Abstract
The emergence of novel drugs has significantly improved outcomes of patients with plasma cell neoplasms (PCN). The Japanese Society of Hematology conducted a prospective observational study in newly diagnosed PCN patients between 2016 and 2021. The analysis focused on 1385 patients diagnosed with symptomatic PCN between 2016 and 2018. The primary endpoint was the 3-year overall survival (OS) rate among patients requiring treatment (n = 1284), which was 70.0% (95%CI 67.4–72.6%). Approximately 94% of these patients received novel drugs as frontline therapy. The 3-year OS rate was 90.3% (95%CI 86.6–93.1%) in the 25% of patients who received upfront autologous stem cell transplantation (ASCT), versus just 61.4% (95%CI 58.0–64.6%) in those who did not receive upfront ASCT. The only unfavorable prognostic factor that affected OS in ASCT recipients was an age of 65 or higher. For patients who did not receive ASCT, independent unfavorable prognostic factors included frontline treatment with conventional chemotherapies, international staging system score of 2/3, extramedullary tumors, and Freiberg comorbidity index of 2/3. This study unequivocally demonstrates that use of novel drugs improved OS in Japanese myeloma patients, and underscores the continued importance of upfront ASCT as the standard of care in the era of novel drugs.
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Introduction
According to data from the Japan National Cancer Registry, there were 7130 newly diagnosed multiple myeloma (NDMM) patients in 2015, comprising 3736 males and 3394 females. 4135 patients, consisting of 2030 males and 2105 females, passed away (1). The annual incidence rate of multiple myeloma gradually increased from 5.0 per 100,000 persons in 2010 to 6.0 in 2019 [1]. The estimated 5-year overall survival (OS) rate between 2009 and 2011 was 42.8% [1].
Multiple novel anti-myeloma drugs, including proteasome inhibitors (PIs), immunomodulatory drugs (IMiDs), and monoclonal antibodies (mAbs), have been developed and approved by the Pharmaceuticals and Medical Devices Agency (PMDA) for the treatment of multiple myeloma (MM) patients under the coverage of the national health insurance system in Japan. Initially, bortezomib was approved in 2006 for the treatment of relapsed and/or refractory multiple myeloma (RRMM). Subsequently, thalidomide and lenalidomide were approved for RRMM in 2008 and 2010, respectively. Based on the pivotal phase 3 VISTA [2] and FIRST [3] trials, bortezomib and lenalidomide were further approved for the treatment of newly diagnosed multiple myeloma (NDMM) in 2011 and 2015, respectively. In subsequent years, pomalidomide, carfilzomib and elotuzumab, ixazomib and daratumumab, and isatuximab were, respectively, approved for the treatment of RRMM in 2015, 2016, 2017, and 2020. Notably, daratumumab was also approved for the treatment of NDMM in 2019 based on the primary analyses of phase 3 trials, namely, ALCYONE [4, 5] and MAIA [6, 7].
Although the Japan National Cancer Registry operated by the National Cancer Center and the hematologic diseases registry operated by the Japanese Society of Hematology (JSH) exist, these registries do not gather sufficient data to conduct in-depth analyses of patient characteristics and outcomes. In 2015, Ozaki et al. provided a comprehensive overview of patient demographics and prognosis for Japanese multiple myeloma (MM) patients treated at hospitals where members of the Japanese Society of Myeloma (JSM) were employed [8]. The study retrospectively collected and analyzed real-world data from two cohorts: the 1990–2000 cohort consisting of 1208 patients and the 2001–2012 cohort consisting of 2234 patients, in collaboration with the JSM [8]. The analysis revealed a notable improvement in the 5-year overall survival (OS) rate, which increased from 31.2% in the 1990–2000 cohort to 50.3% in the 2001–2012 cohort. Furthermore, within the latter cohort, a subset of patients received treatment with novel drugs such as bortezomib, thalidomide, and lenalidomide, leading to a remarkable improvement in their prognosis. Since no national survey of Japanese MM patients has been conducted since the aforementioned report, we have undertaken a prospective collection and analysis of real-world data from the 2016–2018 cohort, in collaboration with the JSH, to elucidate the effects of novel anti-myeloma drugs.
