Time-to-treatment of diffuse large B-cell lymphoma in
                    São Paulo

Xavier, Flávia Dias; Levy, Debora; Pereira, Juliana

doi:10.6061/clinics/2014(05)12

Abstract

OBJECTIVE:

Diffuse large B-cell lymphoma is the most common type of non-Hodgkin lymphoma, accounting for nearly 50% of the cases in the Hematology Department of the Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo and Instituto do Câncer do Estado de São Paulo. The treatment outcome is influenced by age, abnormal lactate dehydrogenase levels, extranodal infiltration, the disease stage and the patient's performance status. In this study, we sought to report the time-to-treatment of diffuse large B-cell lymphoma in São Paulo's public health system network and its impact on patient outcomes.

METHODS:

We prospectively followed a cohort of 42 consecutive patients with de novo diffuse large B-cell lymphoma between 2008 and 2012.

RESULTS:

Our patients had more advanced disease than that reported in the literature (61.9% vs. 46%). In São Paulo's public health system network, it took an average of 7.4 months for a diagnosis to be made and an additional 1.4 months to obtain an appointment with a specialist. Once at our Hematology Department, it took less than 20 days for staging, confirmation of the diagnosis and treatment initiation. An interval from signs or symptoms to treatment of more than 6 months was associated with inferior progression-free survival in 3 years (p = 0.049).

CONCLUSION:

A delay in the diagnosis of diffuse large B-cell lymphoma is a public health problem and may be associated with worse progression-free survival.

Lymphoma; Large B-Cell; Diffuse; Time-to-Treatment; Public Health; Diagnosis; Prognosis

Introduction

Non-Hodgkin lymphoma (NHL) is the ninth most common cancer type in Brazil and the thirteenth leading cause of cancer deaths (¹1. Instituto Nacional do Câncer. Available from: http://www1.inca.gov.br/vigilancia.
http://www1.inca.gov.br/vigilancia... ). Diffuse large B-cell lymphoma (DLBCL) is the most prevalent NHL subtype. This subtype comprises approximately 35% of all cases in the Western world (²2. Anderson JR, Armitage JO, Weisenburger DD. Epidemiology of the non-Hodgkin's lymphomas: distributions of the major subtypes differ by geographic locations. Non-Hodgkin's Lymphoma Classification Project. Annals of Oncology. 1998;9(7):717-20, http://dx.doi.org/10.1023/A:1008265532487.
http://dx.doi.org/10.1023/A:100826553248... ,³3. International Lymphoma Study Group. A clinical evaluation of the International Lymphoma Study Group classification of non-Hodgkin's lymphoma. The Non-Hodgkin's Lymphoma Classification Project. Blood. 1997;89(11):3909-18.) and accounts for nearly 50% of the cases in the Hematology Department of the Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo (Clinics Hospital of the Medical School of the University of São Paulo, hereafter referred to as “HC-FMUSP”) and Instituto do Câncer do Estado de São Paulo (Cancer Institute of the State of São Paulo, hereafter referred to as “ICESP”) (⁴4. Gouveia GR, Siqueira SAC, Chamone DAF, Pereira J. Prevalence of non-Hodgkin lymphomas in São Paulo, Brazil. Rev Bras Hematol Hemoter. 2011;33(4):317, http://dx.doi.org/10.5581/1516-8484.20110085.
http://dx.doi.org/10.5581/1516-8484.2011... ).

According to the World Health Organization's classification (⁵5. The International Agency for Research on Cancer. WHO Classification of Tumours of Haematopoietic and Lymphoid Tissue. 4th ed. Lyon; WHO Press; 2008. 310p.), the clinical and biological heterogeneity of DLBCL results in more than 20 subtypes. The condition is characterized by rapidly enlarging tumor masses, and 46% of patients present at advanced stages (⁶6. Armitage JO, Weisenburger DD. New Approach to Classifying Non-Hodgkin's Lymphomas: Clinical Features of the Major Histologic Subtypes. J Clin Oncol. 1998;16(8):2780-95.). We have recently demonstrated that this percentage can be as high as 61.9% in our department (⁷7. Xavier FD. Padrão de expressão e significado prognóstico dos genes BCL2, BCL6, CCND2, FN1, LMO2 e SCYA3 pela técnica de PCR em tempo real em linfoma difuso de grandes células B tratado com rituximabe [thesis]. São Paulo: Universidade de São Paulo; 2013. 162p.), possibly due to the difficulty in gaining access to a specialist in Brazil's health system network (SUS).

