Key Points
Early introduction of cyclosporine did not improve HLH outcome in patients treated with the HLH-94 etoposide-dexamethasone backbone (P = .06).
HLH-2004 may be improved by risk-group stratification, less therapy reduction weeks 7 to 8 for verified FHL patients, and earlier HSCT.
Abstract
Hemophagocytic lymphohistiocytosis (HLH) is a life-threatening hyperinflammatory syndrome comprising familial/genetic HLH (FHL) and secondary HLH. In the HLH-94 study, with an estimated 5-year probability of survival (pSu) of 54% (95% confidence interval, 48%-60%), systemic therapy included etoposide, dexamethasone, and, from week 9, cyclosporine A (CSA). Hematopoietic stem cell transplantation (HSCT) was indicated in patients with familial/genetic, relapsing, or severe/persistent disease. In HLH-2004, CSA was instead administered upfront, aiming to reduce pre-HSCT mortality and morbidity. From 2004 to 2011, 369 children aged <18 years fulfilled HLH-2004 inclusion criteria (5 of 8 diagnostic criteria, affected siblings, and/or molecular diagnosis in FHL-causative genes). At median follow-up of 5.2 years, 230 of 369 patients (62%) were alive (5-year pSu, 61%; 56%-67%). Five-year pSu in children with (n = 168) and without (n = 201) family history/genetically verified FHL was 59% (52%-67%) and 64% (57%-71%), respectively (familial occurrence [n = 47], 58% [45%-75%]). Comparing with historical data (HLH-94), using HLH-94 inclusion criteria, pre-HSCT mortality was nonsignificantly reduced from 27% to 19% (P = .064 adjusted for age and sex). Time from start of therapy to HSCT was shorter compared with HLH-94 (P = .020 adjusted for age and sex) and reported neurological alterations at HSCT were 22% in HLH-94 and 17% in HLH-2004 (using HLH-94 inclusion criteria). Five-year pSu post-HSCT overall was 66% (verified FHL, 70% [63%-78%]). Additional analyses provided specific suggestions on potential pre-HSCT treatment improvements. HLH-2004 confirms that a majority of patients may be rescued by the etoposide/dexamethasone combination but intensification with CSA upfront, adding corticosteroids to intrathecal therapy, and reduced time to HSCT did not improve outcome significantly.
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Editor Nancy Berliner received grants for clinical research from Novartis. CME questions author Laurie Barclay, freelance writer and reviewer, Medscape, LLC, owns stock, stock options, or bonds from Alnylam, Biogen, and Pfizer Inc. Authors Maurizio Aricó and Jan-Inge Henter served as unpaid consultants for Novimmune. The remaining authors declare no competing financial interests.
Upon completion of this activity, participants will be able to:
Assess survival in patients with hemophagocytic lymphohistiocytosis (HLH) enrolled in the HLH-2004 therapeutic trial.
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Determine the clinical implications of long-term findings from the HLH-2004 therapeutic trial.
Release date: December 21, 2017; Expiration date: December 21, 2018
Introduction
Hemophagocytic lymphohistiocytosis (HLH) is a devastating disturbance of the immune system leading to an uncontrolled accumulation of macrophages and lymphocytes, and hyperinflammation. Without adequate therapy it is often fatal.1 Traditionally, HLH is divided into primary (inherited) and secondary (acquired) forms.2 Both can be diagnosed at any age.
