Copyright
©The Author(s) 2015.
World J Hepatol. Mar 27, 2015; 7(3): 344-361
Published online Mar 27, 2015. doi: 10.4254/wjh.v7.i3.344
Published online Mar 27, 2015. doi: 10.4254/wjh.v7.i3.344
Table 1 Four classes of immunotherapies licensed to treat rheumatoid arthritis
| Class | Mode of action | Drug | Mechanism of action | Route of administration | Therapeutic regimen | Half-life | Major approved indications (FDA) |
| TNF inhibitors | TNF-α neutralization | Adalimumab (fully human monoclonal IgG1 antibody) | Binding to TNF | SC | 40 mg every 2 wk | 13 d | RA, JIA, PsA, AS, CD, UC, PP, non radiographic axial SpA |
| Golimumab (fully human monoclonal IgG1 antibody) | Binding to soluble and membrane bound TNF | SC | 50 mg every 4 wk | 13 d | RA, PsA, AS, UC | ||
| Certolizumab (pegilated FabI fragment of a human monoclonal antibody) | Binding to TNF | SC | 200 mg every 2 wk or 400 mg monthly | 14 d | RA, CD, PsA, AS, non-radiographic axial SpA | ||
| Etanercept (p75 TNF receptor - IgG1 Fc fusion protein | Works as a decoy receptor. It binds to soluble TNF, blocking the binding to its receptor | SC | 50 mg weekly or 25 mg twice a week | 3-6 d | RA, PsA, AS, poliarticular JIA, PP | ||
| Infliximab (chimeric mouse-human monoclonal IgG1 antibody) | Binding to soluble and membrane bound TNF | IV | 3 mg/kg (up to 7.5 mg/kg if not effective) every 8 wk after loading at 0, 2 and 6 wk | 9 d | RA, PsA, AS, CD, pediatric CD, UC, pediatric UC, PP | ||
| B-cell depletion | B-cell lysis | Rituximab (chimeric mouse-human monoclonal IgG1 antibody) | Binding to CD20 and depletion of CD20+ B cells | IV | Two infusions of 1000 mg 2 wk apart. This can be repeated every 6 mo if symptoms return. Infusions are preceded by IV methylprednisolone to reduce the incidence of infusion reactions | 18 d (range 5-76) | BNHL, CLL, RA, GPA, MPA |
| T-cell inhibition | T-cell costimulation blockade | Abatacept (extracellular domain of CTLA4-IgG1 Fc recumbinant human fusion protein) | Binding to CD80/ CD86, blocking T-cell co-stimulation | IV | 500-750-1000 mg infusions (for body weight < 60, between 60 and 100 or > 100 kg) every 4 wk following three loading infusions at 0, 2 and 4 wk | 13 d (range 8-25) | RA, poliarticular JIA |
| SC | 125 mg weekly | ||||||
| IL-6 inhibition | IL-6 receptor blockade | Tocilizumab (humanized monoclonal IgG1 antibody) | Binding to soluble and membrane bound IL-6 receptor | IV | 8 mg/kg every 4 wk | 10-13 d | RA, poliarticular JIA, sistemic JIA |
Table 2 Nomenclatures and definitions used in hepatitis B virus infection
| Markers | Chronic inactive carrier | HBeAg positive CHB | HBeAg negative CHB | “Resolved hepatitis B” |
| HBsAg | + | + | + | - |
| HBeAg | - | + | - | - |
| Anti-HBe | + | - | +/- | +/- |
| Anti-HBs | + | - | +/- | +/- |
| Anti-HBc | + | +/- | + | +/- |
| ALT | - | +/- | + | - |
| Serum HBV-DNA | Undetectable/< 2000 IU/mL | Persistent/intermittent ↑ (> 20000 IU/mL) | Persistent/intermittent ↑ (> 2000 UI/mL) | Detectable or undetectable |
| Liver injury | +/- | Moderate/severe CHB | Minimal to severe CHB | - |
| Necroinflammation | No (> 90%) | Yes (> 90%) | No (> 90%) | No |
Table 3 Hepatitis virus B reactivation in rheumatoid arthritis patients receiving tumor necrosis factor-α inhibitors: studies in patients with markers of chronic or remote hepatitis virus B infection
