Baseline Thrombopoietin Level is Associated with Platelet Count Improvement in Thrombocytopenic Chronic Hepatitis C Patients After Direct-Acting Antiviral Agent Therapy

Abstract

Background

Thrombocytopenia can rapidly improve in chronic hepatitis C (CHC) patients receiving direct-acting antiviral agents (DAA). The role of baseline (BL) thrombopoietin (TPO) in this phenomenon is unclear.

Methods

From June 2016 to February 2019, a total of 104 CHC patients receiving DAA, with a sustained virologic response and BL thrombocytopenia, at Dalin Tzu Chi Hospital, were enrolled in this retrospective study. Significant platelet count improvement and platelet count improvement ratio were analyzed for correlation with BL TPO.

Results

This cohort included 40 men (38.5%). Seventy-two (69.2%) patients had advanced fibrosis. The platelet count [median (range)] increased from 110.5 (32–149) × 10³/µL at BL to 116.5 (40–196) and 118.0 (35–275) × 10³/µL at end of treatment (EOT) and 12 weeks after EOT (P12), respectively, (EOT vs. BL, P < 0.001; P12 vs. BL, P < 0.001).BL TPO was positively correlated with significant platelet count improvement (P < 0.001), platelet count improvement ratio at EOT (P = 0.004), and P12 (P < 0.001). The area under the receiver operating characteristic curve and optimal cutoffs (pg/ml) were 0.77 (95% confidence interval, 0.67–0.86) and 120, respectively, for significant platelet count improvement prediction. The sensitivity, specificity, and accuracy were 88.6%, 71.7%, and 78.8%, respectively.

Conclusions

BL TPO level might be a useful marker for predicting significant platelet count improvement in thrombocytopenic patients after successful DAA therapy.

Background

Thrombocytopenia (defined as < 150 × 10³/µL) in patients with chronic liver disease (CLD) is relatively common, especially in chronic hepatitis C (CHC)-infected patients. The prevalence is about 6% in CLD patients, 24% in CHC patients, and up to 78% in cirrhotic patients. ^1–3 Sustained virologic response (SVR), achieved by interferon-based therapy, for CHC-related advanced liver fibrosis improves thrombocytopenia after a long-term follow-up.^4,5 This was thought to be associated with an improved fibrosis stage and portal hypertension. ^4,5 Reportedly, thrombocytopenia rapidly improves in CHC patients receiving direct-acting antiviral agents (DAA). ^6–10 However, this improvement, within short-term follow-up, is less likely due to changes in the fibrosis stage. ¹¹ It suggests that factors other than fibrosis may play important roles, such as hypersplenism, thrombopoietic cytokines, antiplatelet antibody, or direct effect from hepatitis C virus (HCV) via suppressing hematopoiesis. ^3,12−17

Thrombopoietin (TPO), a thrombopoietic cytokine, is involved in megakaryocyte maturation and platelet production. ¹⁸ TPO is primarily produced in the liver and its level is affected by liver fibrosis stage and platelet turnover. ^{3, 13–15,19} This partly accounts for thrombocytopenia in CLD patients. ³ TPO mimetics have been shown to improve platelet count in thrombocytopenic CLD patients. ²⁰

Data on the relationship between TPO and rapid thrombocytopenia improvement after DAA therapy has not been well reported. Hence, this study investigated the association between baseline (BL) TPO and platelet count improvement after HCV clearance.

Methods

Results

Discussion

This study showed that overall platelet counts were significantly increased in thrombocytopenic CHC patients after successful DAA treatment. BL TPO is positively associated with significant platelet count improvement and platelet count improvement ratio. BL TPO level > 120 pg/ml can predict significant platelet count improvement.

BL TPO can be positively associated with significant platelet count improvement and is correlated with platelet count improvement ratio at EOT and P12 (ρ = 0.282, P = 0.004 and ρ = 0.502, P < 0.001 at EOT and P12, respectively). This association may be related to the splenic size and fibrosis stage. Previous studies have demonstrated that a higher TPO is related to a smaller spleen size^29,30 and less hepatic fibrosis.^{13–15, 19,31} In our study population, it was shown that those without splenomegaly had significantly higher TPO levels. However, analysis of the TPO levels between non-advanced and advanced fibrosis patient groups showed no significant difference. TPO alone may not truly reflect synthesis function of the liver because it is produced by the liver at a constant rate and removed from circulation by TPO receptors on megakaryocytes and platelets.^32,33 Platelet turnover also affects TPO level. ^3,34 We did not check platelet turnover; therefore, the low TPO level might be attributed to either poor liver function or high platelet turnover. Another likely reason is that we classified non-advanced or advanced hepatic fibrosis by the FIB4 score; some patients in the advanced fibrosis group may actually have non-advanced hepatic fibrosis. The actual reason requires further studies checking platelet turnover and using liver biopsy as a classification method for TPO level analysis in different fibrosis stages.

Though we knew baseline TPO was positively correlated to the platelet count change, the cut-off value was unclear. Therefore, we used ROC test and found the baseline TPO level > 120 pg/ml was associated with significant platelet count improvement. The sensitivity is 88.6%, and specificity is 71.7%, with accuracy being 78.8%. Hence, when thrombocytopenia is observed in untreated CHC patients, this cut-off value may be helpful in predicting who would have significant improvement after DAA therapy.