The most common form of primary HLH is familial (familial/genetic HLH [FHL]). FHL is autosomal recessive, and mutations in 4 genes (PRF1, UNC13D, STX11, and STXBP2) are today known to cause disease, all affecting the perforin pathway of lymphocyte cytotoxicity.3-6 Primary HLH also includes X-linked lymphoproliferative disease (XLP), Griscelli syndrome type 2 (GS2), Chediak-Higashi syndrome (CHS), and Hermansky-Pudlak syndrome (HPS). Secondary HLH (sHLH), more common in adults, is often associated with underlying conditions including severe infections, malignancies, or inflammatory disorders.2,7-9 Both primary HLH and sHLH are often triggered by infections.10
Clinical manifestations of HLH include prolonged fever, splenomegaly, cytopenias, hypertriglyceridemia, hypofibrinogenemia, and hyperferritinemia. Hemophagocytosis is not required for diagnosis.11 The central nervous system (CNS) is commonly affected at onset, often leading to neurological late effects.1,12-16 It can be difficult to distinguish between primary HLH and sHLH at onset, and both often require chemotherapy and/or immunotherapy. For primary cases, hematopoietic stem cell transplantation (HSCT) is required for cure,17-19 and may also be necessary for some forms of sHLH such as chronic active Epstein-Barr virus (EBV) infection.20,21
Three decades ago, long-term survival in HLH was <5%.1 Fortunately, thanks to collaborations worldwide and new treatment protocols including HSCT, many patients are now long-term survivors.12,22-26 In 1989, the Histiocyte Society established an HLH registry to which 122 patients were reported with a 5-year survival of 21%.27 In 1994, the Histiocyte Society launched the first international therapeutic study on HLH, HLH-94 (Figure 1A),12 with >200 eligible patients recruited worldwide. It resulted in a remarkably improved outcome with a 5-year probability of survival (pSu) of 54% ± 6%.15,24,26,28 Moreover, XLP, GS2, and CHS also responded well.29 However, early mortality and late neurological effects remained problematic: 29% died before HSCT and 19% displayed late neurological sequelae.15,24,26 A subsequent study, HLH-2004, was therefore initiated (Figure 1B). Here, we present a summary of HLH-2004 with focus on survival, mortality, toxicity, and comparisons with the historical control HLH-94.
Treatment protocol, patients, and methods
The HLH-2004 treatment protocol
HLH-2004 was based on HLH-94, with 8 weeks of initial treatment followed by a continuation phase, both including etoposide and dexamethasone (Figure 1). The first and main aim was “to provide and evaluate a revised initial and continuation therapy, with the goal to initiate and maintain an acceptable condition in order to perform a curative SCT, for patients with familial, relapsing, or severe and persistent HLH.”11 As compared with HLH-94, 3 treatment changes were made. (1) Due to high mortality weeks 1 to 8, treatment was intensified by administrating cyclosporine A (CSA) upfront, aimed at increasing immunosuppression without inducing additional myelotoxicity. Notably, CSA had been reported to inhibit production of interferon-γ (IFN-γ),30 and to be beneficial in initial HLH treatment.31 (2) To reduce time to HSCT, it was recommended that HSCT be performed as soon as an acceptable donor was available. (3) Given their beneficial systemic effect, corticosteroids were added to the intrathecal (IT) methotrexate (MTX) treatment recommended for a subset of patients. For nonverified FHL patients with complete disease resolution after 8 weeks, it was recommended that treatment was stopped.
The choice of HSCT donor, timing, conditioning regimen, and graft-versus-host disease (GVHD) prophylaxis were determined by the treating physician. A suggested conditioning regimen was, however, provided, including busulfan, cyclophosphamide, and etoposide, with CSA and methotrexate (or mycophenolate) as GVHD prophylaxis. When using an unrelated donor, antithymocyte globulin (ATG) was also recommended. When the study was initiated in 2004, limited data were available on reduced-intensity conditioning (RIC), hence no firm suggestions on RIC were provided.32
Study-specific clinical report forms were completed by the treating hospitals at start of treatment and after 2 weeks, 4 weeks, 2 months, 6 months, and thereafter annually. For transplanted patients, data were reported at transplantation, 100 days post-HSCT, and then annually. Serious adverse events (SAEs) and mortality reports were sent to the principal investigator, and subsequently to the external data safety monitoring board. The study started 1 January 2004, and closed for enrollment on 31 December 2011. Cutoff for data entry was 31 March 2016.
The HLH-2004 study was approved by the Histiocyte Society, and the Karolinska Institute Ethics Committee, and registered at clinicaltrials.gov (identifier, NCT00426101).
