https://orcid.org/0000-0001-6044-623X
Key Points
TTP in Jehovah’s Witness patients has been managed successfully without PEX.
This experience, plus new TTP treatments, may make it possible for patients who are not Jehovah’s Witnesses to avoid PEX in the future.
Introduction
Plasma exchange (PEX) has been the principal and presumed essential treatment of acquired thrombotic thrombocytopenic purpura (TTP) since publication of the randomized clinical trial documenting its effectiveness in 1991.1 The requirement for PEX creates a crisis when a Jehovah’s Witness patient presents with TTP because Jehovah’s Witness doctrine is that refusal of transfusions of whole blood or any of its 4 primary components (red cells, white cells, platelets, and plasma) is mandatory.2 Therefore, PEX cannot be performed. However, the use of albumin and other purified protein fractions is not absolutely prohibited; for these products, personal choice is acceptable.2
We report the successful treatment of a Jehovah’s Witness patient with acquired TTP without PEX. We also systematically searched for previous published reports of TTP in Jehovah’s Witness patients.
Case description
A 46-year-old white woman felt increasing fatigue for 2 weeks and noticed jaundiced sclerae 1 week before her hospitalization. However, she continued to work until the day of admission. That morning, she awoke suddenly with weakness, clumsiness, and numbness of both arms and hands and both sides of her face. She also had expressive aphasia. These symptoms were intermittent: throughout that initial day, in the emergency department and after hospital admission, they would resolve, often within 20 minutes, and then recur. During the periods when these symptoms had resolved, she was alert, oriented, and comfortable. After the first hospital day, through day 4, her neurologic symptoms did not recur.
TTP was suspected in the emergency department. The diagnosis of TTP was subsequently supported by severe thrombocytopenia and anemia with features of microangiopathic hemolysis (total bilirubin, 5.1 mg/dL; direct bilirubin, 0.6 mg/dL; direct antiglobulin test, negative; haptoglobin, <30 mg/dL). ADAMTS13 activity was <5% (testing for a functional inhibitor was not performed). Her past history included Graves disease in 2010, which was treated with radioiodine ablation, and hypertension, diagnosed in 2016.
Treatment was begun on day 1 with methylprednisolone and folic acid (Table 1). Rituximab was given on day 3. Plasmapheresis with albumin replacement (not PEX with plasma replacement) was performed on days 4 and 5, but was then stopped because of hypofibrinogenemia (46 mg/dL). Erythropoietin was begun on day 4. IV immunoglobulin (IVIg) was given on days 5 and 8.
Clinical course and treatment of our Jehovah’s Witness patient
| Day . | Hgb, g/dL . | Plt, ×109/L . | Clinical course . | Treatments* . |
|---|---|---|---|---|
| 1 | 8.4 | 12 | Transient aphasia, bilateral arm and face numbness and weakness, hand clumsiness. | MP 375, folic acid |
| 2 | 7.8 | 16 | Neurologic symptoms resolved. | |
| 3 | 7.8 | 24 | Rituximab | |
| 4 | 7.5 | 10 | Apheresis, Epo | |
| 5 | 6.9 | 9 | Acute transient episode of feeling faint, aphasia, left arm weakness. | Apheresis, IVIg |
| 6 | 6.0 | 10 | Neurologic symptoms resolved; no further neurologic abnormalities. | |
| 7 | 5.7 | 15 | MP 1000, IVIg | |
| 8 | — | — | MP 1000, IV iron, rituximab | |
| 9 | 6.6 | 28 | MP 1000 | |
| 10 | — | — | Gradual improvement. Hallucinations and proximal muscle weakness attributed to corticosteroids. | Koate, prednisone 80 |
| 11 | 7.2 | 45 | ||
| 12 | 7.7 | 74 | Rituximab | |
| 14 | 9.1 | 96 | Prednisone 40 | |
| 16 | 9.3 | 109 | Discharged to rehabilitation for steroid-induced proximal muscle weakness. Regained strength with physical therapy. | |
| 19 | 10.0 | 115 | Rituximab | |
| 21 | 11.8 | 90 | ||
| 23 | 12.7 | 125 | ||
| 28 | 13.0 | 231 | Discharged to home. ADAMTS13, 99%. | |
| 60 | — | — | Return to work. |
| Day . | Hgb, g/dL . | Plt, ×109/L . | Clinical course . | Treatments* . |
|---|---|---|---|---|
| 1 | 8.4 | 12 | Transient aphasia, bilateral arm and face numbness and weakness, hand clumsiness. | MP 375, folic acid |
| 2 | 7.8 | 16 | Neurologic symptoms resolved. | |
| 3 | 7.8 | 24 | Rituximab | |
| 4 | 7.5 | 10 | Apheresis, Epo | |
| 5 | 6.9 | 9 | Acute transient episode of feeling faint, aphasia, left arm weakness. | Apheresis, IVIg |
| 6 | 6.0 | 10 | Neurologic symptoms resolved; no further neurologic abnormalities. | |
| 7 | 5.7 | 15 | MP 1000, IVIg | |
| 8 | — | — | MP 1000, IV iron, rituximab | |
| 9 | 6.6 | 28 | MP 1000 | |
| 10 | — | — | Gradual improvement. Hallucinations and proximal muscle weakness attributed to corticosteroids. | Koate, prednisone 80 |
| 11 | 7.2 | 45 | ||
| 12 | 7.7 | 74 | Rituximab | |
| 14 | 9.1 | 96 | Prednisone 40 | |
| 16 | 9.3 | 109 | Discharged to rehabilitation for steroid-induced proximal muscle weakness. Regained strength with physical therapy. | |
| 19 | 10.0 | 115 | Rituximab | |
| 21 | 11.8 | 90 | ||
| 23 | 12.7 | 125 | ||
| 28 | 13.0 | 231 | Discharged to home. ADAMTS13, 99%. | |
| 60 | — | — | Return to work. |
Days begin with hospital admission on day 1.