| Ref. | Study design | Target population | No. of patients | Treatment | Antiviral Prophylaxis | HBsAg+ | Anti-HBc+ and anti-HBs- | Anti-HBc+ and anti-HBs+ | HBV-DNA+ | Anti-HBs+/anti-HBc- | Reactivation |
| Carroll et al[69] | Case series | Rheumatic pts or pts with IBD with CHB | 13 | 11 treated with IFX, 2 treated with ETN | Lamivudine | 13 pts (100%) | - | - | - | - | 7 cases with IFX, 2 cases with ETN |
| Charpin et al[70] | Prospective | RA (12)/SpA (9) pts with resolved HBV infection | 21 | 4 treated with IFX, 14 with ETN, 3 with ADA | 0 pts | 0 pts | 0 pts 100% (with 3 pts < 100 UI/mL) | 0 pts | - | Mean decrease in anti-HBs titre 8%; no cases of HBV reactivation | |
| Chung et al[71] | Retrospective | RA (41), SpA (60), JIA (2) pts | 103 | TNFα inhibitors | 0 pts | 8 pts | - | - | 0 pts | - | 1/8 HBsAg+ (12.5%) after 6 wk of IFX |
| Caporali et al[72] | Prospective | RA (59), SpA (8) pts with resolved HBV infection | 67 | 25 treated with IFX, 23 with ETN, 19 with ADA | 0 pts | 0 pts | 46 pts | 28 pts | 0 pts | - | No cases of HBV reactivation |
| Vassillopoulos et al[73] | Prospective | RA (66), SpA (64), other (1) patients with actual/remote HBV infection or vaccinated for HBV | 131 | 43 treated with IFX, 64 with ETN, 62 with ADA | 14 pts (100% of CHB group): 11 with lamivudine, 2 with entecavir, 1 with telbivudine | 14 pts | 19 pts | 0 pts among CHB group | 19 pts (vaccinated) | No cases of HBV reactivation in pts with resolved HBV infection. In vaccinated pts, slight decrease in anti-HBs titres (median 163 > 105 IU/mL,P= 0.01). Among CHB pts, 1 (7%) treated withLamivudine + ETN developed HBV reactivation due to a resistant mutant strain | |
| Mori et al[74] | Prospective | RA pts with actual/remote HBV infection | 239 | 9 treated with IFX, 18 with ETN, 2 with ADA, 5 with TCZ, 28 with csDMARDs | 2 (100% of HBsAg+ pts) with entecavir | 2 pts | 60 pts | 0 pts | - | 2 cases of HBV reactivation in anti-HBc+ pts (3.3%), 1 with csDMARDs and 1 with ADA | |
| Tamori et al[75] | Prospective | RA pts with positive anti-HBc | 50 | 22 treated with IFX, 20 with ETN, 2 with ADA | Entecavir | 5 pts | 45 pts | - | - | 2/5 (40%) cases of HBV reactivation among HBsAg+ pts; 1/45 (2%) cases of HBV reactivation among HBcAb+/HBsAg- pts, not under TNFI | |
| Pérez-Alvarez et al[76] | Systematic review | TNFI-treated pts | 257 | Anti-TNF (not specified) | Not specified | 89 pts | 168 pts | - | - | HBV reactivation in 35 (39%) pts among HBsAg+ group, fatal in 4 cases. Lower risk if pre-emptive NAs (23%vs62%,P= 0.003). Higher risk with IFXvsETN. Nine cases (5%) of HBV reactivation in HBcAb+/HBsAg- pts, fatal in 1 pt | |
| Lan et al[77] | Prospective | RA anti-HBc+ pts | 88 | 40 pts treated with ETN, 48 with ADA | 10 HBsAg+ pts treated with lamivudine | 18 pts | 12 pts | 58 pts | 0 pts | 22 pts (vaccinated) | Among HBsAg+ pts, no cases of HBV reactivation if pre-emptive NAs; mean decrease in HBV-DNA = 153 IU/mL (P < 0.001); 5/8 cases of reactivation without antivirals. 1 case of HBV reactivation in the HBsAg-/anti-HBs- group |
| Lee et al[78] | Systematic review | HBsAg+ rheumatic disease-positive pts | 122 | 14 pts treated with IFX, 56 with ETN and 25 with ADA | 48 pts (drug not specified) | 122 pts | - | - | Not specified | - | 15 cases (12.3%) of HBV reactivation, including 1 SpA patient treated with pre-emptive lamivudine |