Patients
In HLH-94, 5 of 5 criteria (fever, splenomegaly, bicytopenia [hemoglobin (Hb), <90 g/L; platelets, <100 × 109/L; absolute neutrophil count (ANC), <1.0 × 109/L], hypertriglyceridemia [fasting triglycerides, ≥2.0 mmol/L], and/or hypofibrinogenemia [fibrinogen, ≤1.5 g/L], and hemophagocytosis), and/or an affected sibling (ie, “familial patients”) were required.12 In HLH-2004, 3 new diagnostic criteria were implemented: ferritin ≥ 500 µg/L, low/absent (<10 lytic units) natural killer (NK)-cell activity, and soluble CD25 (soluble interleukin-2 receptor [sIL-2r]) (≥2400 U/mL).11 HLH-2004 enrollment required: 5 of 8 diagnostic criteria, an affected sibling, and/or a molecular diagnosis in FHL-causative genes (PRF1, UNC13D, STX11, STXBP2). Inclusion age was increased from <16 to <18 years.11,12 Inclusion criteria were: no prior cytotoxic or CSA treatment, no other underlying disease, an intention to treat according to HLH-2004, and reported follow-up. Modifications of dosages were allowed, as long as all medications were administered. Supportive therapy or anti-infectious agents, including rituximab for EBV infection (n = 14), was accepted.
Altogether, 369 patients (all with active HLH) from 27 countries were eligible (Argentina, Austria, Bahrain, Belarus, Belgium, Brazil, Canada, China, Czech Republic, Denmark, Germany, Greece, Italy, Japan, Korea, Malaysia, The Netherlands, Norway, Oman, Portugal, Serbia, Spain, Sweden, Switzerland, Turkey, United Kingdom, and United States of America). For the HLH-94 criteria and ferritin, information was available in 347 to 351 of 369 (94%-95%), whereas information on NK-cell activity and sIL-2r was available for 240 (65%) and 223 (60%), respectively (Table 1). Hemophagocytosis was found in 287 of 349 (82%) with information available, and in other organs than bone marrow in only 15 of 287 (most commonly the spleen, n = 8). In addition, information on aspartate aminotransferase and alanine aminotransferase values were available in 319 of 369 (86%) and 333 of 369 (90%), respectively, of which 243 of 319 (76%) and 186 of 333 (56%) were >120 U/L.
The patients (n = 369) were evaluated not only as 1 single cohort but also as subgroups: patients with verified FHL-causative mutations or an affected sibling (n = 168), and patients without any of these 2 characteristics (n = 201). Separately, to compare the HLH-2004 and HLH-94 protocols, HLH-2004 patients were also divided into 2 “criteria subgroups,” 1 where HLH-94 criteria were fulfilled (n = 240) and 1 where HLH-2004 criteria were fulfilled but not HLH-94 criteria (n = 129).
Furthermore, as stated in the protocol, patients with XLP, GS2, CHS, and HPS (n = 29) were analyzed separately.11 Patients with other known underlying defined diseases or immunodeficiencies, that is, malignancies, systemic rheumatic diseases, Langerhans cell histiocytosis, Kawasaki disease, or Leishmaniasis, were excluded from the present analyses.
Statistical analyses
The Mann-Whitney U test was used for continuous variables, and Fisher exact and χ2 tests for categorical variables. pSu was estimated using the Kaplan-Meier method for univariate tests, and the Cox proportional hazards model for multivariate tests. Competing risk methodology was used when analyzing time to HSCT and death prior to HSCT.33 Confounders (age and sex) were adjusted for. Two-sided 95% confidence intervals (CIs) were calculated and P values <.05 were considered significant. Analyses were performed using SPSS (version 23; IBM SPSS for Windows, IBM Corp, Chicago, IL) or R (version 3.2.3; The R Foundation for Statistical Computing, Vienna, Austria).
Results
General characteristics and outcome
Altogether, 369 patients were eligible. This makes HLH-2004 the largest prospective study on HLH to date. From the first HLH registry in 1989 to the 2 therapeutic studies HLH-94 and HLH-2004, >700 patients have been evaluated,26,27 a remarkable amount for such a rare disorder.
In HLH-2004, 230 of 369 patients (62%; median follow-up, 5.2 years) were alive at last follow-up with an estimated 5-year pSu of 61% (56%-67%) (Figure 2A). One aim with HLH-2004 was to induce resolution so that HSCT could be performed, and 187 patients (51%) were reported to have achieved resolution at 2 months (20 of whom had had a reactivation). An overview of the outcome in HLH-2004 and HLH-94 is presented in Table 2.