Epo, recombinant human erythropoietin; Hgb, hemoglobin concentration; MP, methylprednisolone (and prednisone); Plt, platelet count.
Doses, regimens: apheresis, plasmapheresis with albumin replacement; Epo, 10 000 U then 20 000 U, 3 times per week; folic acid, 1 mg per day; IVIg, 70 g (1 g/kg); IV iron, ferrous gluconate, 125 mg IV daily; Koate, 2000 U (30 U/kg), given once; MP, milligrams per day; rituximab, 375 mg/m2.
On day 5, following apheresis and while receiving IVIg, her neurologic symptoms suddenly recurred. She felt faint and had expressive aphasia with left arm weakness. Stroke was suspected but brain computed tomography scan was normal. Later that day, her neurologic examination returned to normal. Methylprednisolone dosage was increased and the second rituximab infusion was given. Koate (Koate-DVI, antihemophilic factor [human]; Kedrion Biopharma) was given to provide ADAMTS13.3,4 Koate contains factor VIII and von Willebrand factor; it is primarily used for treatment of hemophilia A and von Willebrand disease. After day 5, she progressively recovered with no further neurologic symptoms (except hallucinations attributed to corticosteroids, which were treated with risperidone). She was transferred to rehabilitation on day 16 because of corticosteroid myopathy. Recovery was documented by normal ADAMTS13 activity.
Methods
We searched 7 databases (MEDLINE via OVID, MEDLINE via PubMed, EMBASE, Cochrane Database of Systematic Reviews, Cumulative Index to Nursing and Allied Health Literature, Web of Science, and Current Contents) through August 2017 using the medical subject heading terms “thrombotic thrombocytopenic purpura” and “Jehovah’s Witness.” Bibliographies of the identified articles were searched for additional reports. Searches were limited to English language.
Results and discussion
Our systematic literature search identified 12 articles; 6 described management of TTP in Jehovah’s Witness patients. Two of these 6 articles were excluded because the diagnosis of TTP was not confirmed by measurement of ADAMTS13 activity or by occurrence of relapse. Among the 4 included articles, the diagnosis of TTP was supported by ADAMTS13 activity <5% in 35-7 and by the description of relapse in 18 (Table 2).
