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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT02551042
Other study ID # 13/0417
Secondary ID 2014-001101-40
Status Recruiting
Phase Phase 2
First received December 17, 2014
Last updated May 27, 2016
Start date September 2015
Est. completion date September 2018

Study information

Verified date May 2016
Source University College, London
Contact Christopher Denton, PhD
Phone 02073177544
Email c.denton@ucl.ac.uk
Is FDA regulated No
Health authority United Kingdom: Medicines and Healthcare Products Regulatory Agency
Study type Interventional

Clinical Trial Summary

Many patients with Scleroderma (Systemic sclerosis) experience damage to blood vessels, mainly to the small arteries. A common manifestation of this is Raynaud's phenomenon (fingers or toes turning white then blue in the cold) and digital ulcers (open sores on the fingertips). The purpose of this study is to see how effective the study drug Human Factor XIII Concentrate is in treating patients who have these and other common manifestation of Scleroderma. It will be given in addition to the accepted treatments used for this disease.


Description:

This is a phase II, double-blind, randomized, placebo-controlled study to investigate pharmacokinetics (PK), safety and efficacy of intravenous factor XIII treatment in patients with systemic sclerosis.

Scleroderma (Systemic sclerosis) is a multisystem rheumatic disease that is characterised by progressive vascular damage e.g Raynaud's phenomenon and digital ulcers and organ fibrosis e.g. skin thickening and pulmonary fibrosis.The disease is associated with significant morbidity and mortality and current therapeutic options are only partially effective, including Cyclophosphamide for skin or lung fibrosis and Bosentan which reduces but does not heal digital ulcers.

There is no cure available and there is therefore a high need for new therapeutic options.Administration of human Factor XIII (FXIII) concentrate in patients with scleroderma demonstrated promising results in the 1980s and 1990s . However these studies were not performed according to current Good Clinical Practice (GCP) guidelines and involved relatively small sample sizes.

This is a single site study, therefore all study participants will be seen at the Royal Free London National Health Service (NHS) Foundation Trust.Total study duration is 36 months and will involve 2 phases: an initial single dose, pharmacokinetic (PK) phase in 8 subjects over 6 weeks and a multiple dose, active treatment phase in 18 subjects over 24 weeks. During the treatment phase subjects will be randomized at 2:1 ratio to either FXIII or Placebo and will receive biweekly injection of either factor XIII Concentrate or placebo.


Recruitment information / eligibility

Status Recruiting
Enrollment 26
Est. completion date September 2018
Est. primary completion date September 2016
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Male and female adults.

- Subjects with a diagnosis of systemic sclerosis (scleroderma, SSc) according to the 2013 American College of Rheumatology European League Against Rheumatism (ACR EULAR) classification criteria. They will be classified according to LeRoy criteria as limited or diffuse subset.

- Females of childbearing potential must be willing to use a reliable form of medically acceptable contraception and have a negative pregnancy test.

- Subjects will have serological status for hepatitis A and B assessed at screening.

- Patients who have given their free and informed consent. -= 18 years.

Exclusion Criteria:

Participants must:

- Be willing to use an effective method of contraception (hormonal or barrier method of birth control; abstinence) from the time consent is signed until 6 weeks after treatment discontinuation (females of childbearing potential and males)

- Have a negative pregnancy test within 7 days prior to being registered for trial treatment (females of childbearing potential). NOTE: Subjects are considered not of child bearing potential if they are surgically sterile (i.e. they have undergone a hysterectomy, bilateral tubal ligation, or bilateral oophorectomy) or they are postmenopausal.

- Not be breastfeeding (females).

Participants must not:

- Have allergies to excipients of the investigational medicinal product (IMP) and placebo

- Have uncontrolled systemic hypertension as evidenced by sitting systolic blood pressure = 160 mmHg or sitting diastolic blood pressure = 100 mmHg.

- Have portal hypertension or chronic liver disease defined as mild to severe hepatic impairment (Child-Pugh Class A-C). Subjects positive for Hepatitis C with evidence of active viral replication on sensitive polymerase chain reaction (PCR) testing are also excluded.