Primary HLH and sHLH
Altogether, 295 patients (80%) were evaluated for FHL-causative genes; 67 were not studied (missing data = 7). Many analyses were made retrospectively, sometimes postmortem. Of these 295, 158 displayed biallelic FHL-causative mutations whereas 137 did not (90 were screened for ≥3 FHL genes, 43 for 1-2 FHL genes, and 4 had monoallelic mutations reported).
One hundred sixty-eight patients (46%) were either familial cases or displayed biallelic gene defects in PRF1, UNC13D, STX11, or STXBP2, that is, had verified FHL, with an overall 5-year pSu of 59% (52%-67%), as compared with 64% (57%-71%) in patients without verified FHL (n = 201) (Figure 2B). One hundred fifty-eight of 168 patients were identified with biallelic FHL-causative mutations (5-year pSu, 61% [53%-69%]). Fifty-nine of 158 displayed PRF1 mutations (5-year pSu, 55% [43%-69%]), 73 of 158 UNC13D mutations (5-year pSu, 64% [53%-76%]), 6 of 158 STX11 mutations (5-year pSu, 63% [21%-105%]), and 20 of 158 STXBP2 mutations (5-year pSu, 64% [45%-89%]). Forty-seven patients had an affected sibling (5-year pSu, 58% [45%-75%]) (Figure 2D), of whom 37 (79%) had biallelic FHL-causative mutations identified.
Additionally, patients with mutations in other HLH-associated genes were studied separately. These 29 patients (XLP [n = 16], GS2 [n = 11], CHS [n = 1], HPS [n = 1]) had a 5-year pSu of 59% (43%-81%).
Infections at diagnosis
One hundred thirty-seven patients (37%) had a reported infection at diagnosis; 32 of these (23%) were patients with verified FHL. Of these, 93 either had EBV (n = 74), cytomegalovirus (CMV) (n = 14), or combined EBV/CMV (n = 5) infection at onset (DNA copies were often not reported). Sixteen of 93 EBV/CMV-infected patients had verified FHL (EBV = 6, CMV = 8, combined EBV/CMV = 2). Seventeen of 74 EBV-infected patients (23%; 5 with verified FHL) underwent HSCT with 9 HSCT survivors, whereas 11 of 74 died without a HSCT (none with verified FHL) and 46 of 74 (62%) were alive without a HSCT.
Mortality in patients not receiving HSCT
In order to identify therapeutically meaningful information, pre-HSCT fatalities during different treatment-related time periods were thoroughly analyzed. Seventy-five of 369 patients (20%) died without HSCT; 50 within the first 2 months of treatment (17 during the first 10 days, 17 during days 11-28, and 16 during days 29-59; median age at onset, 4, 30, and 13 months, respectively). Another 9 died days 60 to 119 (median age, 17 months) and 16 thereafter (8 >365 days after onset; median age at onset, 17 months). Notably, only 28 of 75 (37%) who died pre-HSCT had verified FHL (verified biallelic mutations = 23, affected sibling = 5).
The 17 patients who died days 11 to 28 had remarkably high median age at onset and, notably, 10 of 17 (59%) were aged ≥1 year and without verified FHL as opposed to 3 of 17 (18%) who died during the first 10 days (P = .032) (Figure 3). Among these 10 patients, septicemia, infections, and/or bleedings (associated with thrombocytopenia) were diagnoses reported by the treating physicians in 7 patients; possibly associated with treatment toxicity. Analyzing the treatment period up to 6 weeks, this pattern was further strengthened because 17 of 25 (68%) who died days 11 to 42 were aged ≥1 year and without verified FHL as compared with 3 of 17 who died during the first 10 days (P = .018) (Figure 3).
In contrast, among the 8 (4 with verified FHL) who died days 43 to 59, 6 (75%) were reported by the treating physicians to suffer “refractory HLH,” “fulminant HLH,” “active HLH,” “multiorgan failure,” “progressive disease,” and “HLH reactivation.”
The information in this section suggests that treatment possibly should be (1) risk group stratified and (2) less aggressive days 11 to 42 for some patients, and (3) with less reduction of initial treatment days 43 to 59 for verified FHL patients.
