Human leukocyte antigens HLA DRB1 influence clinical outcome of chronic lymphocytic leukemia

doi:10.3324/haematol.10910

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Lymphoproliferative Disorders

Human leukocyte antigens HLA DRB1 influence clinical outcome of chronic lymphocytic leukemia

Ewa Lech-Maranda^*^,#, Przemyslaw Juszczynski^*^,#^,@, Anna Szmigielska-Kaplon^*, Krzysztof Jamroziak^*, Ewa Balcerczak^°, Tadeusz Robak^*^,

^* Department of Hematology, Medical University of Lodz, Poland
^° Department of Pharmaceutical Biochemistry, Medical University of Lodz, Poland

Correspondence: Tadeusz Robak, MD, PhD, Department of Hematology, Medical University of Lodz, Ciolkowskiego 2 str, 93-510 Lodz, Poland. Phone/fax: international +4842.6895191/6895192. E-mail: robaktad{at}csk.umed.lodz.pl

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We investigated HLA DRB1 correlations with chronic lymphocyticleukemia (B-CLL) outcome in 90 patients. Neither of the alleleswas associated with B-CLL clinical characteristics or mortality.HLA DRB1*01 and HLA DRB1*02-null were associated with shorteroverall survival (p=0.007, p=0.002). Our results suggest thatHLA-restricted adaptive immunity influences CLL outcome.

Key words: chronic lymphocytic leukemia, HLA class II, HLA DRB1, outcome.

B-cell chronic lymphocytic leukemia (B-CLL) is the most commonadult leukemia in Western countries and North America. It ischaracterized by the clonal accumulation of CD5⁺ B-cells expressingCD19, CD23 and low surface IgM.¹ Its origins still remains largelyunknown, although genetic susceptibility appears to play animportant role.² The Human Leukocyte Antigen complex (HLA) isone of the inherited factors that influences the developmentof B-CLL and clinical outcome of diffuse large B-cell lymphoma.^3–5This led us to examine whether HLA antigens contribute to theclinical course of CLL.

Allelic frequencies of HLA DRB1 were systematically examinedin 90 B-CLL patients seen in the Department of Hematology during2003–2004 for control visits, and in 94 ethnically-matched,healthy controls. Patients’ confidentiality was maintainedin accordance with Polish regulations for studies on human subjects.Clinical characteristics of CLL patients are presented in Table 1.Of 90 patients enrolled in the study, 58 required treatmentand were available for an estimation of treatment response.Forty patients (69%) achieved complete or partial remissionand 18 (31%) did not. Twenty-one patients (36%) experienceddisease progression or relapse and 25 patients died. HLA DRB1genotyping was performed using PCR-based reverse blot technology(RELI SSO; Dynal, Oslo, Norway) according to the manufacturer’sprotocol. Statistical tests were two-tailed with the level ofsignificance p<0.05. Survival was estimated according tothe Kaplan-Meier method. Comparison of survival was based onlog-rank testing as previously described, with death for anycause as a censoring variable.⁵

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Table 1. Clinical characteristics of 90 CLL patients included in the study.

The HLA DRB1 allelic frequencies and distributions were consistentwith the Hardy-Weinberg equilibrium, and did not differ significantlybetween CLL patients and the control group. We assessed HLADRB1 allele frequency using low (two-digit) typing resolution.We were therefore unable to detect previously reported associationsof HLA DRB1*0401 and DRB1*0403 with CLL incidence, or DRB3 (DR52)and DRB4 (DR53) supertypical loci with age-at-onset of CLL.^3,6

There were no associations between HLA DRB1 alleles and clinicalcharacteristics of CLL patients at diagnosis, including age,clinical stage according to Rai classification, surface CD38expression, serum levels of lactate dehydrogenase (LDH) andß2-microglobulin (data not shown). In patients withHLA DRB1*01 allele, there was a trend towards a shorter timefrom diagnosis to treatment (log-rank test, p=0.07, Figure 1A.)Neither of assessed HLA DRB1 alleles was associated with responseto first-line treatment or mortality. With a median follow-upof surviving patients of 49 months(range 2.5–105 months),the subgroups of patients with HLA DRB1*01 and HLA DRB1*02 nullallele had a significantly shorter overall survival (OS), (log–ranktest, p=0.007 and p=0.002, respectively; Figure 1B and C). Tofurther characterize HLA DRB1 linkages with survival in CLLpatients, we analyzed both DRB1*02 splits (DRB1*15 and DRB1*16)and found that only DRB1*15 null allele remained significantlyassociated with shorter OS (p=0.015; Figure 1D). However, neitherof these genetic markers was found to be associated with freedomfrom progression in CLL patients. Clinical stage according toRai classification as a unique parameter (Rai 0–1 vs 2–4),with HLA DRB1* 01, HLA DRB1*02 null alleles and CD38 surfaceexpression was included for analysis. In a multivariate Coxregression model, the HLA DRB1*01 remained an independent factorpredicting for shorter OS (p=0.005, relative risk [RR]= 3.84).

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Figure 1. HLA DRB1 alleles and clinical course of chronic lymphocytic leukemia. A. Time to treatment in HLA DRB1*01 positive and negative patients. B. Overall survival in HLA DRB1*01 positive and negative patients. C. Overall survival in HLA DRB1*02 positive and negative patients. D. Overall survival in HLA DRB1*15 positive and negative patients.

Overall, our studies suggest that HLA-DRB1 alleles influenceCLL outcome. Although T cells from patients with CLL containa number of defects, they are capable of initiating autologouscytotoxic and proliferative responses directed against the CLLcells in vitro. These can be further increased with professionalantigen-presenting cells in an HLA–I and –II restrictedfashion.^7,8 Our data suggest that natural T-cell responses againstCLL antigens are also likely to depend on certain inheritedHLA alleles and their ability to efficiently present tumor-relatedantigens. These observations may explain the differences inoverall survival in CLL patients carrying HLA-DRB*01 and -DRB*02null allele. Alternatively, we cannot exclude that HLA-DRB1alleles are markers of other pathologically relevant genes remainingin linkage disequilibrium with these loci. It has been recentlyreported that HLA-G, a non-classical, immunosuppressive HLAclass I molecule remaining in linkage disequilibrium with certainDRB1 alleles, is an independent factor predicting CLL progression.^9,10

In conclusion, we suggest that HLA-DRB1 alleles influence CLLoutcome. These observations may have profound implications forunderstanding DC-based immunotherapies of CLL, implying thatpatients with certain HLA alleles are less likely to respondto DC vaccinations. Passive immunomodulation with HLA DR monoclonalantibodies may help those with a poor prognosis to achieve astable remission.

Footnotes

^# These authors contributed equally to this work and should bothbe considered first authors

^@ Current address: Dana-Farber Cancer Institute, Boston, MA 02115,USA

Presented in preliminary form at the 10^th Congress of the EuropeanHematology Association, Stockholm, Sweden, June 2–5, 2005.

Funding: supported by the Medical University of Lodz, Poland(Grant 502-11-051).

References

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