Clinical course of the 4 previously published Jehovah’s Witness patients with TTP
| Patient*/year/reference . | Age/sex . | Past medical history, presenting symptoms, laboratory data . | Treatment . | Outcome . |
|---|---|---|---|---|
| 1/2007/5 | 19/F | Previous mixed connective tissue disease treated with hydroxychloroquine and prednisone. Chest pain, headache, syncope. Hgb, 4.9; Plt <10; Cr, 1.0; LDH, 1131; ADAMTS13, <5%; Inh, <0.4 BU | MP, 1000 mg on days 1-3. Vincristine, day 3, 2 mg; days 6 and 9, 1 mg. | Plt, <10 on days 1-3; 125 on day 4; 280 on day 5 |
| 2/2015/6 | 41/F | Previous SLE, treated with hydroxychloroquine. Bruising, dyspnea, abdominal pain. Hgb, 6.1; Plt, 29; Cr, “normal”; LDH, 477; ADAMTS13, <5%; Inh, 1.4 BU | Dex, 40 mg days 1-4, IVIg, 1 g/kg days 1, 2, 5. Vincristine, 2 mg days 3, 8. Rituximab, 375 mg/m2 days 3, 8, 15. Apheresis with albumin replacement days 2, 3, 6, 7. Epo, 30 000 U days 6-11. | Plt, 9-29 until 50 on day 8; 200 on day 12. Nadir Hgb, 3.2 on day 8, 6.3 on day 16. At 6 mo: Hgb, 12.6; Plt, 225; ADAMTS13, 90% |
| 3/2015/8 | 58/F | First episode: Hgb, 5.4; Plt, 16; Cr, 1.2; LDH, 1605; Hpt, <10; ADAMTS13, NR | First episode: rituximab, cyclophosphamide | Both episodes: “Significant improvement within few days” (remission is assumed) |
| Second episode: Transient aphasia, blurred vision. Hgb, 9.1; Plt, 30; Cr, 1.1; LDH, 756; ADAMTS13, NR | Second episode: rituximab, IVIg | |||
| 4/2017/7 | 22/F | Purpura. Hgb, 10.1; Plt, 12; LDH, increased; Hpt, decreased; ADAMTS13, <5%; Inh, >8 BU | “High-dose steroid,” Epo, folic acid beginning day 1. Apheresis, albumin replacement: days 2, 5; cryoprecipitate replacement, days 7, 9, 10, 12, 13. Rituximab, days 3, 10, 17. Vincristine, days 6, 16. Sanguinate, days 10-13. | Discharge on day 19: Hgb, 8.8; Plt, 221 |
| Patient*/year/reference . | Age/sex . | Past medical history, presenting symptoms, laboratory data . | Treatment . | Outcome . |
|---|---|---|---|---|
| 1/2007/5 | 19/F | Previous mixed connective tissue disease treated with hydroxychloroquine and prednisone. Chest pain, headache, syncope. Hgb, 4.9; Plt <10; Cr, 1.0; LDH, 1131; ADAMTS13, <5%; Inh, <0.4 BU | MP, 1000 mg on days 1-3. Vincristine, day 3, 2 mg; days 6 and 9, 1 mg. | Plt, <10 on days 1-3; 125 on day 4; 280 on day 5 |
| 2/2015/6 | 41/F | Previous SLE, treated with hydroxychloroquine. Bruising, dyspnea, abdominal pain. Hgb, 6.1; Plt, 29; Cr, “normal”; LDH, 477; ADAMTS13, <5%; Inh, 1.4 BU | Dex, 40 mg days 1-4, IVIg, 1 g/kg days 1, 2, 5. Vincristine, 2 mg days 3, 8. Rituximab, 375 mg/m2 days 3, 8, 15. Apheresis with albumin replacement days 2, 3, 6, 7. Epo, 30 000 U days 6-11. | Plt, 9-29 until 50 on day 8; 200 on day 12. Nadir Hgb, 3.2 on day 8, 6.3 on day 16. At 6 mo: Hgb, 12.6; Plt, 225; ADAMTS13, 90% |
| 3/2015/8 | 58/F | First episode: Hgb, 5.4; Plt, 16; Cr, 1.2; LDH, 1605; Hpt, <10; ADAMTS13, NR | First episode: rituximab, cyclophosphamide | Both episodes: “Significant improvement within few days” (remission is assumed) |
| Second episode: Transient aphasia, blurred vision. Hgb, 9.1; Plt, 30; Cr, 1.1; LDH, 756; ADAMTS13, NR | Second episode: rituximab, IVIg | |||
| 4/2017/7 | 22/F | Purpura. Hgb, 10.1; Plt, 12; LDH, increased; Hpt, decreased; ADAMTS13, <5%; Inh, >8 BU | “High-dose steroid,” Epo, folic acid beginning day 1. Apheresis, albumin replacement: days 2, 5; cryoprecipitate replacement, days 7, 9, 10, 12, 13. Rituximab, days 3, 10, 17. Vincristine, days 6, 16. Sanguinate, days 10-13. | Discharge on day 19: Hgb, 8.8; Plt, 221 |
Doses, regimens: Cr, mg/dL; Hgb, g/dL; Hpt, mg/dL; LDH, U/L; Plt, × 109/L.
BU, Bethesda unit; Cr, serum creatinine; Dex, dexamethasone; Hpt, haptoglobin; Inh, functional ADAMTS13 inhibitor; LDH, lactate dehydrogenase; MP, methylprednisolone; NR, not reported; SLE, systemic lupus erythematosus.
Patients 1, 2, and 4: platelet count values were extrapolated from the published figures. Patient 3 was described in an abstract with minimal detail. No presenting symptoms were described for her first episode; ADAMTS13 activity was not reported. No regimens or days of administration were reported for the treatments; no outcomes were described for either episode. Patient 4: Sanguinate (pegylated bovine carboxyhemoglobin) is a product in development for patients with severe anemia (NCT02754999). For patients 3 and 4, drug doses were not reported.