Methods
Study design
The study described was a non-interventional, multicenter, prospective cohort study of the patients with plasma cell neoplasms (PCN) conducted in Japan, overseen by the Japanese Society of Hematology (UMIN000022099). The study adhered to the ethical principles outlined in the Declaration of Helsinki and the Ethical Guidelines for Medical and Health Research. The study protocol received approval from the institutional review boards (IRB) at all participating sites.
Patients and treatments
A total of 67 sites across Japan participated in this study. Patients who were diagnosed with PCN between January 2016 and December 2018 were registered and followed up until the end of December 2021, patient withdrawal, or death. The PCN group encompassed both symptomatic conditions (such as symptomatic multiple myeloma, non-secretory multiple myeloma, multiple plasmacytoma, and plasma cell leukemia) and non-symptomatic conditions (such as monoclonal gammopathy of undetermined significance [MGUS], smoldering multiple myeloma, solitary plasmacytoma of bone, and extramedullary plasmacytoma), as per the diagnostic criteria of the International Myeloma Working Group (IMWG) [9, 10]. Patients with symptomatic PCN received treatment with drugs approved by the Pharmaceuticals and Medical Devices Agency (PMDA) based on the physician’s discretion.
Endpoints
The primary endpoint of this study was the 3-year overall survival (OS) of newly diagnosed patients with symptomatic PCN who were treated with systemic chemotherapy. Secondary endpoints included progression-free survival (PFS), time to next treatment (TNT), treatment-free interval (TFI), and the best overall response rates (ORR) based on the International Myeloma Working Group (IMWG) uniform response criteria [11] as determined by the first-line treatment. The definitions of OS, PFS, TNT, and TFI can be found in Supplementary Method S1.
Statistical analysis
In the United States, where novel anti-myeloma drugs were widely utilized, the real-world data showed a 3-year OS rate of 70% [12]. To achieve a 3-year survival rate with a 95% confidence interval (CI) range of less than 7%, a sample size of 800 patients with symptomatic PCN would be required. Accounting for non-symptomatic PCN and potential dropouts, the number of patients in this study was set at 1100. The analysis focused on patients diagnosed with symptomatic PCN who received treatment with anti-myeloma drugs, as well as patients initially diagnosed with non-symptomatic PCN at registration but progressed to symptomatic PCN requiring treatment during the study period. Baseline patient characteristics were summarized using descriptive statistics. PFS, OS, TNT, and TFI were estimated using the Kaplan–Meier method, and the 95% CI was calculated using the Greenwood formula. Univariable and multivariable Cox proportional hazards regression analyses were performed to assess the association between OS or PFS and clinically significant baseline factors, providing hazard ratios (HR) and their corresponding 95% CI. All statistical analyses were conducted using SAS version 9.4 (SAS Institute, Cary, NC, USA).
Results
Patient characteristics
Between January 2016 and December 2018, a total of 1951 patients with PCN were registered from 67 hospitals across Japan. After excluding 52 patients due to ineligibility or insufficient data, 1899 patients were included in the analysis. Among them, 1349 patients were diagnosed with symptomatic PCN and required some form of treatment, while the remaining 550 patients were initially diagnosed with non-symptomatic PCN. During the study period, 59 patients with non-symptomatic PCN progressed to symptomatic PCN, with 36 of them experiencing this progression by December 2018. Therefore, a total of 1385 patients with symptomatic PCN (1349 plus 36) were analyzed in this report. Among these patients, 1274 were diagnosed with symptomatic multiple myeloma (MM), 14 with non-secretary MM, 70 with multiple plasmacytoma, and 27 with plasma cell leukemia (PCL) (Fig. 1).
