Advanced search
Publication Cover
Journal of Blood Medicine Volume 10, 2019 - Issue
Submit an article Journal homepage
124
Views
2
CrossRef citations to date
0
Altmetric
Original Research

Lenograstim and filgrastim in the febrile neutropenia prophylaxis of hospitalized patients: efficacy and cost of the prophylaxis in a retrospective survey

Rolando Innocenti1 Hematology Department, University of Florence and AOU Careggi, Florence, Italy, [email protected]
,
Luigi Rigacci1 Hematology Department, University of Florence and AOU Careggi, Florence, Italy, [email protected];2 Hematology Unit and Bone Marrow Transplant Unit, San Camillo Forlanini Hospital, Rome, Italy, [email protected]Correspondence[email protected]
,
Umberto Restelli3 Center for Health Economics, Social and Health Care Management, LIUC – Università Cattaneo, Castellanza (VA), Italy;4 School of Public Health, Faculty of Health Sciences, University of the Witwatersrand, Johannesburg, South Africa
,
Barbara Scappini1 Hematology Department, University of Florence and AOU Careggi, Florence, Italy, [email protected]
,
Giacomo Gianfaldoni1 Hematology Department, University of Florence and AOU Careggi, Florence, Italy, [email protected]
,
Rosa Fanci1 Hematology Department, University of Florence and AOU Careggi, Florence, Italy, [email protected]
,
Francesco Mannelli1 Hematology Department, University of Florence and AOU Careggi, Florence, Italy, [email protected]
,
Francesca Scolari3 Center for Health Economics, Social and Health Care Management, LIUC – Università Cattaneo, Castellanza (VA), Italy
,
Davide Croce3 Center for Health Economics, Social and Health Care Management, LIUC – Università Cattaneo, Castellanza (VA), Italy;4 School of Public Health, Faculty of Health Sciences, University of the Witwatersrand, Johannesburg, South Africa
,
Erminio Bonizzoni5 Section of Medical Statistics and Biometry “GA Maccacaro”, Department of Clinical Science and Community, University of Milan, Milan, Italy
,
Tania Perrone6 Medical Affairs Department, Italfarmaco SpA, Milan, Italy
&
Alberto Bosi1 Hematology Department, University of Florence and AOU Careggi, Florence, Italy, [email protected]
 show all
Pages 21-27 | Published online: 27 Dec 2018

Abstract

Purpose

We conducted a retrospective study to evaluate the efficacy and related costs of using two different molecules of granulocyte-colony stimulating factor (G-CSF) (lenograstim – LENO or filgrastim – FIL) as primary prophylaxis of chemotherapy-induced neutropenia in a hematological inpatient setting.

Methods

The primary endpoints of the analysis were the efficacy of the two G-CSFs in terms of the level of white blood cells, hemoglobin and platelets at the end of the treatment and the per capita direct medical costs related to G-CSF prophylaxis.

Results

Two hundred twelve patients (96 LENO, 116 FIL) have been evaluated. The following statistically significant differences have been observed between FIL and LENO: the use of a higher number of vials (11 vs 7; P<0.03) to fully recover bone marrow, a higher grade 3–4 neutropenia at the time of G-CSF discontinuation (29.3% vs 16.7%; P=0.031) and an increased number of days of hospitalization (8 vs 5; P<0.005). A longer hospital stay before discharge was necessary (12 vs 10), which reflects the higher final costs per patient (median treatment cost per cycle 10.706 € for LENO, compared to 12.623 € for FIL).

Conclusion

The use of LENO has been associated with a lower number of days of hospitalization, number of vials and less incidence of grade 3–4 neutropenia at the time of G-CSF discontinuation. LENO seems to be cost-saving when compared with FIL (–15.2%).