In this study, we report the time-to-treatment of DLBCL in São Paulo's public health system network and its impact on patient outcomes.

Materials and Methods

Patients from HC-FMUSP and ICESP with de novo CD20-positive DLBCL were consecutively enrolled from September 2008 to March 2010. Patients with immunosuppression-related lymphomas were not included. The participants were treated with R-CHOP-21 (rituximab 375 mg/m², cyclophosphamide 750 mg/m², doxorubicin 50 mg/m² and vincristine 1.4 mg/m² (maximum 2 mg) on day 1 and prednisone 100 mg/d for five days) (⁸8. Coiffier B, Lepage E, Briere J, Herbrecht R, Tilly H, Bouabdallah R, et al. CHOP chemotherapy plus rituximab compared with CHOP alone in elderly patients with diffuse large-B-cell lymphoma. N Engl J Med. 2002;346(4):235-42.,⁹9. Moreno A, Colon-Otero G, Solberg LA Jr. The prednisone dosage in the CHOP chemotherapy regimen for non-Hodgkin's lymphomas (NHL): is there a standard? Oncologist. 2000;5(3):238-49, http://dx.doi.org/10.1634/theoncologist.5-3-238.
http://dx.doi.org/10.1634/theoncologist.... ). A prospective follow-up of the cohort was performed until July 2012.

The onset of lymphoma-related symptoms or signs was defined as the first disease manifestation recognized by the patients. These manifestations were B symptoms (night sweats, unexplained fever above 38°C and/or unexplained weight loss above 10% of the total body weight over a period of 6 months), lymph node enlargement or a mass (palpable or discovered by imaging exams). These data were recorded during the first appointment of each patient by a hematologist. Time-to-treatment was defined as the interval between the first signs or symptoms and the beginning of treatment. This interval was divided into three steps: the time from first symptoms or signs until diagnosis by biopsy, the time from biopsy diagnosis until the first appointment with a hematologist and the time from the first appointment with a hematologist until the beginning of treatment. The staging and the response assessment were based on Cheson's revised response criteria for malignant lymphoma (¹⁰10. Cheson BD, Pfistner B, Juweid ME, Gascoyne RD, Specht L, Horninget SJ, et al. Revised response criteria for malignant lymphoma. J Clin Oncol. 2007;25(5):579-86, http://dx.doi.org/10.1200/JCO.2006.09.2403.
http://dx.doi.org/10.1200/JCO.2006.09.24... ). Overall survival was calculated as the time from diagnosis to the date of death or last follow-up, and the event was death. Progression-free survival was calculated as the time from diagnosis to the date of progression, relapse, last follow-up or death, and the events were progression and relapse. A univariate analysis of categorical variables was performed using the Mantel-Haenszel test. The Kaplan-Meier method was used to estimate overall survival and progression-free survival, and the log-rank test was used to compare survival curves. STATA 9.1 software was used for the data analysis. A p-value less than 0.05 was considered significant.

Ethics

The study was approved by the Ethics Committees of HC-FMUSP and ICESP. The clinical investigations were conducted according to the principles contained in the Declaration of Helsinki.