Finally, there was an overrepresentation of deaths after the first 100 days in patients who had had resolution and reactivation, and 8 of 16 children who died after day 120 had verified FHL, stressing the importance of acute/subacute HSCT for these patients (Figure 3).
Serious adverse events
No suspected unexpected serious adverse reaction was reported. In total, 89 SAEs grade III or IV were reported, of which 48 reported 1 or more suspected causative drugs. With regard to 1 single suspected drug, 13 reported CSA (the most common complication being CNS affection, n = 6), 6 reported etoposide (the hepatobiliary system being most frequently affected, n = 3), and 6 reported dexamethasone (5 with cardiac hypertension). In 15 reports, 2 drugs were suspected (CSA = 14, dexamethasone = 14, etoposide = 2), with the most common SAE being cardiac hypertension associated with dexamethasone and CSA (n = 11). Eight reports suspected all 3 drugs to be involved, with infections (n = 5) being most frequent. Posterior reversible encephalopathy syndrome (PRES) was altogether mentioned in 3 SAE reports (2 were drug-associated, both with CSA).
In addition, as in HLH-94,26 1 patient developed acute myeloid leukemia (AML). This patient received no etoposide after 3 weeks of therapy due to infections, and was in complete resolution at 2 months. Two years later, the patient was diagnosed with AML and underwent HSCT but died.
HSCT outcome
One hundred eighty-eight of 369 patients (51%) in HLH-2004 underwent HSCT. Of these, data were available for 185 of whom 121 (65%) were alive at last follow-up (5-year pSu post-HSCT, 66% [59%-73%]) (Figure 4A). One hundred thirty-five of 188 (72%) had verified FHL with 5-year pSu of 70% (63%-78%) (no data = 2) as compared with 54% (63%-78%) for patients without verified FHL (n = 52) (P = .06, log rank) (Figure 4B).
Fifteen (8%) were transplanted before 2 months of therapy, 60 (32%) between 2 and 4 months. Six months after starting treatment, 118 (64%) had received HSCT. The median time to HSCT was 148 days (range, 25-2105 days).
Sixty-four patients died post-HSCT, 36 (56%) prior to day +100, 57 (89%) within the first year, and 7 thereafter. According to reporting clinicians, 31 deaths (48%) were reported as transplant-related mortality (TRM), 16 (25%) as dead of disease/relapse/graft failure, in 11 (17%) the cause of death could not be specified as TRM or death of disease, and 1 (2%) died of a surgical complication. Mortality data were missing in 5 cases.
Patients alive without HSCT
Both HLH-2004 and HLH-94 were designed so that patients without FHL, relapsing, or severe and persistent HLH should stop treatment after 2 months. In HLH-2004, 88 of 369 patients (24%; median age at onset, 2.3 years; range, 33-5675 days) stopped therapy and were off HLH treatment of >1 year and alive without HSCT, that is, presumed sHLH. Interestingly, 2 of these 88 patients, both alive for ≥5 years, displayed biallelic PRF1 p.Ala91Val mutations, a variant debated but sometimes considered a polymorphism.34 Notably, 6 patients had reactivated after stopping initial therapy and restarted initial therapy before they finally became off treatment, but despite their reactivations these 6 were all alive without HSCT. Another patient was off HLH treatment ≥1 year but died due to other reasons (congenital heart failure). In addition, 18 were alive without HSCT with <1 year follow-up.
Comparisons between HLH-2004 and HLH-94
When comparing HLH-2004 with the historical control HLH-94 (n = 232), HLH-2004 patients were divided into 2 groups. In 1 group, patients fulfilled all 5 HLH-94 criteria (n = 240) (“HLH-2004, 1994-criteria”) and in the other 5 of 8 HLH-2004 criteria but not the HLH-94 criteria (n = 129) (“HLH-2004, 2004-criteria”). Patients who fulfilled the HLH-94 criteria in both studies were compared.12 Baseline characteristics were comparable between the 2 studies (Table 2). Patients with an affected sibling (HLH-2004 [n = 47] and HLH-94 [n = 52]) also underwent special evaluation.11,26
Treatment intensification.