There was no consistent plan of treatment of the 5 episodes of TTP in the 4 previously reported patients, as well as in our patient. This inconsistency clearly reflects the urgency for treatment and the uncertainty regarding what treatments to use. Rituximab was used in 5 of the 6 episodes, vincristine in 3, and cyclophosphamide in 1. High-dose corticosteroids were used in 4 episodes; corticosteroids were not mentioned in 2 episodes.8 IVIg and apheresis with albumin replacement were used in 3 patients. Koate, to provide ADAMTS13, was only used in our patient. All 5 patients recovered without PEX; 1 patient recovered twice, from both of her episodes.8
There are ∼8 300 000 Jehovah’s Witness adherents worldwide.9 Because the incidence of TTP is ∼2 patients per million in the population per year,10 we must assume that there have been many other unpublished occurrences of TTP among Jehovah’s Witnesses. Death from TTP in Jehovah’s Witness patients has not been reported, only recovery. However biased these case reports may be, only reporting successful treatment, the experience with these 5 Jehovah’s Witness patients suggests that TTP can be effectively treated without PEX.
From our experience, how would we treat future Jehovah’s Witness patients, or our patient if she relapses? The most effective treatment may be rituximab, 375 mg/m2 twice weekly for 2 weeks, and methylprednisolone, 1000 mg per day for 3 days, followed by more conventional corticosteroid doses, similar to the regimen used in a United Kingdom study.11 Koate, to provide ADAMTS13,3,4 would be repeated while thrombocytopenia persists. Erythropoietin and folic acid would be given to provide support for erythropoiesis. Additional immunosuppressive agents and apheresis with albumin replacement may not be necessary. It may be prudent to avoid IVIg because its efficacy is unknown and adverse reactions to IVIg may mimic the thrombotic,12 neurologic,13 and renal14 manifestations of TTP.
This proposed regimen will change with the anticipated approval of new treatments for TTP. Caplacizumab, a nanobody that blocks von Willebrand factor interaction with platelets, can promptly prevent microvascular thrombosis.15 Recombinant ADAMTS13 will provide ADAMTS13 activity to decrease the concentration of ultra-large von Willebrand factor multimers.16 These new treatments may provide a major benefit for Jehovah’s Witness patients.
These observations on Jehovah’s Witness patients suggest the possibility that PEX may not be an essential treatment of TTP. If PEX could be avoided, management of patients with TTP could be simpler and safer. PEX requires mobilization of specialized personnel and instruments that may not be available in many hospitals or at all times. PEX requires insertion of a central venous dialysis catheter, with its risk for hemorrhage and infection. We have systematically documented adverse reactions to PEX among Oklahoma TTP Registry patients during the past 20 years.17,18 Three of our 78 TTP patients (4%) have died of complications of PEX: 2 from sepsis and 1 from hemorrhage caused by central venous catheter insertion.18,19 Twelve additional patients (18%) have had sepsis with documented bacteremia, related to their central venous catheter. Three patients have had venous thrombosis at the central venous catheter site requiring systemic anticoagulation. One patient had an anaphylactic reaction to plasma with cardiac arrest; she had a complete recovery.18
We acknowledge that PEX is the current essential treatment of TTP. However, the successful management of Jehovah’s Witness patients without PEX may provide insight for effective and safer future management of all patients with TTP.
Acknowledgments
The authors thank Jessica Reese for assistance with the systematic literature review. The authors thank both their patient and T. J. Bullock, chairman of the Chicago Hospital Liaison Committee for Jehovah’s Witnesses, for their discussions concerning religious and ethical positions on medical therapy.
Authorship
Contribution: J.N.G. consulted with J.S. and S.A.S. throughout the patient’s hospitalization, helped perform the systematic literature review, and wrote the manuscript; and J.S. and S.A.S. provided the primary care for the patient, including continuing follow-up, provided the patient’s medical records for J.N.G., and reviewed the manuscript for accuracy and appropriate interpretation.
Conflict-of-interest disclosure: For J.N.G., Ablynx, developer of caplacizumab, provided partial salary support for a research assistant in 2016 for organization of Oklahoma TTP Registry data that were published in a previous Blood Advances article. The remaining authors declare no competing financial interests.
Correspondence: James N. George, Department of Biostatistics and Epidemiology, College of Public Health, The University of Oklahoma Health Sciences Center, P.O. Box 26901, Oklahoma City, OK 73126-0901; e-mail: james-george@ouhsc.edu.