View correction statement:
Lenograstim and filgrastim in the febrile neutropenia prophylaxis of hospitalized patients: efficacy and cost of the prophylaxis in a retrospective survey [Corrigendum]

Introduction

The occurrence of neutropenia is a frequent complication for patients who undergo cytostatic chemotherapy for the treatment of a malignant hematological disease or a solid tumor, and when fever occurs (febrile neutropenia), it is considered as a severe complication.Citation1 The frequency of neutropenia and its severity, as well as the probability of febrile neutropenia, are related to the scheme of chemotherapy used, malignancy and patient-specific factors (gender, age, presence of concomitant diseases and general health status);Citation1,Citation2 in most cases, febrile neutropenia indicates a severe infection.Citation3 Its incidence is between 80% and 90% in patients affected with acute myeloid leukemia and about 50% in patients with solid tumors.Citation4Citation6 Whether febrile neutropenia is associated with infection or not is one of the principal causes of hospitalization, which can lead to high follow-up costs.Citation7Citation9 Prophylaxis with recombinant granulocyte-colony stimulating factor (G-CSF) is recommended to prevent febrile neutropenia and associated secondary events such as infections.Citation1,Citation2 Current guidelines recommend primary prophylactic administration of G-CSF during the first chemotherapy cycle (and hence all subsequent cycles) when the risk of febrile neutropenia is over 20%.Citation1,Citation2 The risk assessment should be performed before each cycle, since the risk constellation for febrile neutropenia may change during treatment.Citation1,Citation2

Currently, 4 original G-CSF molecules are commercially available in the European Union (EU) and Italy: filgrastim (FIL), lenograstim (LENO) and pegfilgrastim (PEG), as well as lipegfilgrastim, which is the most recently available preparation; moreover, various filgrastim biosimilars are available, whereas no biosimilars exist for LENO and PEG.Citation10Citation12

However, the active ingredients differ in their dosage, duration of use, available strength, package size and price.Citation13,Citation14 PEG is administered in a standardized 6 mg dose, once per chemotherapy, an active ingredient amount equivalent to individual doses of 30 million units of daily G-CSF for 11 consecutive days.Citation15Citation17

LENO, unlike FIL and PEG, is a glycosylated form of G-CSF. Glycosylation increases the receptor affinity of the protein to the corresponding receptor, creates a higher plasma half-life and confers temperature resistance (no need for refrigeration).Citation18 In vitro studies have demonstrated that granulocytes primed with filgrastim show a lower functionality and a less mature phenotype compared with those primed with glycosylated G-CSF.Citation19Citation21 From a clinical point of view, lenograstim demonstrated a lower incidence of febrile episodes compared to filgrastim; a higher number of patients achieved the target dose of CD34+ cells during mobilization of autologous stem cells and in a slightly shorter time, reducing the duration of neutropenia.Citation22Citation24 The dose of LENO and FIL is patient specific, which is calculated based on body weight and administered daily until neutrophil counts recover.Citation25 In outpatient treatment, this goal is achieved after an average of 5–6 days for LENO,Citation26 while for some patients, a longer duration of G-CSF has been prescribed (maximum of 10–11 days).Citation25,Citation26 The individual dose required and the frequency of G-CSF administration, in one chemotherapy cycle, have been considered the only determining factors in the cost of G-CSF prophylaxis per cycle.

Assuming that a clinical difference between LENO and FIL could also be observed in the hospital setting, we decided to conduct a retrospective study to evaluate the efficacy and related costs of using LENO or FIL as primary prophylaxis of chemotherapy-induced neutropenia in a hematological inpatient setting.

Patients and methods

In the Hematological Department of Careggi Hospital, Florence (Tuscany, Italy), a retrospective comparative study has been carried out to evaluate two different cohorts of patients: one treated with LENO (from 2009 to 2011) and one with FIL (from 2012 to 2014). From 2009 until the end of 2011, LENO was the only G-CSF available in the hospital, while from January 2012, due to an expenditure restraint, the bio-similar form of FIL replaced the glycosylated G-CSF.

Data sources and resources

Since 2008, medical records have been converted into electronic documents and the following inclusion criteria have been considered to recover patient data in the electronic database: patients affected by hematological malignancies and who were admitted to the hospital for the administration of chemotherapy regimens and required G-CSF prophylaxis. The main exclusion criteria were hospitalization, mobilization of autologous stem cell or other concomitant illness different from chemotherapy administration, which requires G-CSF prophylaxis. Our retrospective database analysis has been conducted in accordance with the Declaration of Helsinki, and informed consent was not required due to the anonymous and retrospective design of the data collection. The analysis has been notified to the ethical committee of Careggi Hospital that received and approved the study.

Endpoint

The primary endpoints of the analysis were the efficacy of the two G-CSFs in terms of the level of white blood cells (WBCs), hemoglobin and platelet at the end of the treatment and the per capita direct medical costs related to G-CSF prophylaxis.

