Phase 1 Trial of Orally Administered Pentosan Polysulphate (Pps) in Patients With Advanced Malignancies

Marshall, J.; Wellstein, Anton; Al‐Kawas, Firas H.; Andris, Robert T; Hawkins, MJ

doi:10.1097/00002371-199410000-00067

Cited by 18 publications

(25 citation statements)

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“…Polysaccharide pentosan polysulfate has been shown to prevent complement-mediated myocardial injury in the rabbit isolated perfused heart model (54). Unlike other glycosaminoglycans, it is orally bioavailable and has undergone phase I testing as an orally administered drug in patients with advanced cancer (55). Compound 7 (based on the structure of FUT-175 or nafamostat mesilate), a newly synthesized inhibitor of active center-directed trypsinlike serine proteases such as C1r and C1s, has been reported to exhibit greater potency and stability in vivo than FUT-175 as an inhibitor of both the classical and alternative complement activation pathways (56).…”

Section: Inhibitors Of Complement Activationmentioning

confidence: 99%

Chronic Progression of Tubulointerstitial Damage in Proteinuric Renal Disease Is Mediated by Complement Activation

Hsu¹,

Couser²

2003

Journal of the American Society of Nephrology

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Abstract. The mechanisms by which increased urinary protein concentrations lead to nephrotoxic injury are certain to be multifactorial and involve complex interactions between numerous pathways of cellular damage mediated by both cellular and humoral pathways. These may include a major role for the podocyte in glomerular diseases leading to chronic renal failure, the loss of microvascular endothelium, the albumin-induced upregulation of renal cytokines and growth factors that promote tubulointerstitial injury by inflammation and fibrogenesis, and the role of complement-mediated tubulointerstitial injury due to proteinuria. This review will focus on the last mechanism, and emphasize recent studies implicating a primary role for activation of complement in proteinuric urine as the principal mediator of tubulointerstitial damage and progressive renal disease in various experimental animal models of nephrosis. It will be our contention that intraluminal activation of the terminal complement cascade leading to the formation of the C5b-9 membrane attack complex is the principal mediator of chronic progressive interstitial damage and progressive renal failure irrespective of the type of primary glomerular injury. This paradigm has important implications for the potential therapeutic role of complement inhibitors that are currently being developed.

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Section: Inhibitors Of Complement Activationmentioning

confidence: 99%

Chronic Progression of Tubulointerstitial Damage in Proteinuric Renal Disease Is Mediated by Complement Activation

Hsu¹,

Couser²

2003

Journal of the American Society of Nephrology

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“…In addition, children affected with the hemolytic uremic syndrome show high levels of circulating FGF-2 (23,24) and are at high risk of intestinal bleeding. Thus these findings might have wider clinical implications for patients treated systemically with PPS and other heparinoids for angiogenic tumors, ulcers, and intestinal inflammatory-angiogenic disorders (5,16,30,34). In contrast, patients treated orally with PPS for cystitis are not likely to be at higher risk of bleeding, since FGF-2 is not accumulated in the bladder, and PSS given orally should not induce anticoagulant changes in the bladder.…”

Section: Discussionmentioning

confidence: 94%

“…Pentosan polysulfate (PPS), a semisynthetic sulfated heparinoid polysaccharide, can antagonize the binding of FGF-2 to its cell surface receptors and has been shown to modulate the angiogenic activity of FGF-2 in human and mouse tumors (16,22,30,34). However, its use as an antiangiogenic agent in humans is limited by its heparin-like anticoagulant activity, which leads to the development of bleeding disorders in several tissues, including the intestine (16,22).…”

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confidence: 99%

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A novel role of fibroblast growth factor-2 and pentosan polysulfate in the pathogenesis of intestinal bleeding in mice

Jerebtsova

Wong²,

Przygodzki³

et al. 2007

American Journal of Physiology-Heart and Circulatory Physiology

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“…Several have been developed, including synthetic, low-molecular weight molecules such as compastatin, a C3-binding peptide that inhibits C3 activation and generation of C5a and C5b-9 (19), and polysaccharide pentosan sulfate (PPS), which inhibits the alternative complement pathway and generation of C5b-9 (20). Because of their size, both of these may be effective orally, and PPS is now in clinical trial in cancer patients (21). But neither has been tested in kidney disease.…”

mentioning

confidence: 99%

Complement Inhibitors And Glomerulonephritis

Couser¹

2003

Journal of the American Society of Nephrology

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Phase 1 Trial of Orally Administered Pentosan Polysulphate (Pps) in Patients With Advanced Malignancies

Cited by 18 publications

References 0 publications

Chronic Progression of Tubulointerstitial Damage in Proteinuric Renal Disease Is Mediated by Complement Activation

Chronic Progression of Tubulointerstitial Damage in Proteinuric Renal Disease Is Mediated by Complement Activation

A novel role of fibroblast growth factor-2 and pentosan polysulfate in the pathogenesis of intestinal bleeding in mice

Complement Inhibitors And Glomerulonephritis

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