For the HLH-2004, 1994-criteria subgroup, 151 (63%) were alive at last follow-up. This subgroup had a nonsignificant tendency to better survival (5-year pSu, 62% [56%-68%]) compared with HLH-94 (5-year pSu, 56% [50%-63%]) with an HLH-94 vs HLH-2004 hazard ratio (HR) of death of 1.23 (95% CI, 0.93-1.64; P = .15) (Figure 2C). Patients included in the HLH-2004, 2004-criteria subgroup displayed a 61% 5-year pSu (53%-70%). Five-year pSu for familial patients in HLH-2004 was 58% (45%-75%) and 56% (44%-71%) in HLH-94 (Figure 2D).
In the HLH-2004, 1994-criteria subgroup, 46 (19%) died pre-HSCT compared with 63 (27%) in HLH-94. Pre-HSCT mortality was further compared using the competing risk methodology, with death and HSCT considered competing events.33 The HLH-94 vs the HLH-2004, 1994-criteria subgroup displayed a HR of 1.45 (0.99-2.12; P = .055), approaching borderline statistical significance to enhanced pre-HSCT survival in HLH-2004. Adjusted for age and sex, the HR was 1.44 (0.98-2.11; P = .064). Among familial patients in HLH-2004, 12 of 47 (26%) died before HSCT, as compared with 12 of 52 (23%) in HLH-94.
In the HLH-2004, 1994-criteria subgroup, 48 of 240 (20%) were off treatment of >1 year and alive without HSCT (median age at onset, 2.5 years), results similar to HLH-94 (48 of 232, 21%) (median age, 2.4 years). Median age at start of therapy, as well as the proportion of patients alive without HSCT, that is, presumed sHLH, were therefore similar in the 2 studies.
During the first 2 months, when CSA was administered in HLH-2004 using the same inclusion criteria, reactivations (15 of 240, 6%) and mortality (27 of 240, 11%) in HLH-2004 were comparable to HLH-94, 18 of 232 (8%), and 33 of 232 (14%), respectively (Table 3).
Results related to HSCT.
For the HLH-2004, 1994-criteria subgroup, median time to HSCT was 154 days (range, 25-2105 days) whereas in HLH-94 it was 180 days (range, 42-1189 days) (HR = 1.25 [0.99-1.6]; P = .074). Adjusted for age and sex, HR was 1.34 (1.047-1.71; P = .020), that is, time to HSCT was significantly reduced in HLH-2004. Among familial patients, median time to HSCT was 126 days (range, 27-2105 days) in HLH-2004 and 165 days (range, 50-1189 days) in HLH-94 (HR = 1.09; 0.69-1.73; P = .70).
In the HLH-2004, 1994-criteria subgroup, 135 (56%) were transplanted with a 5-year pSu post-HSCT of 67% (60%-76%) (no data = 2). In HLH-94, 5-year pSu post-HSCT was 66% (58%-75%) (Figure 4C). For familial patients in HLH-2004, 5-year pSu post-HSCT was 79% (66%-94%) as compared with 70% (57%-86%) in HLH-94 (Figure 4D).
Neurological alterations.
In HLH-2004, 32% displayed CNS involvement at diagnosis, and 17% had CNS complications after 2 months of therapy. For the HLH-2004, 1994-criteria subgroup, 81 of 240 (34%) had neurological alterations at start of therapy, 37 of 205 (18%) displayed CNS complications at 2 months, and 22 of 133 (17%) at start of conditioning. In HLH-94, the corresponding numbers were 32% at onset, 13% at 2 months, and 22% at HSCT (P = .62, P = .22, and P = .26, respectively), that is, the outcome of neurological alterations was not significantly different between the studies.
Discussion
HLH-2004, the second international HLH-study launched by the Histiocyte Society, recruited 369 eligible patients and is, to our knowledge, the largest prospective therapeutic study on HLH to date. Combined with HLH-94 and the first international registry from the Histiocyte Society, over 700 patients have been evaluated, of whom over 600 were prospectively recruited.11,26,27 This is outstanding for such a rare disorder, making the Histiocyte Society an example of what researchers and physicians can accomplish for patients through worldwide collaboration. HLH-2004 itself displays the same international collaborative success with 27 participating countries.