Results

A total of 42 patients were enrolled in the study, with a female predominance (60% vs. 40%) and a median age of 59.4 years (17-84 years). Most patients presented with advanced disease (61.9%). Less than one third of the patients showed the involvement of at least two extranodal sites, bulky disease and a performance status of two or higher based on Eastern Cooperative Oncology Group (ECOG) analysis. More than one half of the patients presented B symptoms or elevated serum lactate dehydrogenase (LDH) levels. Patients with a high-intermediate risk/high-risk International Prognostic Index (IPI) belonged to a poor Revised International Prognostic Index (RIPI) subgroup, representing 42.9% of the cases. The patients' characteristics are described in Table 1.

Thumbnail

Table 1
Characteristics of the cohort at diagnosis.

The mean and median times from the first lymphoma sign or symptom to the final diagnosis by biopsy were 7.42 months and 5.25 months, respectively (range: 0.57 to 28 months). The interval from pathological diagnosis to the first appointment with a hematologist in our department ranged from 0.5 to 5.7 months, and the mean and median times were 1.43 and 1.2 months, respectively.

In the Hematology Department of HC-FMUSP/ICESP, the average time interval between the first appointment and the start of treatment, encompassing diagnostic biopsy review; staging by physical examination; computed tomography of the neck, thorax, abdomen and pelvis; and positron emission tomography with fluorodeoxyglucose and bone marrow biopsy, was 20 days.

The time from the first sign or symptom to the start of treatment (TST) ranged from 2.17 to 29.4 months, with a mean of 9.3 months and a median of 6.4 months (Figure 1) (⁷7. Xavier FD. Padrão de expressão e significado prognóstico dos genes BCL2, BCL6, CCND2, FN1, LMO2 e SCYA3 pela técnica de PCR em tempo real em linfoma difuso de grandes células B tratado com rituximabe [thesis]. São Paulo: Universidade de São Paulo; 2013. 162p.).

Figure 1
Time between first signs or symptoms and commencement of DLBCL patients' treatment. Blue: Time from signs or symptoms to diagnostic biopsy. Red: Time from diagnostic biopsy to first appointment with a hematologist. Green: Time from first appointment with a hematologist (including image staging, bone marrow biopsy and diagnostic review) to treatment commencement.

The complete response rate was 82.5%, and the 3-year overall survival and progression-free survival were 82.8% (Figure 2) and 87.5%, respectively (⁷7. Xavier FD. Padrão de expressão e significado prognóstico dos genes BCL2, BCL6, CCND2, FN1, LMO2 e SCYA3 pela técnica de PCR em tempo real em linfoma difuso de grandes células B tratado com rituximabe [thesis]. São Paulo: Universidade de São Paulo; 2013. 162p.). In the univariate analysis, an interval from signs or symptoms to the beginning of treatment that exceeded 6 months was associated with inferior progression-free survival in 3 years (76.2% vs. 100%, p = 0.049) but not with inferior overall survival (72.1% vs. 93.3%, p = 0.13) (⁷7. Xavier FD. Padrão de expressão e significado prognóstico dos genes BCL2, BCL6, CCND2, FN1, LMO2 e SCYA3 pela técnica de PCR em tempo real em linfoma difuso de grandes células B tratado com rituximabe [thesis]. São Paulo: Universidade de São Paulo; 2013. 162p.) (Table 2).

Figure 2
Overall survival in DLBCL patients treated with R-CHOP at the Hematology Department of HC/ICESP-FMUSP.

Thumbnail

Table 2
Correlation between time-to-treatment and treatment outcomes.

Multivariate analysis by Cox logistic regression using the variables TST (≤6 or >6 months), performance status (<2 vs. ≥ 2), age (≤60 vs. >60 years), LDH levels (normal vs. elevated), extranodal sites (<2 vs. ≥2) and Ann Arbor clinical stage (I/II vs. III/IV) did not yield any independent variable for progression-free survival or overall survival in the entire group (Table 3). Multivariate analysis of TST (≤6 or >6 months) and IPI (low-risk plus low-intermediate-risk vs. high-intermediate-risk plus high-risk) and of TST (≤6 or >6 months) and RIPI (very good, good and poor) (Table 3) also did not reveal a correlation with prognosis. Because of the absence of a sufficient number of events in the good-risk group, we performed a survival analysis only in the poor-risk groups. Therefore, using only an IPI of intermediate-high/high-risk and a poor RIPI (all patients who had an intermediate-high/high risk IPI also had a poor RIPI), the survival curve obtained by log-rank analysis showed that a TST >6 months was an independent variable for progression-free survival (44.43% vs. 100%, p = 0.0184), with a tendency toward a lower overall survival rate (37.53% vs. 87.5%, p = 0.0617) (Table 2 and Figure 3).