It is therefore important to isolate the variables directly related to the use of the two drugs considered (LENO vs FIL/ biosimilar). In this way, it is possible to assess which of the two alternatives would lead to a lower use of hospital resources. We considered direct medical costs (from 2014) related to G-CSF infusion, including drug cost, the personnel directly involved in the medicine’s infusion and consumables and inpatient stay costs, assuming the hospital authority’s point of view.

The cost per infusion was calculated through a micro-costing approach, which was identified through an interview with a Key Opinion Leader, the input resources needed for a standard infusion and the related costs (VAT inclusive) collected within the hospital accounting service. The only variable cost between the two cohorts was that of the drug. The total cost per infusion was 55.9 € for LENO and 22.3 € for FIL (biosimilar), inclusive of drug cost, consumables and human resources.

Due to lack of data from Careggi Hospital, where the analysis was performed, the cost per day of hospitalization in 2014 was estimated considering the data published by the Italian Ministry of Economy and Finance in relation to the average inpatient day cost in Italy and Tuscany in 2004 discounting the values using the Italian annual average inflation rates (International Monetary Fund, 2016), which were 839 € and 1,031 €, respectively.

The direct medical costs per patient were assessed taking into consideration the number of G-CSF infusions administered and the number of inpatient days after starting the treatment with growth factor until discharge.

The collected and analyzed data do not allow a detailed analysis on the real absorption of resources linked to each individual patient (in terms of outpatient services performed during hospitalization, etc.), therefore different statistical index positions were considered in relation to the variables considered: median values for the number of vials used in the two cohorts (LENO vs FIL/biosimilar) and for inpatient days.

To assess the variability of the results, the same evaluation was conducted by considering the first and third quartiles for the number of days of inpatient stay and the number of vials.

Statistical methods

Demographic characteristics were examined according to qualitative or quantitative data. In general, demographic qualitative data were summarized using absolute frequencies and percentages and analyzed using the chi-squared test, while quantitative data were summarized using medians and ranges and analyzed using an unpaired independent t-test. Comparisons between treatments with respect to the times to bone marrow recovery and times from recovery to hospital discharge were performed using a log-rank test with associated event-free curves reported in graphs using the Kaplan–Meier approach. Comparisons between treatments with respect to the number of vials were performed using the Wilcoxon rank sum test. A two-sided test with a P-value less than or equal to 0.05 was considered statistically significant. Computations were performed using SAS software, version 9.2.

Results

A total of 212 patients have been included in the analysis: 96 treated with LENO (Myelostim) and 116 with FIL (Tevagrastim); the median age was 52 and 54, respectively. Leukemia was the predominant disease, 69.8% and 60.3% in the LENO and FIL cohort, respectively. During hospitalization, nearly all patients received antibiotic and antifungal prophylaxis. The patients’ characteristics are reported in .

Table 1 Description of patients’ characteristics

A significantly higher number of FIL vials than LENO vials (11 vs 7; P<0.03) were necessary to obtain the full bone marrow recovery and thus caused an increase in the number of days with high risk for infection in neutropenic patients (8 vs 5; P<0.005). Moreover, a higher number of days before hospital discharge were necessary in patients treated with FIL compared with those treated with LENO (12 vs 10), as reported in , which reflects the higher final cost per patient.

Table 2 Description of G-CSF activity

A statistically significant difference has been detected between LENO and FIL in terms of grade 3–4 neutropenia at the time of discontinuation (29.3% vs 16.7%, P=0.031; ). No differences were observed among patients treated with FIL or LENO in terms of final efficacy (bone marrow recovery; ). A significant hematological toxicity associated with the type of G-CSF was similar in terms of all grades of WBC, hemoglobin and platelet recovery (P=0.70, P=0.70 and P=0.58, respectively), thus reflecting no differences in the completion of chemotherapy and toxic death.

Figure 1 Grade of neutropenia at the time of G-CSF discontinuation in lenograstim and filgrastim cohort.

Abbreviation: G-CSF, granulocyte-colony stimulating factor.
Figure 1 Grade of neutropenia at the time of G-CSF discontinuation in lenograstim and filgrastim cohort.

Figure 2 Kaplan–Meier plot of percentage of patients with bone marrow recovery at the time (days) of G-CSF discontinuation (lenograstim or filgrastim).

