The authors examined the efficacy of 2-chlorodeoxyadenosine (2-CDA) in the treatment of refractory inhibitors to factor VIII in persons without hemophilia. The drug was administered to 6 patients at a dose of 0.1 mg/kg as a 24-hour continuous infusion for a total of 7 days each cycle. An average of 3 immunosuppressive regimens per patient had been administered prior to enrollment in this study. The median inhibitor titer against human and porcine factor VIII before treatment with 2-CDA was 31 Bethesda units (BUs) and 9 BU, respectively. The median inhibitor titer against human and porcine factor VIII after treatment was 3.5 BU and 1.5 BU, respectively. The median time to reach nadir inhibitor titer in this study was 137 days, whereas the median time to reach a 50% increase in factor VIII was 117 days. No major toxicity was observed in any patient in this study. Patients with acquired inhibitors to factor VIII refractory to conventional immunosuppressive therapy may respond favorably to 2-CDA.

The spontaneous formation of inhibitors against clotting factors is a rare event. The most common inhibitors are those directed against factor VIII.1-4 This condition is also referred to as acquired hemophilia. The resulting bleeding episodes are usually more serious than those encountered in persons with hemophilia. A mortality rate of 22% secondary to uncontrolled hemorrhages was reported in one survey of patients with acquired inhibitors.3 The increased awareness of this condition and the availability of more products to manage this condition have improved the outcome of these patients in recent years.4-6Nevertheless, patients with bleeding secondary to spontaneous inhibitors to factor VIII should be approached with great caution because of the seriousness of these episodes.

In the present investigation, we report on the use of 2-chlorodeoxyadenosine (2-CDA) in the treatment of patients with acquired inhibitors to factor VIII. The inhibitor titer declined in all 6 patients, with virtually no serious toxicity. The study demonstrates that 2-CDA is an effective and safe immunosuppressant in patients with inhibitors to factor VIII that is refractory to conventional treatment.

Between 1997 and 2001, 6 patients with acquired inhibitors to factor VIII were enrolled in a prospective study. The criteria for enrollment included patients with a confirmed diagnosis of inhibitor against factor VIII measured by the Bethesda assay, prior treatment with conventional immunosuppressants, and age older than 18 years. Patients were considered candidates for the study if they had experienced bleeding or an increase in inhibitor titer while receiving immunosuppressive therapy. Patients positive for the human immunodeficiency virus were excluded. All patients gave written informed consent.

A complete blood count was obtained at baseline and repeated at the end of chemotherapy and at least monthly during the follow-up period. Liver function tests, blood urea nitrogen tests, and creatinine tests were performed in all patients prior to treatment and at frequent intervals thereafter.

The patients received 2-CDA at a dose of 0.1 mg/kg/24 h as a continuous infusion for a total of 7 days per cycle. The inhibitor titer against human and porcine factor VIII was measured at the end of treatment and once at least every 2 to 3 months for a year after treatment. A second cycle of treatment was administered if the inhibitor titer was not reduced by at least 25% of the baseline value by the eighth week after therapy. If no response was detected after the second cycle, further treatment with 2-CDA was discontinued. The end points of the study were increase in factor VIII level above 50% and the absence of further bleeding episodes during this period.

The median age of the 4 men and 2 women in this study was 67 years. Table 1 depicts the characteristics of the patients treated with 2-CDA. Data on serial inhibiter titers, response, and toxicity were available for all patients. The median time from the diagnosis of inhibitors to the start of treatment with 2-CDA was 14.3 months (range, 11.5-19.5 months). The number of 2-CDA treatments was 1 per patient, with the exception of a single patient who received 2 cycles. The median time from the last dose of concentrates used for acute bleeding episodes to the receipt of 2-CDA was 2.7 days (range, 2.5-3 days). The median inhibitor titer against human and porcine factor VIII prior to 2-CDA was 31 Bethesda Units (BUs) and 9 BU, respectively.

Table 1.