In Table 1, the median age of the patients was 71 years (ranging from 33 to 96 years), and 1044 (75.4%) patients were 65 years or older. Female patients constituted 47.7% of the cohort. Eastern Cooperative Oncology Group Performance Status (ECOG PS) scores were distributed as 78.1% for 0–2 and 21.9% for 3–4. Regarding the ISS, 20.1%, 35.8%, and 40.1% of patients were classified into stages 1, 2, and 3, respectively. The M-protein types were IgG in 55.9% of cases and non-IgG in 40.4%. Various symptoms were observed in the patients, with hypercalcemia in 13.0%, renal insufficiency in 25.3%, anemia in 61.4%, and bone diseases in 61.5% of cases. Accompanying symptoms such as AL amyloidosis, extramedullary tumors, and central nervous system (CNS) invasion were observed in 6.1%, 8.4%, and 0.6% of the patients, respectively. The distribution of Freiburg comorbidity index (FCI) scores [13] was as follows: 61.7% had an FCI of 0, 29.2% had an FCI of 1, 7.9% had an FCI of 2, and 1.1% had an FCI of 3.
In Table 2, we showed the clinical characteristics of the patients treated with and without autologous stem cell transplantation (ASCT). Nine-hundred and twenty-two patients received the initial induction therapy but did not undergo ASCT (non-ASCT-Group), while the remining 342 patients underwent ASCT within 1 year from the start of the initial induction therapy (ASCT-Group). The patients who received no initial induction therapies (n = 101), that who received an allogeneic transplant (n = 1), or those who underwent ASCT after 1 year from the start date of the initial therapy (n = 19) were not included in either group. The median ages (range) were 75 (37–92) in non-ASCT-G and 60 (33–73) in ASCT-G, respectively. 91% and 31.9% of the patients of non-ASCT-G and ASCT-G were over 65 years. ECOG PS 0–2/3–4 in non-ASCT-G and in ASCT-G were 77.7/22.3% and 85.4/14.6%, respectively. ISS 1/2/3 in non-ASCT-G and in ASCT-G were 14.9/35.8/44.9% and 35.4/36/27.5%, respectively. The symptoms of hypercalcemia, renal insufficiency, anemia, and bone diseases were seen in 13.3, 28.4, 65.3, and 58% of non-ASCT-G and in 11.4, 16.4, 51.8, and 75.4% of ASCT-G. FCI 0/1/2/3 in non-ASCT-G and in ASCT-G were 57.9/32.2/8.8/1.1% and 76.6/20.2/2.6/0.6%, respectively.
Overall survival and its prognostic factors
The 3-year overall survival (OS) rate for symptomatic patients with PCN who required any form of treatment (n = 1284) was found to be 70.0% with a 95% CI of 67.4% to 72.6% (Fig. 2a). Among these patients, 342 individuals (24.7%) received upfront ASCT, while 922 patients (66.6%) did not undergo ASCT as their initial therapy but received conventional treatments. In subgroup analysis, the 3-year OS rates for the former and latter patient groups were 90.3% (95%CI 86.6–93.1%) and 61.4% (95%CI 58.0–64.6%), respectively (Fig. 2b). Tables 3 and 4 illustrate the results of further analysis. In the patient group who received ASCT, only age 65 or older had a significant impact on worse OS rate, with a HR of 2.24 (95%CI 1.33–3.77) in multivariable analysis (Suppl Fig. 1a). On the other hand, in the patient group who did not undergo ASCT, induction treatments containing immunomodulatory drugs (IMiD), proteasome inhibitors (PI), and the combination of IMiD and PI were associated with better OS rates compared to conventional chemotherapy, with HRs of 0.64 (95%CI 0.43–0.95), 0.69 (95%CI 0.48–1.00), and 0.59 (95%CI 0.37–0.93), respectively, as determined by multivariable analysis. Furthermore, ISS 2 and ISS 3 were associated with worse OS rates compared to ISS 1, with HRs of 2.05 (95%CI 1.38–3.02) and 2.82 (95%CI 1.91–4.19), respectively (Suppl Fig. 1b). Similarly, patients with extramedullary tumors exhibited a worse OS rate, with a HR of 2.00 (95%CI 1.46–2.76) (Suppl Fig. 1c). In addition, patients with an FCI of 2/3 had a worse OS rate compared to those with an FCI of 0, with an HR of 1.98 (95%CI 1.43–2.72) (Suppl Fig. 1d).