Figure 3
Progression-free survival and overall survival in high-risk groups (an intermediate-high/high risk IPI or a poor RIPI).

Thumbnail

Table 3
Multivariate analysis by Cox logistic regression.

DISCUSSION

In Brazil, there have been no studies on NHL that have assessed the impact of delayed diagnosis and treatment on patients' survival. In our study, all DLBCL patients who did not respond to R-CHOP had waited more than 6 months from signs or symptoms to treatment, while just 54.55% of patients who exhibited a complete response were subjected to the same waiting period. An interval between signs or symptoms and treatment exceeding 6 months was statistically significantly associated with inferior progression-free survival in three years (100% vs. 76.2%, p = 0.049) (⁷7. Xavier FD. Padrão de expressão e significado prognóstico dos genes BCL2, BCL6, CCND2, FN1, LMO2 e SCYA3 pela técnica de PCR em tempo real em linfoma difuso de grandes células B tratado com rituximabe [thesis]. São Paulo: Universidade de São Paulo; 2013. 162p.). Although there was no significant difference in general overall survival, in the group with a high clinical risk (an intermediate-high/high IPI or a poor RIPI), there was a tendency toward a lower survival rate when the time-to-treatment was greater than 6 months (40% vs. 87.5%, p = 0.0617).

In the United Kingdom, the Review of Cancer Waiting Times Standards determined that (i) a patient with suspected cancer should be referred to a specialist for urgent evaluation within two weeks, (ii) the diagnosis should be made within one month and (iii) the total time-to-treatment should not be more than two months (¹¹11. Department of Health. Review of Cancer Waiting Times Standards. Improving Outcomes: A Strategy for Cancer. United Kingdom, 2011. Available from: https://www.gov.uk/government/uploads/system/uploads/attachment_data/file/135516/dh_123394.pdf.pdf.
https://www.gov.uk/government/uploads/sy... ).

On November 22, 2012, the Brazilian government enacted law n. 12.732 (which became enforceable only 180 days after its publication), which specifies a maximum period of 60 days from diagnosis to treatment of cancer patients by the SUS (¹²12. BRASIL. Lei n° 12732, de 22 de novembro de 2012. Dispõe sobre o primeiro tratamento de paciente com neoplasia maligna comprovada e estabelece prazo para seu início. Diário Oficial da União, Brasília, DF, 23 nov. 2012. Seção 1, p. 1.), closing the gap between Brazil and certain developed countries concerning the regulation of the timeline for cancer treatment.

On average, the period from diagnosis to treatment in our service is already very close to what the law specifies (a mean of 2.08 months), which is the result of the joint work of the Hematology, Pathology, Radiology, Surgery and Intensive Care Departments as well as the available resources and physical structure. Together, departments, resources and physical structure are responsible for our positive results: a 3-year overall survival of 82.8% (Figure 2) and a progression-free survival of 87.5% (⁷7. Xavier FD. Padrão de expressão e significado prognóstico dos genes BCL2, BCL6, CCND2, FN1, LMO2 e SCYA3 pela técnica de PCR em tempo real em linfoma difuso de grandes células B tratado com rituximabe [thesis]. São Paulo: Universidade de São Paulo; 2013. 162p.).

Nonetheless, there remains a delay of approximately 7.4 months to obtain a biopsy. The shortening of this time is paramount for the achievement of improved results. However, the timeframe preceding biopsy is not addressed by law 12.732, despite the fact that such a delay can be responsible for disease dissemination and the deterioration of a patient's performance status.