Characteristics of 6 patients with inhibitors against FVIII treated with 2-chlorodeoxyadenosine

PtAge/SexUnderlying conditionTiter
at treatment, BU/mL
BleedingTime to
50% increase in FVIII, d
Time to
50% decline in inhibitor, d
Time to nadir
inhibitor, d
Nadir inhibitor titer (BU/mL)Maximum FVIII, %
HumanPorcineHumanPorcine
72/M Chronic lymphocytic leukemia 26 Soft tissues 95 68 117 62 
63/M None 162 16 Soft tissues, hematuria 265 124 280 54 
67/F Scleroderma 24 Postoperative 105 79 145 82 
59/F Systemic lupus erythematosus 36 Skin, hemarthrosis 128 84 129 87  
78/M Colon cancer resected 2 years prior to inhibitor 18 10 Soft tissues, intra-abdominal 86 54 102 64 
68/M None 54 14 Soft tissues, epistaxis 94 87 218 76 
PtAge/SexUnderlying conditionTiter
at treatment, BU/mL
BleedingTime to
50% increase in FVIII, d
Time to
50% decline in inhibitor, d
Time to nadir
inhibitor, d
Nadir inhibitor titer (BU/mL)Maximum FVIII, %
HumanPorcineHumanPorcine
72/M Chronic lymphocytic leukemia 26 Soft tissues 95 68 117 62 
63/M None 162 16 Soft tissues, hematuria 265 124 280 54 
67/F Scleroderma 24 Postoperative 105 79 145 82 
59/F Systemic lupus erythematosus 36 Skin, hemarthrosis 128 84 129 87  
78/M Colon cancer resected 2 years prior to inhibitor 18 10 Soft tissues, intra-abdominal 86 54 102 64 
68/M None 54 14 Soft tissues, epistaxis 94 87 218 76 

Pt indicates patient; FVIII, factor VIII.

An average of 3 immunosuppressive regimens per patient was administered prior to enrollment in the current study. The median time from the diagnosis of inhibitor to the initiation of immunosuppression was 8.6 days (range, 6-34 days). These agents included prednisone alone at a dose of 1 to 2 mg/kg/d for a median of 58 days in all patients; 1 to 2 mg/kg/d prednisone in combination with 2 mg/kg/d cyclophosphamide for a median of 48 days in 5 patients; 0.5 to 2 mg/kg intravenous immunoglobulin in 4 patients; and 200 mg cyclosporin daily for a median of 74 days in 3 patients. The median time from the last day of immunosuppressive therapy to 2-CDA was 79 days (range, 66-94 days). Treatments aimed at controlling the acute bleeding episodes included porcine factor VIII in 3 patients, activated prothrombin complex concentrates (factor eight inhibitor bypassing activity [FEIBA]) in 2 patients, and activated recombinant factor VII in 1 patient. These concentrates were administrated for a median of 3 days prior to 2-CDA and for a median of 2 days thereafter.

The course of treatment in each individual in this study is depicted in Figure 1. The median time to reach a 50% increase in factor VIII level was 117 days. The median time to a 50% reduction in human inhibiter titer was 81.5 days. The median nadir inhibitor titer against human and porcine factor VIII was 3.5 BU and 1.5 BU, respectively. The median time to reach nadir inhibitor titer in this study was 137 days. The median maximum factor VIII level achieved was 70%.

Fig. 1.

The course of factor VIII inhibitor and factor VIII level in 6 patients with inhibitors against factor VIII.

Day 0 corresponds to the first day of treatment with 2-chlorodeoxyadenosine.

Fig. 1.

The course of factor VIII inhibitor and factor VIII level in 6 patients with inhibitors against factor VIII.

Day 0 corresponds to the first day of treatment with 2-chlorodeoxyadenosine.

Close modal

Overall, treatment was well tolerated by all patients. Mild neutropenia with an absolute neutrophil count of 655/mm3 was observed in patient no. 2 following the administration of a second cycle of 2-CDA. Atypical pneumonia was diagnosed in patient no. 1 approximately 5 weeks following treatment. This patient had a lymphocyte count of 370/mm3 at the time of diagnosis of pneumonia. The lymphopenia in this patient lasted approximately 9 weeks. The number of CD4 cells was not measured, and no organism was isolated as an offending agent in this case. No grade 4 toxicity or death from treatment was observed during the study.