Response rates
As first-line therapies, 604 patients received PI, 250 patients received a combination of PI and IMiD, 238 patients received IMiD alone, and 68 patients received conventional chemotherapies. Regarding overall response rates, including partial response (PR) or better and very good PR or better, the combination of PI and IMiD exhibited the highest rate (Fig. 3a). Notably, in both patient groups, those who received ASCT and those who did not receive ASCT, the combination regimens involving both PI and IMiD as the first-line therapy demonstrated better response rates compared to PI-based or IMiD-based regimens (Fig. 3b). Furthermore, ASCT-G showed higher rates of deeper responses represented by very good PR (VGPR) or better than non-ASCT-G regardless of the kinds of the induction regimens (Fig. 3b).
Progression free survival (PFS) and its prognostic factors
The 3-year progression-free survival (PFS) rate, which is one of the secondary endpoints of this study, was found to be 43.0% with a 95% CI of 40.2% to 45.8% (Fig. 4a). Among patients who received ASCT and those who did not, the 3-year PFS rates were 64.3% (95%CI 58.8–69.2%) and 34.0% (95%CI 30.8–37.3%), respectively (Fig. 4b). At a median follow-up of 4.5 years, the median PFS for all symptomatic PCN patients was 27.8 months (95%CI 24.8–30.4). In the ASCT group, the median PFS was 53.4 months (95%CI 44.6–65.0), whereas in the non-ASCT group, it was 19.9 months (95%CI 17.7–22.3). Tables 5 and 6 present the results of multivariable analysis. In the patient group who received ASCT, no factors were significantly associated with PFS. However, in the patient group who did not undergo ASCT, induction treatment with IMiD was associated with better PFS compared to conventional chemotherapy, with an HR of 0.70 (95%CI 0.50–0.97). As unfavorable prognostic factors, ISS 3 was found to be associated with poorer PFS compared to ISS 1, with an HR of 1.83 (95%CI 1.40–2.38) (Fig. 4c). In addition, the presence of extramedullary tumors was significantly associated with a worse PFS rate, with an HR of 1.87 (95%CI 1.42–2.46) (Fig. 4d).
OS and PFS analyses according to the cytogenetic risk category and revised-ISS (R-ISS)[14]
Among the 284 patients who received ASCT and had available baseline fluorescence in situ hybridization (FISH) data, the 3-year overall survival (OS) rate for 84 patients with high-risk cytogenetics carrying either t(4;14), t(14;16), or del(17p) was 84.3% with a 95% CI of 74.6% to 90.6%. In contrast, the 3-year OS rate for 200 patients with standard-risk cytogenetics was 93.2% (95%CI 88.6–96.0) (Suppl Fig. 2a). For the 654 patients who did not receive ASCT and had available baseline FISH data, the 3-year OS rate and median OS for 164 patients with high-risk cytogenetics were 49.7% (95%CI 41.6–57.2) and 35.4 months (95%CI 29.7–46.9), respectively. In comparison, the 3-year OS rate and median OS for 490 patients with standard-risk cytogenetics were 65.2% (95%CI 60.6–69.4) and 60.9 months (95%CI 49.4-NA) (Suppl Fig. 2b). Among the 256 patients who received ASCT and were categorized into revised International Staging System (ISS) based on baseline data, the 3-year OS rates were 92.9% (95%CI 82.1–97.3), 89.4% (95%CI 83.5–93.3), and 87.9% (95%CI 70.9–95.3) for stages 1, 2, and 3, respectively (Suppl Fig. 2c). For the 565 patients who did not receive ASCT and were categorized into revised ISS stages based on baseline data, the 3-year OS rates were 88.1% (95%CI 76.5–94.1), 64.7% (95%CI 59.2–69.6), and 41.4% (95%CI 33.2–49.5) for stages 1, 2, and 3, respectively (Suppl Fig. 2d).