- Have hepatic dysfunction, defined as aspartate aminotransferase (AST) and/or alanine aminotransferase (ALT) = 3 times the upper limit of the normal range (× ULN) at the Screening Visit.

- Have chronic renal insufficiency as defined by a serum creatinine = 2.5 mg/dL (= 221 micromol/L) or requires dialysis.

- Have a haemoglobin concentration = 10 g/dL (= 100 g/L) at the Screening Visit.

- Have a history of left-sided heart disease and/or clinically significant cardiac disease, including but not limited to any of the following: aortic or mitral valve disease (stenosis or regurgitation) defined as more than minimum aortic insufficiency and more than moderate mitral regurgitation (stenosis or regurgitation= grade 1); pericardial constriction; restrictive or congestive cardiomyopathy; left ventricular ejection fraction = 40 % by multiple gated acquisition scan (MUGA), angiography, or echocardiography; left ventricular shortening fraction = 22 % by echocardiography; or symptomatic coronary disease with demonstrable ischemia.

- Have a history of malignancies within 5 years of Screening Visit with the exception of localized skin or cervical carcinomas.

- Have psychiatric, addictive, or other disorder that compromises the ability to give informed consent for participating in this study. This includes subjects with a recent history of abusing alcohol or illicit drugs.

- Be receiving ongoing treatment with hyperbaric oxygen

- Have pulmonary artery hypertension (PAH)

- Have received IV Iloprost within the last 2 months

- Have been treated with sympathectomy or toxin botulinum A within the last 3 months

- Have had thrombosis, stroke, pulmonary embolism or myocardial infarction in the last 6 months

- Have a diagnosis of diabetes mellitus requiring dietary restriction of carbohydrate.

- Be on a low sodium diet on medical advice.

- Be participating in another clinical trial involving an investigational medicinal product.

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment


Intervention

Drug:
Fibrogammin®P, coagulation factor XIII concentrate (Human)
IV infusion
0.9% sodium chloride
IV infusion

Locations

Country Name City State
United Kingdom Royal Free London NHS Foundation Trust London

Sponsors (2)

Lead Sponsor Collaborator
University College, London CSL Behring

Country where clinical trial is conducted

United Kingdom, 

References & Publications (33)

Avouac J, Clemessy M, Distler JH, Gasc JM, Ruiz B, Vacher-Lavenu MC, Wipff J, Kahan A, Boileau C, Corvol P, Allanore Y. Enhanced expression of ephrins and thrombospondins in the dermis of patients with early diffuse systemic sclerosis: potential contribution to perturbed angiogenesis and fibrosis. Rheumatology (Oxford). 2011 Aug;50(8):1494-504. doi: 10.1093/rheumatology/keq448. Epub 2011 Mar 30. — View Citation

Crawford SE, Stellmach V, Murphy-Ullrich JE, Ribeiro SM, Lawler J, Hynes RO, Boivin GP, Bouck N. Thrombospondin-1 is a major activator of TGF-beta1 in vivo. Cell. 1998 Jun 26;93(7):1159-70. — View Citation

Dallabrida SM, Falls LA, Farrell DH. Factor XIIIa supports microvascular endothelial cell adhesion and inhibits capillary tube formation in fibrin. Blood. 2000 Apr 15;95(8):2586-92. — View Citation

Dardik R, Leor J, Skutelsky E, Castel D, Holbova R, Schiby G, Shaish A, Dickneite G, Loscalzo J, Inbal A. Evaluation of the pro-angiogenic effect of factor XIII in heterotopic mouse heart allografts and FXIII-deficient mice. Thromb Haemost. 2006 Mar;95(3):546-50. — View Citation

Dardik R, Loscalzo J, Eskaraev R, Inbal A. Molecular mechanisms underlying the proangiogenic effect of factor XIII. Arterioscler Thromb Vasc Biol. 2005 Mar;25(3):526-32. Epub 2004 Dec 23. — View Citation