Long-term survival in HLH has improved dramatically over the last decades, from a few percent in the early 1980s, with 1 long-term survivor with verified familial HLH first treated in 1981 still alive,1,27,35,36 to an overall 5-year pSu of 54% in HLH-94, and a 5-year pSu of 61% in HLH-2004.24,26 The reduced pre-HSCT mortality from 27% in HLH-94% to 19% in HLH-2004 was rewarding. Furthermore, both FHL patients (with biallelic mutations in PRF1, UNC13D, STX11, STXBP2, or an affected sibling) and patients with related disorders (XLP, GS2, CHS, and HPS) displayed an overall 5-year pSu of 59%, confirming that the treatment is valuable for patients with all of these genetic defects.29
During the first 2 months of treatment, there was no significant reduction in mortality and reactivations in HLH-2004 as compared with HLH-94. However, there was a trend to reduced pre-HSCT mortality (P = .064 adjusted for age and sex), statistically analyzed using competing risk methodology.33 However, a weakness of HLH-2004 was the nonrandomized design, hence the historical control HLH-94 was used, which obviously makes conclusions less reliable, in particular because supportive care, including anti-infectious treatment, has in all likelihood improved over time.
Altogether, 121 of 185 patients (65%) who underwent HSCT were alive at last follow-up and the overall 5-year pSu post-HSCT was 66%, unfortunately not better than in HLH-94 (Figure 4C). However, time to HSCT (median, 154 days) was significantly reduced in HLH-2004 compared with HLH-94 (P = .020, adjusted for age and sex).
CNS involvement including encephalopathy is frequent in HLH and may result in potentially severe late neurological effects.15,16 In HLH-2004, IT corticosteroids were added to the IT MTX suggested in HLH-94 and, in addition, CSA was initiated on day 1; both were alterations that hopefully would reduce late neurological effects. In HLH-2004, 32% displayed neurological alterations at diagnosis, 17% after 2 months, and 19% at start of HSCT conditioning; proportions not significantly different from those in HLH-94. Notably, despite the increased focus on CNS symptoms in HLH-2004, the proportion of children with reported neurological alterations at HSCT was 22% in HLH-94 and 17% in HLH-2004 (using the HLH-94 inclusion criteria). It has been suggested that CSA may contribute to PRES in HLH,37,38 but PRES has also been associated with other drugs, including corticosteroids.39,40 Notably, encephalopathy is common in the natural course of HLH, and CSA has been reported to be beneficial in rheuma-associated HLH/macrophage activation syndrome.41 In our data, we found no evidence of a marked increase of CSA-induced PRES.
Corticosteroids are important anti-inflammatory drugs for HLH, with dexamethasone having higher concentrations in the cerebrospinal fluid and a longer half-life in the CNS than prednisone.42 Importantly, etoposide can compensate for the cytotoxic defect in FHL and, more specifically, if lymphocytes isolated from FHL patients were subjected to etoposide in vitro, this normalized the otherwise deficient induction of apoptosis.43 Moreover, etoposide can substantially alleviate all symptoms of murine HLH, and the therapeutic mechanism of etoposide involves potent selective deletion of activated T cells and efficient suppression of inflammatory cytokine production.44 Etoposide may induce secondary AML,45 but only 2 of over 600 eligible patients included in the HLH-94/HLH-2004 studies were reported to develop malignancies, hence we feel secure in recommending treatment with etoposide for future HLH studies.
Importantly, based on reports by treating physicians, treatment with HLH-94/HLH-2004 may, possibly, be further improved (Figure 3). (1) Only 28 of 75 (37%) of the patients who died pre-HSCT had verified FHL, whereas in 47 of 75, a verified genetic defect was not identified or not analyzed and, notably, 32 of these 47 (68%) were ≥1 year at onset of disease. Deaths in these somewhat older patients without verified FHL were significantly overrepresented during days 11 to 28, and many of these deaths may be associated with toxicity, suggesting that reduced early cytotoxic therapy might be beneficial for these patients (such as etoposide once weekly instead of twice).46 (2) In contrast, many who died days 43 to 59 suffered active HLH, possibly suggesting a value of intensified therapy during this phase for verified FHL patients compared with the reduced treatment intensity in HLH-2004. (3) Finally, 8 of 16 (50%) who died >120 days after start of initial treatment had verified FHL. Many of these died of reactivation of disease, stressing the importance of an early HSCT.