Due to the limited number of cases studied, we believe that our results should be confirmed in future studies. A public health bias likely contributed to our superior survival outcome; with a median of 6.4 months between symptoms/signs to the first appointment with a hematologist, most patients with aggressive lymphomas with worse biological features or poor clinical conditions are likely to die before being diagnosed or before meeting a hematologist. Solving this public bias could rescue these missing data and allow for more realistic statistics.

In conclusion, we understand that it is necessary to invest in health care training and the capacitation of primary and secondary health care assistance in Brazil to accelerate the discovery of lymphoma in patients. We also understand that it is equally important to establish the proceedings for the transfer of such patients to specialized centers.

References

¹
Instituto Nacional do Câncer. Available from: http://www1.inca.gov.br/vigilancia.
» http://www1.inca.gov.br/vigilancia
²
Anderson JR, Armitage JO, Weisenburger DD. Epidemiology of the non-Hodgkin's lymphomas: distributions of the major subtypes differ by geographic locations. Non-Hodgkin's Lymphoma Classification Project. Annals of Oncology. 1998;9(7):717-20, http://dx.doi.org/10.1023/A:1008265532487.
» http://dx.doi.org/10.1023/A:1008265532487
³
International Lymphoma Study Group. A clinical evaluation of the International Lymphoma Study Group classification of non-Hodgkin's lymphoma. The Non-Hodgkin's Lymphoma Classification Project. Blood. 1997;89(11):3909-18.
⁴
Gouveia GR, Siqueira SAC, Chamone DAF, Pereira J. Prevalence of non-Hodgkin lymphomas in São Paulo, Brazil. Rev Bras Hematol Hemoter. 2011;33(4):317, http://dx.doi.org/10.5581/1516-8484.20110085.
» http://dx.doi.org/10.5581/1516-8484.20110085
⁵
The International Agency for Research on Cancer. WHO Classification of Tumours of Haematopoietic and Lymphoid Tissue. 4th ed. Lyon; WHO Press; 2008. 310p.
⁶
Armitage JO, Weisenburger DD. New Approach to Classifying Non-Hodgkin's Lymphomas: Clinical Features of the Major Histologic Subtypes. J Clin Oncol. 1998;16(8):2780-95.
⁷
Xavier FD. Padrão de expressão e significado prognóstico dos genes BCL2, BCL6, CCND2, FN1, LMO2 e SCYA3 pela técnica de PCR em tempo real em linfoma difuso de grandes células B tratado com rituximabe [thesis]. São Paulo: Universidade de São Paulo; 2013. 162p.
⁸
Coiffier B, Lepage E, Briere J, Herbrecht R, Tilly H, Bouabdallah R, et al. CHOP chemotherapy plus rituximab compared with CHOP alone in elderly patients with diffuse large-B-cell lymphoma. N Engl J Med. 2002;346(4):235-42.
⁹
Moreno A, Colon-Otero G, Solberg LA Jr. The prednisone dosage in the CHOP chemotherapy regimen for non-Hodgkin's lymphomas (NHL): is there a standard? Oncologist. 2000;5(3):238-49, http://dx.doi.org/10.1634/theoncologist.5-3-238.
» http://dx.doi.org/10.1634/theoncologist.5-3-238
¹⁰
Cheson BD, Pfistner B, Juweid ME, Gascoyne RD, Specht L, Horninget SJ, et al. Revised response criteria for malignant lymphoma. J Clin Oncol. 2007;25(5):579-86, http://dx.doi.org/10.1200/JCO.2006.09.2403.
» http://dx.doi.org/10.1200/JCO.2006.09.2403
¹¹
Department of Health. Review of Cancer Waiting Times Standards. Improving Outcomes: A Strategy for Cancer. United Kingdom, 2011. Available from: https://www.gov.uk/government/uploads/system/uploads/attachment_data/file/135516/dh_123394.pdf.pdf.
» https://www.gov.uk/government/uploads/system/uploads/attachment_data/file/135516/dh_123394.pdf.pdf
¹²
BRASIL. Lei n° 12732, de 22 de novembro de 2012. Dispõe sobre o primeiro tratamento de paciente com neoplasia maligna comprovada e estabelece prazo para seu início. Diário Oficial da União, Brasília, DF, 23 nov. 2012. Seção 1, p. 1.