Among the 282 patients who received ASCT and had available baseline FISH data, the 3-year PFS rate and median PFS for 83 patients with high-risk cytogenetics were 52.4% (95%CI 41.1–62.6) and 36.6 months (95%CI 26.8–55.7), respectively. In contrast, the 3-year PFS rate and median PFS for 199 patients with standard-risk cytogenetics were 72.8% (95%CI 65.9–78.6) and 65.0 months (95%CI 53.3-NA), respectively (Suppl Fig. 2e). For the 654 patients who did not receive ASCT and had available baseline FISH data, the 3-year PFS rate and median PFS for 164 patients with high-risk cytogenetics were 20.9% (95%CI 15.0–27.6) and 15.2 months (95%CI 11.8–17.5), respectively. In comparison, the 3-year PFS rate and median PFS for 490 patients with standard-risk cytogenetics were 38.6% (95%CI 34.1–43.1) and 23.5 months (95%CI 19.5–27.9), respectively (Suppl Fig. 2f).
Time to next treatment (TNT) and treatment free interval (TFI)
The median TNT for all symptomatic patients with PCN was 30.9 months with a 95% CI of 28.7 to 33.7 months. Among patients who received ASCT, the median TNT was 62.5 months (95%CI 53.4-NA), whereas for those who did not receive ASCT, it was 22.8 months (95%CI 20.7–25.5) (Fig. 5).
The median TFI for all symptomatic PCN patients was 1.2 months with a 95% CI of 1.0 to 1.4 months. Among patients who received ASCT, the median TFI was 2.8 months (95%CI 2.1–8.8), while for those who did not receive ASCT, it was 1.0 month (95%CI 0.8–1.1) (data not shown).
Discussion
In this prospective observational study conducted in Japan from 2016 to 2018, the overall survival (OS) rate of patients with PCN was found to be 70.0% at 3 years. This OS rate is consistent with data reported by Kumar SK, et al. from Mayo Clinic, Rochester, MN, USA [12]. In the Mayo Clinic study, they analyzed 1038 patients with newly diagnosed multiple myeloma (MM) between 2001 and 2010, grou** them into two 5-year periods: the 2001–2005 cohort and the 2006–2010 cohort. The OS rate at 3 years was 65% in the 2001–2005 cohort and 72% in the 2006–2010 cohort. Furthermore, the Mayo Clinic study also showed that the 3-year OS rate was 77% in patients receiving one of the novel drugs, such as thalidomide, lenalidomide, or bortezomib, as their initial therapy, compared to 67% in patients who did not receive these drugs. Similarly, in our cohort, until the approval of daratumumab for newly diagnosed MM in 2019, only bortezomib and lenalidomide among the novel drugs were approved for the patients with newly diagnosed MM. As a result, approximately 94% of the patients in our cohort received bortezomib and/or lenalidomide as their initial therapy, which contributed to achieving similar outcomes to that of the Mayo Clinic cohort in the 2006–2010 period. This study clearly demonstrates that the use of novel drugs has significantly improved the outcomes of Japanese patients with PCN.
The previous retrospective study of the real-world outcomes of Japanese patients with symptomatic MM reported by S. Ozaki et al. showed that the 3-year OS rates improved from 55% in the 1990–2000 cohort to 70% in the 2001–2012 cohort [8]. They also demonstrated that the 3-year OS rates were 70% in the patients receiving the novel drugs and 58% in the patients receiving the conventional chemotherapies alone in 2001–2012 cohort. In our current prospective study (2016–2018 cohort), we found a 3-year OS rate of 70.0% for patients with symptomatic PCN who received any kinds of treatment. Although there were differences in the median age (67 years and 71 years, respectively) and rates of patients receiving ASCT (32.3% and 27.1%, respectively) between the previous study and our current study, the 3-year OS rates at 3 years were similar. However, it is important to note that our current study enrolled patients prospectively from various kinds of hospitals, including those with general hematologists belonging to the Japanese Society of Hematology (JSH), representing a broader real-world population of symptomatic PCN patients. Based on this perspective, our current study’s findings suggest that the real-world outcomes of MM treatment have continued to improve further in 2016–2018 compared to the previous period (2001–2012). This improvement may be attributed to the wider availability and use of novel drugs in the treatment of symptomatic PCN patients during this study period.