The results of HLH-2004 compare well with the largest study reported on ATG-based therapy with an overall survival of 21 of 38 (55%) obtained in a highly experienced center.25 Nevertheless, despite the reduced pre-HSCT mortality in HLH-2004 from 27% to 19%, there is still a need for improved pre-HSCT survival; interesting trials with alternative therapeutic approaches for HLH have been initiated, including ATG in combination with etoposide (clinicaltrials.gov identifier: NCT01104025), alemtuzumab (NCT02472054),47 tocilizumab (NCT02007239),48,49 ruxolitinib (NCT02400463),50,51 and a targeted anti-IFN-γ monoclonal antibody (NCT01818492).52-55 Whether these drugs can be sufficient to halt HLH alone or require the addition of etoposide remains to be elucidated, as well as how they are best used (doses, drug combinations, in adults/children, etc).
We conclude that the improvement in survival in HLH/FHL has been extraordinary over the past decades but that the reduced pre-HSCT mortality in HLH-2004 by around one-third, from 27% to 19% compared with HLH-94, was not sufficient to reach statistical significance (P = .064). Positively, time to HSCT was significantly reduced (P = .020), but not neurological alterations. There is thus no strong statistical evidence to suggest HLH-2004 instead of HLH-94. HLH-94 therefore remains the recommended standard of care. Independently, we still recommend the HLH-2004 diagnostic criteria. With regard to improved outcome of HSCT, there are already now promising results reported.32,56,57 Finally, because there is a need for improved pre-HSCT therapy, it would be valuable to perform a randomized study comparing 1 of the novel therapeutic approaches with the HLH-94/HLH-2004 concept updated with the knowledge reported here.
Note added in proof
After acceptance of the manuscript, the principal investigator was notified that 1 patient had to be withdrawn due to incorrect ethical approval in the corresponding country. The patient was a girl aged 54 days at start of therapy with biallelic STXBP2 mutations and in remission after 2 months who died treatment day 366 after relapse (no HSCT performed). Recalculations revealed that 368 patients were eligible with an estimated 5-year pSu of 62% (57%-67%).
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Acknowledgments
The authors sincerely thank all reporting clinicians. They also thank Shinsaku Imashuku, Jorge Braier, David Webb, and Jacek Winiarski for valuable contributions to the protocol design. They are grateful for the invaluable contributions of their previous data managers Martina Löfstedt, Désirée Gavhed, and Tatiana von Bahr Greenwood, and Ida Hed Myrberg for statistical expertise.
This work was supported by grants from the Swedish Childhood Cancer Foundation, the Swedish Research Council, the Cancer and Allergy Foundation of Sweden, the Märta and Gunnar V Philipson Foundation, the Karolinska Institute, and Stockholm Country Council (ALF-project).
Authorship
Contribution: J.-I.H., A.H., M.A., R.M.E., A.H.F., G.J., S.L., and K.L.M. planned the study and recruited patients, with A.H. as study coordinator and J.-I.H. as principal investigator; I.A., E.I., K.L., M.M., V.N., and D.R. served as regional coordinators and recruited patients; S.M. provided epidemiologic advice; E.B. performed data entry and compiled data; and E.B., A.H., and J.-I.H. analyzed results and also wrote the manuscript, which was drafted by E.B. and reviewed and approved by all authors.
Conflict-of-interest disclosure: M.A. and J.-I.H. have been unpaid consultants to NovImmune. The remaining authors declare no competing financial interests.
R.M.E. is retired from the Division of Hematology/Oncology, The Hospital for Sick Children, Toronto, ON, Canada.
A.H.F. is retired from the Division of Bone Marrow Transplant and Immune Deficiency, Cincinnati Children’s Hospital Medical Center, Cincinnati, OH.
Correspondence: Jan-Inge Henter, Childhood Cancer Research Unit, Karolinska University Hospital, SE-171 76 Stockholm, Sweden; e-mail: jan-inge.henter@ki.se.