No potential conflict of interest was reported.

Publication Dates

Publication in this collection
2014

History

Received
27 Sept 2013
Reviewed
10 Oct 2013
Accepted
15 Oct 2013

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] ¹
Instituto Nacional do Câncer. Available from: http://www1.inca.gov.br/vigilancia.
» http://www1.inca.gov.br/vigilancia

[2] ²
Anderson JR, Armitage JO, Weisenburger DD. Epidemiology of the non-Hodgkin's lymphomas: distributions of the major subtypes differ by geographic locations. Non-Hodgkin's Lymphoma Classification Project. Annals of Oncology. 1998;9(7):717-20, http://dx.doi.org/10.1023/A:1008265532487.
» http://dx.doi.org/10.1023/A:1008265532487

[3] ³
International Lymphoma Study Group. A clinical evaluation of the International Lymphoma Study Group classification of non-Hodgkin's lymphoma. The Non-Hodgkin's Lymphoma Classification Project. Blood. 1997;89(11):3909-18.

[4] ⁴
Gouveia GR, Siqueira SAC, Chamone DAF, Pereira J. Prevalence of non-Hodgkin lymphomas in São Paulo, Brazil. Rev Bras Hematol Hemoter. 2011;33(4):317, http://dx.doi.org/10.5581/1516-8484.20110085.
» http://dx.doi.org/10.5581/1516-8484.20110085

[5] ⁵
The International Agency for Research on Cancer. WHO Classification of Tumours of Haematopoietic and Lymphoid Tissue. 4th ed. Lyon; WHO Press; 2008. 310p.

[6] ⁶
Armitage JO, Weisenburger DD. New Approach to Classifying Non-Hodgkin's Lymphomas: Clinical Features of the Major Histologic Subtypes. J Clin Oncol. 1998;16(8):2780-95.

[7] ⁷
Xavier FD. Padrão de expressão e significado prognóstico dos genes BCL2, BCL6, CCND2, FN1, LMO2 e SCYA3 pela técnica de PCR em tempo real em linfoma difuso de grandes células B tratado com rituximabe [thesis]. São Paulo: Universidade de São Paulo; 2013. 162p.

[8] ⁸
Coiffier B, Lepage E, Briere J, Herbrecht R, Tilly H, Bouabdallah R, et al. CHOP chemotherapy plus rituximab compared with CHOP alone in elderly patients with diffuse large-B-cell lymphoma. N Engl J Med. 2002;346(4):235-42.

[9] ⁹
Moreno A, Colon-Otero G, Solberg LA Jr. The prednisone dosage in the CHOP chemotherapy regimen for non-Hodgkin's lymphomas (NHL): is there a standard? Oncologist. 2000;5(3):238-49, http://dx.doi.org/10.1634/theoncologist.5-3-238.
» http://dx.doi.org/10.1634/theoncologist.5-3-238

[10] ¹⁰
Cheson BD, Pfistner B, Juweid ME, Gascoyne RD, Specht L, Horninget SJ, et al. Revised response criteria for malignant lymphoma. J Clin Oncol. 2007;25(5):579-86, http://dx.doi.org/10.1200/JCO.2006.09.2403.
» http://dx.doi.org/10.1200/JCO.2006.09.2403

[11] ¹¹
Department of Health. Review of Cancer Waiting Times Standards. Improving Outcomes: A Strategy for Cancer. United Kingdom, 2011. Available from: https://www.gov.uk/government/uploads/system/uploads/attachment_data/file/135516/dh_123394.pdf.pdf.
» https://www.gov.uk/government/uploads/system/uploads/attachment_data/file/135516/dh_123394.pdf.pdf

[12] ¹²
BRASIL. Lei n° 12732, de 22 de novembro de 2012. Dispõe sobre o primeiro tratamento de paciente com neoplasia maligna comprovada e estabelece prazo para seu início. Diário Oficial da União, Brasília, DF, 23 nov. 2012. Seção 1, p. 1.