Our study showed that the OS, PFS rates and TNT of patients who received ASCT showed better outcome. It possibly results from that many patients in ASCT-G achieved deeper responses. The DETERMINATION study’s results, which compared continuous therapy with a novel drug triplet regimen containing bortezomib, lenalidomide, and dexamethasone with upfront ASCT, demonstrated that continuous therapy did not show superior progression-free survival (PFS) despite showing similar overall survival (OS) [15]. This finding suggests that upfront ASCT remains a standard of care for transplant-eligible (TE) patients. On the other hand, daratumumab-containing therapies (D-MPB [daratumumab, melphalan, prednisolone plus bortezomib] and D-Ld [daratumumab, lenalidomide plus dexamethasone]) have shown more favorable PFS in transplant-ineligible (TIE) patients in the ALCYONE and MAIA studies [4, 6]. As these therapies become more widely used, the role of upfront ASCT may become less significant in the near future. The next prospective observational cohort study (JSH-MM-20) that started in Japan in January 2022 will provide further insights into the use of daratumumab-containing therapies in newly diagnosed MM patients and will help clarify the role of upfront ASCT in the context of evolving treatment options. Overall, ongoing research and clinical trials will continue to shape the treatment landscape for MM patients, and the role of upfront ASCT will be better understood in the context of novel drug therapies and patient selection criteria.
This study has revealed valuable insights into the factors influencing OS and PFS in patients with PCN, particularly those who did or did not receive upfront ASCT. Currently, upfront ASCT is one of the alternative choices for the patients aged 65–70 years as reported by a retrospective study conducted by Japanese Society of Myeloma and European Myeloma Network [16]. However, this study showed in patients who received upfront ASCT, the primary factor affecting OS was age. Specifically, the study found that patients aged 65 or older had an unfavorable OS, highlighting the need for careful patient selection when considering upfront ASCT, especially in elderly patients. This finding emphasizes the importance of considering age-related factors and potential treatment-related risks when deciding on treatment strategies for older MM patients. Conversely, in patients who did not receive ASCT, several risk factors were associated with unfavorable outcomes, including the treatment regimen of conventional chemotherapies, ISS stages 2/3, the presence of extramedullary tumors, and FCI stages 2/3. These factors did not include age in the group of patients who did not receive ASCT, indicating that other clinical factors play a more significant role in predicting OS in this subgroup. The study’s findings have important implications for clinical decision-making, especially when considering upfront ASCT as an alternative treatment choice for elderly patients, particularly those aged at 65 or older. The results underscore the need for a personalized and comprehensive assessment of individual patient characteristics, including age, comorbidities, disease stage, and treatment response, when determining the appropriateness of upfront ASCT. This approach ensures that the potential benefits of ASCT are balanced against the individual patient’s overall health status and potential risk factors.
It was confirmed that the use of novel drugs, particularly bortezomib and lenalidomide, as initial therapies has led to better ORR and improved OS compared to conventional chemotherapies in non-ASCT group. This improvement is noteworthy, even though the number of patients treated with conventional chemotherapies was limited. Among the novel drug options, the combination of bortezomib and lenalidomide emerged as particularly effective, as evidenced by the highest ORR and a deeper response with VGPR or higher. In non-ASCT group, it was observed that factors such as ISS stage 3 and the presence of extramedullary tumors were associated with unfavorable OS and PFS even in the era of novel drugs. This suggests that the current treatment approaches with bortezomib and/or lenalidomide may not be sufficient for these specific high-risk TIE patients. This highlights the need for alternative treatment strategies, such as incorporating daratumumab-containing therapies, such as D-MPB or D-Ld, which have shown more favorable results in the context of high-risk MM patients. In addition, the study’s findings emphasize that it’s not just chronological age, but comorbidities, that significantly influence OS in TIE patients. This suggests that older patients who are otherwise fit and without significant comorbidities can still benefit from bortezomib and/or lenalidomide-based regimens. Individualized treatment decisions based on a patient’s overall health status, beyond just age, are crucial for optimizing outcomes. While the study did not conduct a multivariable analysis for baseline prognostic factors related to FISH analyses due to the small number of patients, the mention of high-risk cytogenetics (such as t(4;14), t(14;16), or del(17p)) aligns with previous reports that these cytogenetic abnormalities can negatively impact both PFS and OS [17, 18]. This underscores the importance of develo** novel immune-based therapies, such as chimeric antigen receptor-T (CAR-T) cell therapy and bispecific antibodies, to address these high-risk cases and further improve treatment outcomes [19, 20]. Overall, this study identifies several areas where additional research and novel therapeutic approaches are needed to address the specific challenges faced by high-risk TIE patients with MM. This underscores the ongoing unmet need to improve treatment strategies for this patient population.