In the current study, BL TPO levels were not correlated with BL platelet count (ρ = 0.054, P = 0.587). This result was also corroborated by other studies. ^19,29,30 It is reasonable to see this phenomenon because absolute platelet count is affected by TPO, spleen size, autoimmune status, megakaryocyte mass in bone marrow, and the aforementioned viral effect. ^16,29 We also found that the TPO level (32–3944 pg/mL) in patients was more variable, compared to the normal population (81.3–237.7 or 19.25–377.75 pg/ml).^29,35 This suggests that the ability of our patients to produce or destroy TPO differed significantly. Although some patients, with liver disease, had higher TPO levels, the elevation was mostly inadequate, compared with thrombocytopenic patients due to other diseases such as aplastic anemia or chemotherapy-induced thrombocytopenia. ³¹ In patients with early stage liver fibrosis, TPO production may increase to partly compensate for the decreased platelet count; those with more advanced fibrosis or liver cirrhosis produce relatively and inappropriately low TPO. ^{13–15, 19,31} Moreover, other factors such as hypersplenism, may offset the positive effect of elevated TPO. Congested spleen contains a large platelet mass, which would bind to, internalize, and destroy TPO. ^30,36 We found that those with splenomegaly had significantly lower TPO than those without splenomegaly. A negative association between TPO level and spleen size was also reported by other studies,^29,30 but there was a study revealing no correlation between them.¹⁹ These differences may be due to the relatively small number of cases in these studies and patient selection criteria.

This study found that the only factor associated with significant platelet count improvement was high BL TPO. Other BL characteristics were not related to such changes after DAA therapy. This was partly different from our previous study.⁸Our previous study showed that moderate to severe fatty liver and low BL platelet count could predict significant platelet count improvement. The most likely reasons were that some differences existed in the previous study, compared to findings of the present study, including more case numbers (n = 249), more cancer patients (n = 19 vs. n = 0, P = 0.001), viable HCC patients (n = 14 vs. n = 0, P = 0.013), more advanced hepatic fibrosis patients (n = 213 vs. n = 72, P = 0.001), and more moderate to severe fatty liver patients (n = 24 vs. n = 5, P = 0.2).

There are some limitations of our study. First, we did not perform biopsy of the liver in all patients to check inflammation and fibrosis severity. Instead, we used noninvasive indices such as the FIB-4 test, to identify patients with advanced fibrosis; this is a relatively reliable method. ²² Second, we did not perform bone marrow biopsy in this study to exclude possible indolent hematological disorders in our patients. Bone marrow biopsy is an invasive procedure, which could not be performed except with a clinically strong indication. Third, we did not check for platelet turnover. However, hypersplenism is the main contributor to platelet turnover in patients with splenomegaly,³⁴ which were included in our study. In patients without splenomegaly, more evidence is required to clarify the association between platelet count and turnover, TPO level, and liver fibrosis severity. Fourth, other thrombopoietic cytokines such as interleukin-6, -11, and-3, were not evaluated. Their importance among these thrombocytopenic patients remains unknown. Therefore, further studies are needed.

Conclusion

Successful DAA therapy for CHC patients results in significant platelet count improvement. BL TPO level is positively correlated with significant platelet count improvement and platelet count improvement ratio. The BL TPO cutoff value of 120 pg/ml can predict significant platelet count improvement among CHC-related thrombocytopenic patients.

Abbreviations

CLD, chronic liver disease; CHC, chronic hepatitis C; SVR, sustained virologic response; DAA, direct-acting antiviral agent; HCV, hepatitis C virus; TPO, thrombopoietin; BL, baseline; P12, 12 weeks after end of treatment; AST, aspartate aminotransferase; ALT, alanine aminotransferase; EOT, end of treatment; FIB-4, fibrosis-4; HCC, hepatocellular carcinoma; eGFR, estimated glomerular filtration rate; and AFP, alpha-fetoprotein.

Declarations

Ethics approval and consent to participate

The study protocol was approved by the Ethics Committee of Dalin Tzu Chi Hospital (approval number B10704013). All patients signed the informed consent.

Consent for publication

Not applicable.

Availability of data and materials

The datasets generated and analyzed during the current study are available from the corresponding author on reasonable request.

Competing interests

The authors declare that they have no competing interests.

Funding

This study was funded by the Dalin Tzu Chi Hospital, Buddhist Tzu Chi Medical Foundation through grant number DTCRD108-I-05. The sponsors played no role in the study design; in the collection, analysis, and interpretation of data; in the writing of the report; and in the decision to submit the article for publication.

Authors' contributions

Chen YC: the drafting of the article, acquisition of patients and clinical data, analysis, interpretation of the data, critical revision for important intellectual content; Ping Ko PH: acquisition of patients and clinical data; Lee CC: experimental procedures, analysis of the data; Tseng CW: acquisition of patients and clinical data, analysis, interpretation of the data, critical revision for important intellectual content; Tseng KC: substantial contributions to the conception and design, acquisition of patients and clinical data, analysis, interpretation of the data, the drafting of the article, critical revision for important intellectual content, final approval of the version to be published, agreement to be accountable for all aspects of the work. All authors approved the final version of the article.

Acknowledgements

We would like to thank Miss Yi-Ting He for her assistance in procuring the record.

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