Characteristic	No.	(%)
Male	17	(40)
Age (median)	59.4 (17-84)
>60 years	21	(50)
Ann Arbor stage
I/II	16	(38.1)
III/IV	26	(61.9)
≥ 2 extranodal sites	12	(28.6)
Bulky (≥ 10 cm)	12	(28.6)
ECOG performance status ≥ 2	11	(26.2)
B symptoms	23	(54.8)
High serum LDH level	22	(52.4)
Low serum albumin level	4	(9.5)
Unknown	2	(04.8)
High serum β2-microglobulin level	25	(59.5)
Unknown	14	(33.3)
IPI
Low risk/Low-intermediate risk	15/9	(35.7)/(21.4)
High-intermediate risk/High risk	10/8	(23.8)/(19.1)
RIPI
Very good risk	5	(11.9)
Good risk	19	(45.2)
Poor risk	18	(42.9)

TST (months)	N (%)	CR	3-year PFS		3-year OS
		p-value ^* *Significant at p<0.05.	(%)	p-value ^* *Significant at p<0.05.	(%)	p-value ^* *Significant at p<0.05.
>3		0.5518		0.439		0.688
No	4 (10.8)		100		75
Yes	33 (89.2)		84.4		81.5
>3 (intermediate-high/high IPI or poor RIPI subgroup¹ 1The patients' distribution was the same for an intermediate-high/high IPI and a poor RIPI. ,² 2Low-risk subgroup analysis was not possible because there was no event (relapse, disease progression or death) in this group. )		-		0.2995		0.9186
No	3 (16.7)		100		66.7
Yes	15 (83.3)		66.7		60,0
>6		0.8650		0.049		0.133
No	15 (16.7)		100		93.3
Yes	22 (59.5)		76.2		72.1
>6 (intermediate-high/high IPI or poor RIPI subgroup¹ 1The patients' distribution was the same for an intermediate-high/high IPI and a poor RIPI. ,² 2Low-risk subgroup analysis was not possible because there was no event (relapse, disease progression or death) in this group. )		-		0.0184		0.0617
No	8 (44.4)		100		87.5
Yes	10 (55.6)		44.4³ 32.8-year PFS.		37.5³ 32.8-year PFS.

Variable	PFS	OS
	p-value ^* *Significant at p<0.05.	p-value ^* *Significant at p<0.05.
TST (>6 or ≤6 months)	1.00	0.13
Performance status (≥2 vs. <2)	0.60	0.22
Age (≤60 vs. >60 years)	0.75	0.91
Lactate dehydrogenase level (normal vs. elevated)	1.00	^ Variables were excluded because of the absence of an event in patients with normal lactate dehydrogenase levels or Ann Arbor clinical stage I/II.
Extranodal sites (≥2 vs. <2)	0.59	0.36
Ann Arbor stage (I/II vs. III/IV)	1.00	^ Variables were excluded because of the absence of an event in patients with normal lactate dehydrogenase levels or Ann Arbor clinical stage I/II.
TST (>6 or ≤6 months)	1.00	0.09
IPI (low-intermediate risk plus low risk vs. intermediate-high risk plus high risk)	1.00	1.00
TST (>6 or ≤6 months)	1.00	0.09
RIPI (very good, good or poor)	1.00	1.00

Brasil

Brasil

Time-to-treatment of diffuse large B-cell lymphoma in São Paulo

Abstract

OBJECTIVE:

METHODS:

RESULTS:

CONCLUSION:

Introduction

Materials and Methods

Ethics

Results

DISCUSSION

References

Publication Dates

History