Peter Groß scite author profile

Urinary exosomes containing apical membrane and intracellular fluid are normally secreted into the urine from all nephron segments, and may carry protein markers of renal dysfunction and structural injury. We studied methods for collection, storage, and preservation of urinary exosomal proteins. We collected urine from healthy volunteers, added protease inhibitors, and stored urine samples at 4, -20, and -80 degrees C for 1 week or 7 months. Samples were thawed with and without extensive vortexing, and three fractions were isolated: urinary sediment, supernatant, and exosome fraction. Protein concentration, electrophoresis patterns, and abundance of seven exosome-associated proteins were measured. Exosome-associated proteins were not detected in sediment or supernatant fractions. Protease inhibitors prevented degradation of exosome-associated proteins. Freezing at -20 degrees C caused a major loss in exosomes compared to fresh urine. In contrast, recovery after freezing at -80 degrees C was almost complete. Extensive vortexing after thawing markedly increased exosome recovery in urine frozen at -20 or -80 degrees C, even if frozen for 7 months. The recovery from first and second morning urine was similar. The abundance of cytosolic exosome-associated proteins did not decrease during long-term storage. We concluded: (1) protease inhibitors are essential for preservation; (2) storage at -80 degrees C with extensive vortexing after thawing maximizes the recovery of urinary exosomes; (3) the difference between first and second morning urine exosome-associated protein was small, suggesting minimal protein degradation in the urinary tract/bladder; (4) urinary exosomes remain intact during long-term storage. These urine collection, storage, and processing conditions may be useful for future biomarker discovery efforts.

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Guidelines for the Management of Adults with Community-acquired Pneumonia

Niederman¹,

Mandell²,

Anzueto³

et al. 2001

Am J Respir Crit Care Med

1,874

356

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Phase I Trial of Intravenous Administration of PV701, an Oncolytic Virus, in Patients With Advanced Solid Cancers

Pecora

Rizvi

Cohen

et al. 2002

JCO

342

330

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Peter Groß

Tolvaptan, a Selective Oral Vasopressin V₂-Receptor Antagonist, for Hyponatremia

Collection, storage, preservation, and normalization of human urinary exosomes for biomarker discovery

Guidelines for the Management of Adults with Community-acquired Pneumonia

Phase I Trial of Intravenous Administration of PV701, an Oncolytic Virus, in Patients With Advanced Solid Cancers

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Peter Groß

Tolvaptan, a Selective Oral Vasopressin V2-Receptor Antagonist, for Hyponatremia

Collection, storage, preservation, and normalization of human urinary exosomes for biomarker discovery

Guidelines for the Management of Adults with Community-acquired Pneumonia

Phase I Trial of Intravenous Administration of PV701, an Oncolytic Virus, in Patients With Advanced Solid Cancers

Contact Info

Product

Resources

About

Tolvaptan, a Selective Oral Vasopressin V₂-Receptor Antagonist, for Hyponatremia