Dardik R, Loscalzo J, Inbal A. Factor XIII (FXIII) and angiogenesis. J Thromb Haemost. 2006 Jan;4(1):19-25. Epub 2005 Aug 26. — View Citation

Dardik R, Shenkman B, Tamarin I, Eskaraev R, Harsfalvi J, Varon D, Inbal A. Factor XIII mediates adhesion of platelets to endothelial cells through alpha(v)beta(3) and glycoprotein IIb/IIIa integrins. Thromb Res. 2002 Feb 15;105(4):317-23. — View Citation

Dardik R, Solomon A, Loscalzo J, Eskaraev R, Bialik A, Goldberg I, Schiby G, Inbal A. Novel proangiogenic effect of factor XIII associated with suppression of thrombospondin 1 expression. Arterioscler Thromb Vasc Biol. 2003 Aug 1;23(8):1472-7. Epub 2003 Jun 12. — View Citation

Delbarre F, Godeau P, Thivolet J. Factor XIII treatment for scleroderma. Lancet. 1981 Jul 25;2(8239):204. — View Citation

Denton CP, Zheng B, Evans LA, Shi-wen X, Ong VH, Fisher I, Lazaridis K, Abraham DJ, Black CM, de Crombrugghe B. Fibroblast-specific expression of a kinase-deficient type II transforming growth factor beta (TGFbeta) receptor leads to paradoxical activation of TGFbeta signaling pathways with fibrosis in transgenic mice. J Biol Chem. 2003 Jul 4;278(27):25109-19. Epub 2003 Apr 21. — View Citation

Euller-Ziegler L, Corolleur YR, Marcou J, Commandre F, Grisot C, Ziegler G. [Long-term treatment of systemic scleroderma with coagulation factor XIII. Developmental monitoring, especially of respiratory function]. Rev Rhum Mal Osteoartic. 1984 Oct;51(9):503-5. French. — View Citation

Farina G, Lafyatis D, Lemaire R, Lafyatis R. A four-gene biomarker predicts skin disease in patients with diffuse cutaneous systemic sclerosis. Arthritis Rheum. 2010 Feb;62(2):580-8. doi: 10.1002/art.27220. — View Citation

Gabrielli A, Avvedimento EV, Krieg T. Scleroderma. N Engl J Med. 2009 May 7;360(19):1989-2003. doi: 10.1056/NEJMra0806188. Review. — View Citation

Guillevin L, Chouvet B, Mery C, De Gery A, Thivolet J, Godeau P, Delbarre F. Treatment of progressive systemic sclerosis using factor XIII. Pharmatherapeutica. 1985;4(2):76-80. — View Citation

Guillevin L, Chouvet B, Mery C, Thivolet J, Godeau P, Delbarre F. [Treatment of generalized scleroderma with factor XIII. Study of 25 cases]. Rev Med Interne. 1982;3(3):273-7. French. — View Citation

Guillevin L, Euller-Ziegler L, Chouvet B, De Gery A, Chassoux G, Lafay P, Ziegler G, Godeau P, Amor B, Thivolet J. [Treatment of systemic scleroderma with factor XIII in 86 patients, with long-term follow-up]. Presse Med. 1985 Dec 28;14(46):2327-9. French. — View Citation

Ivaskevicius V, Seitz R, Kohler HP, Schroeder V, Muszbek L, Ariens RA, Seifried E, Oldenburg J; Study Group. International registry on factor XIII deficiency: a basis formed mostly on European data. Thromb Haemost. 2007 Jun;97(6):914-21. — View Citation

Khanna D, Furst DE, Hays RD, Park GS, Wong WK, Seibold JR, Mayes MD, White B, Wigley FF, Weisman M, Barr W, Moreland L, Medsger TA Jr, Steen VD, Martin RW, Collier D, Weinstein A, Lally EV, Varga J, Weiner SR, Andrews B, Abeles M, Clements PJ. Minimally important difference in diffuse systemic sclerosis: results from the D-penicillamine study. Ann Rheum Dis. 2006 Oct;65(10):1325-9. Epub 2006 Mar 15. — View Citation