| Lee et al[79] | Systematic Review | HBsAg-/anti-HBc+ rheumatic disease-positive (RA 327, SpA 121) pts | 468 | 100 pts treated with IFX, 269 with ETN and 95 with ADA | Not specified | 0 pts | Not specified | Not specified | Not specified | - | 8 cases (1.7%) of HBV reactivation, 7 with ETN and 1 with ADA; satisfactory clinical outcomes with antiviral therapy |
| Droz et al[38] | Retrospective | Pts with immune-mediated inflammatory diseases (RA 14, CTD 7, vasculitis 5, other 9) developing HBV reactivation | 35 | 7 pts treated with TNF-α inhibitors (not specified), 4 with RTX, 1 with ABA, 1 with TCZ, the others with steroids and/or other immunosuppressants | 5 pts (drug not specified) | 23 pts | 12 pts | Not specified | - | Reactivation occurred a median of 35 wk after therapy start. 88.6% were asymptomatic; 25.7% had severe hepatitis. Management were NAs in 91.4% cases and decrease/withdrawal of immunosuppressants in 45.7%. Pooling these data with literature, earlier reactivation for RTX and HBsAg/HBV-DNA+ pts | |
| Ye et al[80] | Prospective | Inflammatory arthritis pts (50 RA, 37 SpA) | 87 | TNFα inhibitors: 56 treated with IFX, 31 with ETN) | 4 pts among CHB group , 9 pts among inactive carriers (not specified) | 37 (6 HBV-DNA+, 31 HBV-DNA-) pts | 50 pts | Not specified | - | 2 cases of HBV reactivation among CHB pts not receiving pre-emptive NAs, none in those receiving it. Among inactive HBsAg carriers, 6 cases of reactivation in pts who didn’t receive NAs, none in those who did. No cases in HBsAg- pts | |
| Nakamura et al[81] | Retrospective | RA | 57 | 48 treated with TNFα inhibitors (including 9 receiving also TCZ); 7 with TCZ alone and 2 with TCZ and ABA | 0 pts | 0 pts | 11 pts | 38 pts | 0 pts | 8 pts (not vaccinated) | HBV-DNA detected in 3 pts (5.3%), 2 receiving TCZ and 1 receiving ETN, with serum HBV-DNA < 2,1 log copies/mL, and subsequent undetectable HBV-DNA within months |
Table 4 Case reports and studies of hepatitis B virus reactivation in rheumatoid arthritis patients undergoing rituximab
| Ref. | Study design | Patients charachteristics | Therapy | Baseline virological status | Timing of HBV reactivation | Antiviral Therapy | Results | Comments |
| Pyrpasopoulou et al[88] | Case Report | 56-year-old female RA pt starting RTX after 3 anti-TNF (ETN, IFX, ADA) and ABA. Previous diagnosis of CHB | RTX Antiviral prophylaxis with lamivudine | HBsAg+, anti-HBe+ | 1 mo after first RTX administration | Tenofovir + lamivudine RTX withdrawal | Good clinical, serological and virological response | - |
| Ghrénassia et al[89] | Case Report | 78-year-old with RA test+ and erosive RA starting RTX after IFX because of a concomitant diagnosis of lymphoma | RTX monotherapy | HBsAg-/anti-HBc+ | 9 mo after RTX starts | Entecavir RTX withdrawal | Good clinical, serological and virological response | - |
| Gigi et al[90] | Case Report | 64-year-old female RA pt starting RTX as a first-line bDMARD | RTX + methotrexate | HBsAg-/anti-HBc+ | 2 yr after RTX start | Entecavir RTX withdrawal | Good clinical, serological and virological response | - |