Spontaneous inhibitors against factor VIII in persons without a history of bleeding tendency constitute the most common inhibitors against clotting factor. In general, management of patients with these inhibitors is based on a 2-fold principle: treatment of the acute hemorrhagic event and long-term control of the inhibitor.1-6 Concentrates used for the treatment of bleeding episodes include porcine factor VIII, activated prothrombin complex concentrates, high-dose factor VIII, and recombinant activated factor VII.1,4-6 Prednisone alone or in combination with cyclophosphamide is considered the standard immunosuppressive agent to be administered once the acute bleeding episode has been controlled. The reported response rate (disappearance of inhibitor) with the use of these agents is approximately 70%.5Patients with low inhibitor titer appear to achieve a better response when using immunosuppressants, but the cutoff level between low and high inhibitor titer is not well defined.5 Other agents used in the treatment of acquired inhibitors to factor VIII include cyclosporin, azathioprine, immunoadsorption, vincristine, 6-mercaptopurine, and intravenous immunoglobulin.7-9 

In the current investigation, 2-CDA was administered to 6 patients with inhibitors against factor VIII that failed to respond to other immunosuppressants. Although the exact mechanism of action of 2-CDA is not well characterized, its strong immunosuppressive properties are thought to be mediated through the Fas/Fas ligand pathway and subsequent activation of cellular apoptosis.10-12 Defects in this particular pathway appear to be important for the induction of some autoimmune disorders.11,12 Modulation of the Fas receptor and the Fas ligand by various pharmacologic agents may lead to suppression of autoimmune phenomena. The toxicity profile of 2-CDA includes neutropenic fever, atypical infections, and prolonged but reversible immunosuppression and myelosuppression.13Disorders in which 2-CDA has shown high efficacy include hairy cell leukemia, chronic lymphocytic leukemia, and angioimmunoblastic lymphadenopathy with dysproteinemia.14 All these disorders are thought to have a strong autoimmune basis.

All patients in this study responded with long-term control of the inhibitor and bleeding episodes. Decline in inhibitor titer was achieved regardless of the level of inhibitor at the onset of treatment or the primary therapy received by these patients. It is noteworthy that no hemorrhages were recorded after the administration of 2-CDA. The few patient series available in the literature on the long-term control of acquired inhibitors against factor VIII differ in the type of immunosuppression used, follow-up period, and, most importantly, definition of response. One may argue whether continuing immunosuppression is essential in eradicating the inhibitor in our patients. It has been suggested that spontaneous resolution of inhibitors against factor VIII may occur in some patients.15 However, the severity of bleeding in such patients and the lack of sufficient supportive literature are 2 important issues to consider before adopting a strategy of watch and wait. Immunosuppression has been recommended even in postpartum inhibitors, which are considered by many to be the most likely type of inhibitors to remit spontaneously.7 Remarkably, 5 patients in this series achieved sustained remission after only one course of treatment with 2-CDA. Equally important is that all patients were heavily pretreated with a variety of agents prior to the administration of the study drug.

In summary, 2-CDA appears to be an effective agent for inhibitors to factor VIII. It provides long-term immunosuppression with an acceptable toxicity profile. It is our view that this agent may be administered after failure of other standard treatments used to reduce and eradicate the inhibitor. Further studies with a larger number of patients and longer follow-up are needed before determining the best use of 2-CDA in patients with inhibitors against factor VIII.

Prepublished online as Blood First Edition Paper, September 5, 2002; DOI 10.1182/blood-2002-07-2139.

The publication costs of this article were defrayed in part by page charge payment. Therefore, and solely to indicate this fact, this article is hereby marked “advertisement” in accordance with 18 U.S.C. section 1734.

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Roberts HR, Sallah S. Immunology of inhibitors to clotting factors with emphasis on factor VIII inhibitors. Autoimmune Disorders of Blood. In: Silberstein LE, ed. Bethesda MD: American Association of Blood Banks; 1996;155-170.
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Author notes

Sabah Sallah, Associate Professor of Medicine and Pathology, Thrombosis and Hemostasis Program and Feist-Weiller Cancer Center, Louisiana State University Health Sciences Center, 1501 Kings Hwy, Shreveport, LA 71130; e-mail:asalla@lsuhsc.edu.

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