Abbreviation: G-CSF, granulocyte-colony stimulating factor.
Figure 2 Kaplan–Meier plot of percentage of patients with bone marrow recovery at the time (days) of G-CSF discontinuation (lenograstim or filgrastim).

shows the average cost of patients treated with FIL/biosimilar and LENO, using the median days of treatment with growth factor at discharge and the number of vials, the cost data of daily hospitalization presented in the patients and methods section, and data obtained using the first and third quartiles.

Table 3 Cost per patient in the lenograstim and filgrastim groups and percentage difference

The use of LENO instead of FIL would lead to a decrease of direct medical costs related to inpatient stay and infusions considering median values, with a cost (€) per patient (using inpatient costs data from Tuscany) of 10,706 and of 12,623, respectively, and with a cost (€) per patient (using inpatient costs data from Italy) of 8,777 and of 10,309, respectively. The use of LENO would lead to cost decreases of –15.2% and –14.9%.

The data from the first quartile for the number of vials used per patient and inpatient stay show a further decrease of costs due to the use of LENO, leading to cost decreases of –31.6% and –31.3% (using data from Tuscany and Italy, respectively). The data from the third quartile show an increase of costs of 8.3% and of 8.8% (using data from Tuscany and Italy, respectively).

Discussion

The chemotherapy regimen is one of the primary determinants of the risk of neutropenia, given that some regimens are more myelotoxic than others,Citation3 and this is one of the most relevant causes of morbidity and mortality.Citation8,Citation9 Febrile neutropenia remains a life-threatening medical condition, despite the wide availability of effective antibiotics.Citation8,Citation9

It frequently causes significant hospitalization costs when developed by patients treated with chemotherapy.Citation27,Citation28 These costs include both direct medical costs and indirect costs that are borne by the patient and caregivers.

The administration of G-CSF decreases the incidence of febrile neutropenia and allows the maintenance of a correct dose density and intensity.Citation1,Citation2 It is also important to underline the fact that completion of all planned chemotherapy cycles is essential in order to provide patients with the maximum chance of treatment success,Citation29,Citation30 and febrile neutropenia may cause dose reduction and treatment delay limiting the efficacy of therapy.Citation29,Citation30

It has been clearly established that in patients receiving myelotoxic chemotherapy regimens, prophylaxis with a G-CSF, the primary regulator of granulopoiesis, decreases the occurrence of febrile neutropenia.Citation1,Citation2

Three original G-CSF preparations are commercially available in the EU and Italy: LENO, FIL and its biosimilars, PEG,Citation31 as well as lipegfilgrastim, which is the most recently available preparation.

Despite the fact that all the G-CSFs are reported as similar, considerable evidence has been published indicating that there are chemical, biological and clinical differences between glycosylated and non-glycosylated (pegylated and non-pegylated) molecules.Citation32

According to international guidelines, in settings characterized by a high risk of febrile neutropenia (20% or more), prophylaxis with G-CSF is indicatedCitation1,Citation2 starting at 24–48 hours after chemotherapy. The number of injections and the duration of prophylaxis are still a matter of debate, and we know that the onset and the duration of nadir are key points to establish the starting day and duration of G-CSF administration after chemotherapy.Citation3

A shorter schedule seems to decrease the incidence and severity of side effects, is cost saving and more effective.Citation33Citation36 In addition, a large survey by Falandry et alCitation26 indicates that the required duration of daily G-CSF administration is significantly shorter than recommended in guidelines, namely, 5.5 days, whereas only 9.3% of the patients exceed 7 days. Possible explanations for the discrepancies between guidelines and clinical practice could be that guidelines are often based on studies designed to ascertain the efficacy of G-CSF vs placebo, regardless of proper timing and duration.

In our study, a significantly higher number of FIL vials than LENO vials have been necessary to fully recover bone marrow depletion, with a significant difference between the two G-CSF in terms of grade 3–4 neutropenia at the time of G-CSF discontinuation, 29.3% vs 16.7%, P=0.031. The delay in bone marrow recovery increased the days of hospitalization in patients treated with FIL compared with those treated with LENO (12 days vs 10 days).

Despite the higher cost per vial of LENO with respect to FIL/biosimilar, the median direct medical costs per treatment (drug, infusion and inpatient stay) in patients with neutropenia were lower due to a lower use of vials to resolve neutropenia and due to the reduction of inpatient stay.