| Mitroulis et al[91] | Prospective study | 41 rheumatic pts (34 RA; 7 others) who had received ≥ 1 cicle of RTX and had ≥ 6 mo of follow-up | 17 pts treated with concomitant methotrexate, 35 with concomitant steroids. 2 pts treated with NAs without HBV reactivation | 23 pts not HBV exposed; 4 vaccinated pts; 12 HBsAg-/anti-HBc+ (9 anti-HBs+); 2 pts HBsAg+ anti-HBc+. HBV-DNA undetectable in all pts | No cases of viral reactivation observed | - | - | Slight decrease in anti-HBs titres in vaccinated pts (P = 0.29), never under protective levels |
| Droz et al[38] | Retrospective (subgroup analysis) | 4 pts affected with immune-mediated inflammatory disease treated with RTX | Not specified | Not specified | 4 cases of HBV reactivation a median of 35 wk after therapy start (global data) | Not specified | No cases of fulminant hepatitis | Early reactivation with RTX and in HBsAg+/HBV-DNA+ pts (global data) |
Table 5 Case reports of hepatitis B virus reactivation in rheumatoid arthritis patients undergoing tocilizumab
| Ref. | Study design | Patient charachteristics | Therapy | Basal virological Status | Timing of HBV reactivation | Antiviral Therapy | Results | Comments |
| Nagashima et al[92] | Case Report | 60-year-old female RA pt, RA test and ACPA positive with erosive disease, starting TCZ after IFX and methotrexate | TCZ + steroids | HBsAg-10 yr before TCZ start, basal serological screening not performed | 6, 5 years after TCZ start | Entecavir Ongoing TCZ | Subclinical, good serological and virological responses | Diagnosis made by detection of persistently high serological markers in an asymptomatic pt without liver function tests’ alterations |
| Tsuboi et al[93] | Case Report | 59-year-old female RA pt initially treated with IFX thus withdrawn for HBV reactivation | IFX and then TCZ (after HBV reactivation) | Serological screening not performed before IFX. At 5th IFX infusion HBsAg+/HBV-DNA+/HBeAg+ | 32 wk after IFX start | Lamivudine Ongoing TCZ | Good clinical, serological and virological response until 2 years after TCZ start | - |
| Kishida et al[94] | Case Report | Adult-onset Still’s disease pt affected with CHB | TCZ + ongoing entecavir | HBsAg+ | No reactivation observed | - | Good clinical, serological and virological response until end of follow-up | - |
| Nakamura et al[81] | Retrospective | Among 9 RA pts treated with TCZ (7 with TCZ alone and 2 with TCZ and ABA in sequence), 2 cases of HBV reactivation were detected: (a) 75-year old male pt starting TCZ as a first line therapy | TCZ monotherapy | HBcAb+ Undetectable HBV-DNA | 4 mo after TCZ start | - | Subclinical, subserological, good virological response | HBV-DNA fluctuated always < 2, 1 log copies/mL throughout 4 mo until it became persistently undetectable, even after switch to ETN (due to lack of efficacy) |
| (b) 55-year-old female pt starting TCZ after IFX and ETN | TCZ + methotrexate | HBcAb+ Undetectable HBV-DNA | 2 mo after TCZ start | - | Subclinical, subserological, good virological response | HBV-DNA fluctuated always < 2, 1 log copies/mL throughout 5 mo until it became persistently undetectable, even after switch to ADA (due to lack of efficacy) | ||
