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Dive into the research topics where Harold H. Handley is active.

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Featured researches published by Harold H. Handley.


Blood Purification | 2009

Reduction of Hepatitis C Virus Using Lectin Affinity Plasmapheresis in Dialysis Patients

Richard H. Tullis; R. Paul Duffin; Harold H. Handley; Puneet Sodhi; Jeevan Menon; James A. Joyce; Vijay Kher

Background/Aims: To test the safety and efficacy of the Aethlon Hemopurifier®, a lectin affinity cartridge, in clearing hepatitis C virus (HCV) from the blood of HCV-positive end-stage renal disease patients undergoing dialysis. Viral RNA was measured using real-time quantitative reverse transcriptase polymerase chain reaction. Results: HCV clearance from plasma or blood was measured using either direct capture on immobilized Galanthus nivalis agglutinin (GNA) or using miniature plasmapheresis cartridges containing immobilized GNA. HCV in plasma samples was rapidly cleared by direct affinity capture (t1/2 = approx. 20 min) and HCV in human blood was cleared using the Hemopurifier (t1/2 = 2–3 h). Institutional-review-board-sanctioned clinical safety studies were conducted at the Apollo and Fortis Hospitals in India. At Apollo, 4 patients were treated 3 times/week for 2 weeks. HCV captured on the Hemopurifier averaged 8.9 × 108 viral copies/cartridge (n = 5), representing approximately 30% of the initial viral body burden. At Fortis, 3 patients treated 3 times/week for 1 week completed the viral load studies. Two patients showed measurable viral load reduction, while the third showed both increases and decreases in viral load. After Hemopurifier treatment, average HCV viral load was reduced by 57%. Surprisingly, average viral load was also 82% lower 7 days after treatment. Control samples also showed a marked transient reduction in HCV viral load as previously reported. Conclusion: The Hemopurifier rapidly cleared HCV from blood treated in vitro. In patients, the combination of the Hemopurifier plus dialysis decreased HCV viral load by 57% in 1 week. Moreover, viral load reduction continued up to 7 days after treatment.


Blood Purification | 2002

Intravenous Catheter for Intracorporeal Plasma Filtration

Harold H. Handley; Rey Gorsuch; Nathan W. Levin; Claudio Ronco

Future advances in dialysis of end-stage renal disease patients may include improvements in therapeutic continuity and patient mobility. Continuous renal replacement therapies could lead to self-contained, mobile and potentially wearable dialysis units. We investigated an experimental, intravenous slow-continuous plasma separation system (IPSS) as a precursor to direct intravenous hemofiltration. An intracorporeal catheter employs asymmetric hollow fibers to separate blood cells from plasma in vivo. The fibers possess a sieving coefficient of 0.7 µm and remove 99.99% of all platelets. In vivo, catheters sustain an average plasma separation flow rate of 3 ml/min over 22 h, sufficient to remove 2 net liters of water from pigs through an extracorporeal hemofilter. Used catheter fibers are relatively free of protein deposition or clots in situ. In vitro studies suggest that human catheters may perform at 3–4 times the rate of porcine catheters. IPSS is proposed for acute fluid removal in CHF patients refractory to diuretics.


Blood Purification | 2003

Slow Continuous Intracorporeal Plasmapheresis for Acute Fluid Overload

Harold H. Handley; Rey Gorsuch; Nathan W. Levin; Claudio Ronco

Intermittent dialysis is still the predominant treatment for acute or chronic renal insufficiency in the USA despite increasing evidence that slower and longer fluid management therapies are more beneficial to the patient. We have investigated the use of slow continuous intracorporeal plasmapheresis (SCIP) as a more efficient and hemodynamically stable alternative means of treating acute fluid overload. In this paper we discuss preliminary observations on the safety of SCIP catheter insertion, fluid removal, extraction and pathology in Yorkshire pigs. SCIP catheters removed plasma for extracorporeal plasma water removal without significant gross or histopathological changes. Blood chemistry and cell counts remained stable during therapy. Toxicological studies indicated no pyrogenicity, hemolysis, cytotoxicity, acute systemic toxicity, delayed-type hypersensitivity, or blood recalcification coagulation inhibition. Intracutaneous extracts caused only mild irritation. SCIP therapy appears to be safe for use in the removal of plasma and plasma water from experimental animals.


Contributions To Nephrology | 2005

Slow Continuous Intravenous Plasmapheresis (SCIPTM): Clinical Applications and Hemostability of Extracorporeal Ultrafiltration

Harold H. Handley; Rey Gorsuch; Harold W. Peters; Thomas G. Cooper; Richard H. Bien; Nathan W. Levin; Claudio Ronco

An intravenous plasmapheresis catheter which excludes >99.4% of platelets from external ultrafiltration circuits is currently undergoing safety and efficacy trials for fluid removal from NYHA class II-IV congestive heart failure patients resistant to diuretic drug therapy. In animals, the SCIP catheter allowed a four fold increase in ultrafiltration efficiency without hemolysis, hemoinstability or external cartridge changes in 72 hours of treatment. Further, systemic anticoagulation was not required. These techniques might be envisioned for treatment of fluid overload in heart failure, surgery or trauma and may have applications in therapeutic apheresis, venous thrombosis, liver disease or autologous tissue engineering.


Archive | 2002

Plasmapheresis filter device and apparatus for therapeutic apheresis

Reynolds G. Gorsuch; Harold W. Peters; Harold H. Handley


Archive | 2009

Enhanced antiviral therapy methods and devices

Richard H. Tullis; Harold H. Handley; R. Paul Duffin; James A. Joyce


Archive | 2005

Method and apparatus for patient fluid management

Reynolds G. Gorsuch; Harold H. Handley; Harold W. Peters


Archive | 2004

Apparatus for therapeutic apheresis

Reynolds G. Gorsuch; Harold W. Peters; Harold H. Handley; Tommy Cooper


Archive | 2004

Structurally optimized hollow fiber membranes

Reynolds G. Gorsuch; Harold W. Peters; Harold H. Handley


Archive | 2001

Plasmapheresis filter device and catheter assembly

Reynolds G. Gorsuch; Harold W. Peters; Harold H. Handley

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Nathan W. Levin

Beth Israel Medical Center

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C. Ronco

Beth Israel Medical Center

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