Kilian O, Fuhrmann R, Alt V, Noll T, Coskun S, Dingeldein E, Schnettler R, Franke RP. Plasma transglutaminase factor XIII induces microvessel ingrowth into biodegradable hydroxyapatite implants in rats. Biomaterials. 2005 May;26(14):1819-27. — View Citation

LeRoy EC, Black C, Fleischmajer R, Jablonska S, Krieg T, Medsger TA Jr, Rowell N, Wollheim F. Scleroderma (systemic sclerosis): classification, subsets and pathogenesis. J Rheumatol. 1988 Feb;15(2):202-5. — View Citation

Levy JH, Greenberg C. Biology of Factor XIII and clinical manifestations of Factor XIII deficiency. Transfusion. 2013 May;53(5):1120-31. doi: 10.1111/j.1537-2995.2012.03865.x. Epub 2012 Aug 28. Review. — View Citation

Macko RF, Gelber AC, Young BA, Lowitt MH, White B, Wigley FM, Goldblum SE. Increased circulating concentrations of the counteradhesive proteins SPARC and thrombospondin-1 in systemic sclerosis (scleroderma). Relationship to platelet and endothelial cell activation. J Rheumatol. 2002 Dec;29(12):2565-70. — View Citation

Maekawa Y, Nogita T, Yamada M. Favorable effects of plasma factor XIII on lower esophageal sphincter pressure of progressive systemic sclerosis. Arch Dermatol. 1987 Nov;123(11):1440-1. — View Citation

Mimura Y, Ihn H, Jinnin M, Asano Y, Yamane K, Tamaki K. Constitutive thrombospondin-1 overexpression contributes to autocrine transforming growth factor-beta signaling in cultured scleroderma fibroblasts. Am J Pathol. 2005 May;166(5):1451-63. — View Citation

Mirochnik Y, Kwiatek A, Volpert OV. Thrombospondin and apoptosis: molecular mechanisms and use for design of complementation treatments. Curr Drug Targets. 2008 Oct;9(10):851-62. Review. — View Citation

Nihtyanova SI, Brough GM, Black CM, Denton CP. Clinical burden of digital vasculopathy in limited and diffuse cutaneous systemic sclerosis. Ann Rheum Dis. 2008 Jan;67(1):120-3. Epub 2007 Jul 27. — View Citation

Nör JE, Mitra RS, Sutorik MM, Mooney DJ, Castle VP, Polverini PJ. Thrombospondin-1 induces endothelial cell apoptosis and inhibits angiogenesis by activating the caspase death pathway. J Vasc Res. 2000 May-Jun;37(3):209-18. — View Citation

Nugent DJ. Prophylaxis in rare coagulation disorders -- factor XIII deficiency. Thromb Res. 2006;118 Suppl 1:S23-8. Epub 2006 Apr 17. Review. — View Citation

Paye M, Nusgens BV, Lapière CM. Factor XIII of blood coagulation modulates collagen biosynthesis by fibroblasts in vitro. Haemostasis. 1989;19(5):274-83. — View Citation

Quillinan NP, McIntosh D, Vernes J, Haq S, Denton CP. Treatment of diffuse systemic sclerosis with hyperimmune caprine serum (AIMSPRO): a phase II double-blind placebo-controlled trial. Ann Rheum Dis. 2014 Jan;73(1):56-61. doi: 10.1136/annrheumdis-2013-203674. Epub 2013 Sep 25. — View Citation

Streit M, Velasco P, Riccardi L, Spencer L, Brown LF, Janes L, Lange-Asschenfeldt B, Yano K, Hawighorst T, Iruela-Arispe L, Detmar M. Thrombospondin-1 suppresses wound healing and granulation tissue formation in the skin of transgenic mice. EMBO J. 2000 Jul 3;19(13):3272-82. — View Citation