The median treatment cost per cycle, in terms of infusions and inpatient stay, amounted to 10.706 € for LENO, compared to 12.623 € for FIL/biosimilar, considering data for inpatient stay from Tuscany (the region where the hospital in which the analysis was performed is located), with a difference of –15.2%. The identification of LENO as a cost-saving G-CSF compared with FIL in Italy is in line with other published cost comparisons.Citation37,Citation38

Conclusion

The use of LENO has been associated with a lower number of days of hospitalization, number of vials and less incidence of grade 3–4 neutropenia at the time of G-CSF discontinuation. LENO seems to be cost-saving compared to FIL.

The economic analysis performed is to be considered conservative due to the lack of quantification of the costs associated with the management of drugs (purchase, storage and handling), which in the case of FIL/biosimilar are likely to be higher due to the need for storage at a low temperature. Future prospective economic evaluations should consider the collection of all direct medical costs and assume a societal perspective to assess indirect costs related to patients and caregivers.

Acknowledgments

The authors thank the nurses of the Hematology Department of AOU Careggi Firenze.

Disclosure

TP is an employee of Italfarmaco SpA; UR declares personal fees from Italfarmaco SpA and Bayer SpA outside the present work. The other authors report no other conflicts of interest in this work.

References

  • AaproMSBohliusJCameronDA2010 update of EORTC guidelines for the use of granulocyte-colony stimulating factor to reduce the incidence of chemotherapy-induced febrile neutropenia in adult patients with lymphoproliferative disorders and solid tumoursEur J Cancer201147183221095116
  • SmithTJKhatcheressianJLymanGH2006 update of recommendations for the use of white blood cell growth factors: an evidence-based clinical practice guidelineJ Clin Oncol200624193187320516682719
  • RiaRRealeAMoschettaMDammaccoFVaccaANeutropenia and G-CSF in lymphoproliferative diseasesHematology201318313113723321273
  • BodeyGPBuckleyMSatheYSFreireichEJQuantitative relationships between circulating leukocytes and infection in patients with acute leukemiaAnn Intern Med19666423283405216294
  • ChangHYRodriguezVNarboniGBodeyGPLunaMAFrei-reichEJCauses of death in adults with acute leukemiaMedicine19765532592681063911
  • CherpillodAPétignatCLeyvrazSInfectious complications during chemotherapy for solid tumorsClin Microbiol Infect1997332911864129
  • LinkHMaschmeyerGMeyerPStudy Group of the Paul Ehrlich Society for ChemotherapyInterventional antimicrobial therapy in febrile neutropenic patientsAnn Hematol1994692312437948312
  • KudererNMDaleDCCrawfordJCoslerLELymanGHMortality, morbidity, and cost associated with febrile neutropenia in adult cancer patientsCancer2006106102258226616575919
  • KudererNMDaleDCCrawfordJLymanGHImpact of primary prophylaxis with granulocyte colony-stimulating factor on febrile neutropenia and mortality in adult cancer patients receiving chemotherapy: a systematic reviewJ Clin Oncol200725213158316717634496
  • WelteKG-CSF: filgrastim, lenograstim and biosimilarsExpert Opin Biol Ther201414798399324707817
  • YangBBSavinMAGreenMPrevention of chemotherapy-induced neutropenia with pegfilgrastim: pharmacokinetics and patient outcomesChemotherapy201258538739823296266
  • BennettCLDjulbegovicBNorrisLBArmitageJOColony-stimulating factors for febrile neutropenia during cancer therapyN Engl J Med2013368121131113923514290
  • KubotaNOritaTHattoriKOh-EdaMOchiNYamazakiTStructural characterization of natural and recombinant human granulocyte colony-stimulating factorsJ Biochem199010734864921692828
  • CrawfordJCasertaCRoilaFESMO Guidelines Working GroupHematopoietic growth factors: ESMO clinical practice guidelines for the applicationsAnn Oncol201021Suppl 5v248v25120555091
  • HolmesFAJonesSEO’ShaughnessyJComparable efficacy and safety profiles of once-per-cycle pegfilgrastim and daily injection filgrastim in chemotherapy-induced neutropenia: a multicenter dose-finding study in women with breast cancerAnn Oncol200213690390912123336
