP2) characterized by differences in inflammation and endothelial dysfunction. Here we identify these sub-phenotypes using biospecimens collected in the emergency department and test for differential response to restrictive versus liberal fluid strategy in sepsis-induced hypotension in the CLOVERS trial.

Methods: We applied a previously validated 3-biomarker model using plasma angiopietin-1 and 2, and soluble tumor necrosis factor receptor-1 to classify sub-phenotypes in patients with kidney dysfunction (AKI or end-stage kidney disease [ESKD]).

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The suppressor of T cell receptor signaling (Sts) proteins are negative regulators of immune signaling. Genetic inactivation of these proteins leads to significant resistance to infection. From a 590,000 compound high-throughput screen, we identified the 2-()-quinolinone derivative, rebamipide, as a putative inhibitor of Sts phosphatase activity.

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Background: Our objective was to discover novel urinary biomarkers of antibiotic-associated nephrotoxicity using an ex-vivo human microphysiological system (MPS) and to translate these findings to a prospectively enrolled cystic fibrosis (CF) population receiving aminoglycosides and/or polymyxin E (colistin) for a pulmonary exacerbation.

Methods: We populated the MPS with primary human kidney proximal tubule epithelial cells (PTECs) from three donors and modeled nephrotoxin injury through exposure to 50 µg/mL polymyxin E for 72 h. We analyzed gene transcriptional responses by RNAseq and tested MPS effluents.

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Article Synopsis
  • - Non-small cell lung cancer (NSCLC) is the most prevalent form of lung cancer, representing about 84% of cases, and it has a low 5-year survival rate of under 25%, highlighting the need for improved treatment strategies.
  • - Research focuses on the tumor microenvironment and the development of advanced 3D primary cell tumor models that better represent actual tumors, leveraging new technologies that make 3D cell culture more efficient and cost-effective.
  • - The study utilizes a Natural Products Library to screen potential therapies in a high-throughput 3D format against various NSCLC cell lines, aiming to identify compounds that are effective against both wild type and mutant cancer cells.
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"A significant problem facing patients throughout the country is the rising cost of medical care. In addition to the physician's fees and laboratory charges of a routine office visit, patients may face an even greater bill from the pharmacy. There are several ways that physicians can help.

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