It’s clear that while this study provides valuable insights into the outcomes of patients with PCN, there are certain limitations that should be considered. One significant limitation is the lack of comprehensive safety data beyond the occurrence of second primary malignancies. Detailed safety data, adverse events, and the relative dose intensities of the drugs used could provide a more complete picture of the treatment landscape and potential challenges faced by patients. The observational nature of this study, with treatment decisions being based on physicians’ choice and the availability of national health insurance, introduces variability in the treatments and examinations received by patients. This variability can impact the comprehensiveness of data collected, such as the limited availability of baseline chromosomal analysis like FISH, which in turn affects the ability to conduct multivariable analyses. Despite these limitations, the study’s reliance on real-world data collected from a national survey is still highly valuable. This type of data is particularly important in rapidly evolving fields like multiple myeloma, where treatment strategies are continually changing due to the emergence of new therapies. Real-world data can provide insights into the effectiveness of these treatments in actual clinical practice, and it also enables international comparisons. The commitment to continuing this type of survey in collaboration with the Japanese Society of Hematology demonstrates a dedication to advancing the understanding of plasma cell neoplasms and improving patient outcomes. The approach of using real-world data to identify unresolved clinical questions and guide future research is an essential step toward refining treatment strategies and ultimately enhancing the prognosis of patients with these conditions.
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Acknowledgements
We express our gratitude to the patients and their families, as well as the physicians, nurses, study coordinators, and research staff, for their valuable participation in this study. We would like to extend our appreciation to Dr. Akiko Saito, Chief of the OSCR data center, and Ms. Maho Kawasaki, Ms. Risa Hioki, Ms. Emiko Nishioka, and Ms. Kumiko Agata for their assistance in data management. We would also like to acknowledge the contributions of Ms. Noriko Ito and Mr. Akihiro Sano from NHO Nagoya Medical Center for their support in statistical analysis. The funding for this study was provided by Chugai, Astellas, Abbvie, Kyowa Kirin, Shionogi, Sanofi, and Shire Japan.
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HS reports honoraria from Takeda, Ono, Fujimoto, Janssen, Chugai, Eisai, Sanofi, AstraZeneca, Meiji Seika Pharma, and AbbVie, research funding from Ono, Bristol Myers Squibb, and AbbVie. HH reports honoraria from Janssen, Bristol Myers Squibb, and Takeda, research funding from Bristol Myers Squibb and Takeda. AY reports honoraria from Kyowa Kirin, Chugai, Janssen, Sanofi, Bristol Myers Squibb, Eisai, Takeda, and Nippon-Shinyaku, research funding from Kyowa Kirin. SK reports honoraria from Eisai, Mundipharma, Chugai, Otsuka, Sanofi, Meiji Seika Pharma, AbbVie, Ono, Janssen, Takeda, Amgen, Novartis, and Nippon-Shinyaku. SO reports honoraria from Bristol Myers Squibb, Takeda, AstraZeneca, Janssen, and Sanofi. MY reports honoraria from Takeda, Sanofi, Novartis, Bristol Myers Squibb, Meiji Seika Pharma, and Daiichi Sankyo. SF reports honoraria from Takeda, Sanofi, Janssen, Ono, and Bristol Myers Squibb. TS reports honoraria from