| Droz et al[38] | Retrospective (subgroup analysis) | 1 pt affected with immune-mediated inflammatory disease treated with TCZ | Not specified | Not specified | median of 35 wk after therapy start (global data) | Not specified | No cases of fulminant hepatitis | Early reactivation in HBsAg+/HBV-DNA+ pts (global data) |
Table 6 Case reports of hepatitis B virus reactivation in rheumatoid arthritis patients undergoing abatacept
| Ref. | Study design | Patientscharacteristics | Therapy | Basal virological status | Timing of HBV reactivation | Antiviral therapy | Results | Comments |
| Kim et al[95] | Retrospective | 8 RA pts affected with CHB | ABA + pre-emptive NAs (4 pts: 3 with entecavir and 1 with tenofovir) ABA without antiviral prophylaxis (4 pts) | HBsAg+ Detectable HBV-DNA in 3/8 pts | Not specified | Not specified | Among pts receiving NAs, no cases of HBv reactivation. Among pts without antiviral prophylaxis, all pts experienced HBV reactivation | Among pts receiving NAs, a statistically significant improve in DAS28-ERS was detected; which was not noted in the control group |
| Germanidis et al[96] | Case Report | 72-year-old female RA pt starting ABA after ADA | ABA + leflunomide | Anti-HBc+/HBsAg-/anti-HBs+/anti-HBe+ | 6 mo after ABA start | ABA and leflunomide withdrawal Consequent anviral treatment with tenofovir (12 about 1 yr later) | Good clinical, serological and virological response to tenofovir | 2 mo time lag between ABA withdrawal and liver tests flare, suggesting that HBV reactivation evolved in parallel with T cell immune reconstitution |
| Fanouriakis et al[97] | Case report | 68-year-old female RA pt with erosive disease | ABA + methotrexate | HBsAg-/anti-HBc+ Basal HBV-DNA unknown | 10 mo after ABA start | Tenofovir ABA withdrawal | Good clinical, serological and virological response | - |
| De Nard et al[98] | Case series | 9 RA pts treated with ABA | ABA 8/9 pts treated with concomitant methotrexate Lamivudine in 2 pts (1 HBsAg+ and 1 HBsAg-) from baseline, and in 1 pt with comorbid HCV infection after ABA start | 8 HBsAg-/anti-HBc+ 1 HBsAg+/HBV-DNA- | 1 pt with comorbid HCV infection experienced aminotransferases elevation (< 2 x ULN) 2 mo after ABA start | Lamivudine Ongoing ABA | Subclinical, gradual amelioration of liver function tests, persistently undetectable HBV-DNA | No cases of HBV reactivation among pts receiving pre-emptive NAs |
| 1 pt with resolved HBV infection not receiving NAs developed HBV-DNA positivation 12 mo after ABA start | Ongoing ABA No prophylaxis | ConsecutiveHBV-DNA fluctuations; no flares in liver function tests even after entecavir initiation at 24 mo while switching to ADA (unpublished data) | ||||||
| Droz et al[38] | Retrospective (subgroup analysis) | 1 pt affected with immune-mediated inflammatory disease treated with ABA | Not specified | Not specified | median of 35 wk after therapy start (global data) | Not specified | No cases of fulminant hepatitis (global data) | Early reactivation in HBsAg+/HBV-DNA+ pts (global data) |
- Citation: Nard FD, Todoerti M, Grosso V, Monti S, Breda S, Rossi S, Montecucco C, Caporali R. Risk of hepatitis B virus reactivation in rheumatoid arthritis patients undergoing biologic treatment: Extending perspective from old to newer drugs. World J Hepatol 2015; 7(3): 344-361
- URL: https://www.wjgnet.com/1948-5182/full/v7/i3/344.htm
- DOI: https://dx.doi.org/10.4254/wjh.v7.i3.344