Thivolet J, Perrot H, Meunier F, Bouchet B. [Therapeutic action of coagulation factor XIII in scleroderma. 20 cases]. Nouv Presse Med. 1975 Nov 15;4(39):2779-82. French. — View Citation

Yee VC, Pedersen LC, Le Trong I, Bishop PD, Stenkamp RE, Teller DC. Three-dimensional structure of a transglutaminase: human blood coagulation factor XIII. Proc Natl Acad Sci U S A. 1994 Jul 19;91(15):7296-300. — View Citation

* Note: There are 33 references in allClick here to view all references

Outcome

Type Measure Description Time frame Safety issue
Other Safety endpoints: Physical examination (including height, weight, BMI, digital ulcer characterization) Physical examination (including height, weight, BMI, digital ulcer characterization) 24 weeks Yes
Other Safety endpoints: Adverse events Adverse events 24 weeks Yes
Other Safety endpoints: Serious adverse events Serious adverse events 24 weeks Yes
Other Safety endpoints: ECG ECG 24 weeks Yes
Other Safety endpoints: Vital signs Vital signs 24 weeks Yes
Other Safety endpoints: Clinical laboratory parameters Clinical laboratory parameters 24 weeks Yes
Other Safety endpoints: Pregnancy Serum or urine pregnancy tests will be performed at each visit and will be reported positive or negative 24 weeks Yes
Other Safety endpoints -Adverse events of special interest: thromboembolic events Adverse events of special interest: thromboembolic events 24 weeks Yes
Primary Primary outcome assessed by skin involvement measured with modified Rodnan skin score 24 weeks No
Primary Primary outcome assessed by skin involvement measured with Raynaud condition score 24 weeks No
Secondary Pulmonary function measured by pulmonary function test Pulmonary function measured by pulmonary function test 24 weeks No
Secondary Hand function measured with Cochin hand function Hand function measured with Cochin hand function 24 weeks No
Secondary Quality of life measured with Short Form-36 (SF-36) quality of life questionnaire Quality of life measured with SF36 quality of life questionnaire 24 weeks No
Secondary Number of new digital ulcers (DU) Prevention of new DU: Number of new DU developed during a 24-week period of treatment 24 weeks No
Secondary Complete healing of digital ulcers (DU) Healing of DU: Complete healing of DUs present at baseline; each DU is considered as an entity 24 weeks No
Secondary Digital ulcer pain assessment DU Pain assessment at 4, 8, 12, 16, 24 weeks of treatment: Pain will be assessed by analogue scale for pain (Visual Analogue Scale, VAS) 24 weeks No
Secondary Digital ulcer pain assessment DU Pain assessment at 4, 8, 12, 16, 24 weeks of treatment: Pain will be assessed by Raynaud's severity (Raynaud's condition score) 24 weeks No
Secondary Digital ulcer worsening: hospitalisation required Number of overnight hospitalisations for digital ulcers 24 weeks No
Secondary Digital ulcer worsening: surgical intervention required Number of additional surgical treatments for digital ulcer in outpatient clinic 24 weeks No
Secondary Digital ulcer worsening: Digital ulcer infection Number of digital ulcers with infections 24 weeks No
Secondary Digital ulcer worsening: Gangrene Number of episodes of gangrene 24 weeks No
Secondary Digital ulcer worsening: Amputation Number of amputations 24 weeks No
Secondary Digital ulcer worsening: Need of local sympathectomy Number of local sympathectomies 24 weeks No
Secondary Digital ulcer worsening: Need of toxin Botulinum A Number of treatments with Botulinum toxin A 24 weeks No
Secondary Digital ulcer worsening: Need of oral or parenteral antibiotic Number of treatments needed with oral or parenteral antibiotic 24 weeks No
Secondary Digital ulcer worsening: Need of intravenous (IV) Iloprost : this is considered treatment failure Number of treatments needed with intravenous (IV) Iloprost : this is considered treatment failure 24 weeks No
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