Ono, Otsuka, Eisai, SymBio, Takeda, Chugai, Sumitomo, Daiichi Sankyo, MSD, and PharmaEssentia. KM reports honoraria from Kyowa Kirin, Chugai, MSD, Tei** Pharma, Nippon-Shinyaku, Taiho, Takeda, Otsuka, Nippon Kayaku, Daiichi Sankyo, Sumitomo, Novartis, Pfizer, Celgene, Bristol Myers Squibb, Mochida, AbbVie, Alexion, Ono, Sanofi, Janssen, SymBio, AstraZeneca, CSL Bering, Amgen, Fujimoto, Eisai, Meiji Seika Pharma, Asahi Kasei, and Astellas, research funding from Kyowa Kirin, Chugai, MSD, Tei** Pharma, Nippon-Shinyaku, Taiho, Takeda, Otsuka, Nippon Kayaku, Daiichi Sankyo, and Sumitomo, advisory board fees from Bristol Myers Squibb, Novartis, and Otsuka, travel expense from Kyowa Kirin. HT reports honoraria from Sanofi, Ono, Janssen, Takeda, Bristol Myers Squibb, and Chugai, research funding from Asahi Kasei. MA reports honoraria from Takeda, Bristol Myers Squibb, Janssen, Sanofi, Ono, and Daiichi Sankyo. HI reports honoraria from Sanofi, SymBio, Janssen, Daiichi Sankyo, Chugai, Takeda, AstraZeneca, AbbVie, and Kyowa Kirin. JK reports honoraria from Janssen, Bristol Myers Squibb, Ono, Chugai, Takeda, Sanofi, and Kyowa Kirin, research funding from Kyowa Kirin, Mochida, Sanofi, Chugai, Bristol Myers Squibb, Takeda, and Ono, consulting fees from Janssen and Bristol Myers Squibb. HT reports honoraria from Janssen, Ono, Sanofi, and Bristol Myers Squibb, consulting fee from SRL, research funding from Bristol Myers Squibb. KS reports honoraria from Ono, Bristol Myers Squibb, Janssen, and Sanofi, research funding from Ono, Celgene, AbbVie, Takeda, Sanofi, Bristol Myers Squibb, GSK, Chugai, Otsuka, Janssen, MSD, Novartis, Pfizer, and Kyowa Kirin. MK reports honoraria from Bristol Myers Squibb, Novartis, Janssen, MSD, Nippon-Shinyaku, Ono, Takeda, and Sumitomo, research funding from Ono, Takeda, Kyowa Kirin, Chugai, and Daiichi Sankyo. TI reports honoraria from Takeda, Sanofi, Janssen, Bristol Myers Squibb, and Ono, research funding from Takeda, Pfizer, Sanofi, Janssen, and Bristol Myers Squibb. IM reports honoraria from Bristol Myers Squibb, Novartis, Otsuka, Pfizer, Janssen, Astellas, Takeda, Daiichi Sankyo, Ono, Chugai, AstraZeneca, SymBio, AbbVie, and Amgen, research funding from Ono, Janssen, Nippon-Shinyaku, Kyowa Kirin, Sumitomo, Shionogi, Tei** Pharma, Boehringer Ingelheim, Sanofi, Chugai, Eisai, MSD, Asahi Kasei, Astellas, Takeda, Nihon Pharma, Daiichi Sankyo, AbbVie, Taiho, Mitsubishi Tanabe, Nippon Kayaku, CSL Behring, Mundipharma, Ayumi Pharma, Eli Lilly Japan, Actelion Pharma, and Amgen, consulting fee from Otsuka. KA reports honoraria from AbbVie, Eisai, Ono, Kyowa Kirin, Chugai, Pfizer, Bristol Myers Squibb, and Janssen, research funding from Otsuka, Kyowa Kirin, Asahi Kasei, AbbVie, Chugai, and Takeda. SI reports honoraria from Janssen, Bristol Myers Squibb, Takeda, Sanofi, Ono, and Pfizer, research funding from Chugai, Janssen, Bristol Myers Squibb, Sanofi, Daiichi Sankyo, Pfizer, Celgene, Novartis, Ono, Takeda, Amgen, Shionogi, AbbVie, Otsuka, Kyowa Kirin, and GSK, advisory board fees from Janssen, Bristol Myers Squibb, Pfizer, Sanofi, AbbVie, Otsuka, Novartis, and Takeda. All the other authors have no conflicts of interest to disclose.
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Shibayama, H., Itagaki, M., Handa, H. et al. Primary analysis of a prospective cohort study of Japanese patients with plasma cell neoplasms in the novel drug era (2016–2021). Int J Hematol 119, 707–721 (2024). https://doi.org/10.1007/s12185-024-03754-8
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DOI: https://doi.org/10.1007/s12185-024-03754-8