  • HolmesFAO’ShaughnessyJAVukeljaSBlinded, randomized, multicenter study to evaluate single administration pegfilgrastim once per cycle versus daily filgrastim as an adjunct to chemotherapy in patients with high-risk stage II or stage III/IV breast cancerJ Clin Oncol200220372773111821454
  • GreenMDKoelblHBaselgaJA randomized double-blind multicenter phase III study of fixed-dose single-administration pegfilgrastim versus daily filgrastim in patients receiving myelosuppressive chemotherapyAnn Oncol2003141293512488289
  • ChamoreyALMagnéNPivotXImpact of glycosylation on the effect of cytokines. A special focus on oncologyEur Cytokine Netw201213154160
  • RibeiroDVeldwijkMRBennerADifferences in functional activity and antigen expression of granulocytes primed in vivo with filgrastim, lenograstim, or pegfilgrastimTransfusion200747696998017524085
  • KopfBde GiorgiUVertogenBA randomized study comparing filgrastim versus lenograstim versus molgramostim plus chemotherapy for peripheral blood progenitor cell mobilizationBone Marrow Transplant200638640741216951690
  • AtaerginSArpaciFTuranMReduced dose of lenograstim is as efficacious as standard dose of filgrastim for peripheral blood stem cell mobilization and transplantation: a randomized study in patients undergoing autologous peripheral stem cell transplantationAm J Hematol200883864464818508321
  • OrciuoloEBudaGMarturanoELenograstim reduces the incidence of febrile episodes, when compared with filgrastim, in multiple myeloma patients undergoing stem cell mobilizationLeuk Res201135789990321134693
  • RiaRGasparreTMangialardiGComparison between filgrastim and lenograstim plus chemotherapy for mobilization of PBPCsBone Marrow Transplant201045227728119584820
  • RiaRRealeAMelaccioARacanelliVDammaccoFVaccaAFilgrastim, lenograstim and pegfilgrastim in the mobilization of peripheral blood progenitor cells in patients with lymphoproliferative malignanciesClin Exp Med201515214515024722996
  • SwansonGBergstromKStumpEMiyaharaTHerfindalETGrowth factor usage patterns and outcomes in the community setting: collection through a practice-based computerized clinical information systemJ Clin Oncol20001881764177010764438
  • FalandryCCamponeMCartronGGuerinDFreyerGTrends in G-CSF use in 990 patients after EORTC and ASCO guidelinesEur J Cancer201046132389239820732287
  • GómezHHidalgoMCasanovaLRisk factors for treatment-related death in elderly patients with aggressive non-Hodgkin’s lymphoma: results of a multivariate analysisJ Clin Oncol1998166206520699626205
  • LymanGHLymanCHAgboolaORisk models for predicting chemotherapy-induced neutropeniaOncologist200510642743715967836
  • BoslyABronDvan HoofAAchievement of optimal average relative dose intensity and correlation with survival in diffuse large B-cell lymphoma patients treated with CHOPAnn Hematol200887427728317952688
  • PettengellRSchwenkglenksMLeonardRImpact of Neutropenia in Chemotherapy-European Study Group (INC – EU): neutropenia occurrence and predictors of reduced chemotherapy delivery: results from the INC – EU prospective observational European neutropenia studySupport Care Cancer2008161299130918351398
  • GuarigliaRMartorelliMCLeroseRTelescaDMilellaMRMustoPLipegfilgrastim in the management of chemotherapy-induced neutropenia of cancer patientsBiologics201610101826858523
  • KeatingGMLenograstim: a review of its use in chemotherapy-induced neutropenia, for acceleration of neutrophil recovery following haematopoietic stem cell transplantation and in peripheral blood stem cell mobilizationDrugs20111671667970721504247
  • PapaldoPLopezMMarollaPImpact of five prophylactic filgrastim schedules on hematologic toxicity in early breast cancer patients treated with epirubicin and cyclophosphamideJ Clin Oncol200523286908691816129844
  • HendlerDRizelSYerushalmiRDifferent schedules of granulocyte growth factor support for patients with breast cancer receiving adjuvant dose-dense chemotherapy: a prospective nonrandomized studyAm J Clin Oncol201134661962421217400
  • WolffACJonesRJDavidsonNEJeterSCStearnsVMyeloid toxicity in breast cancer patients receiving adjuvant chemotherapy with pegfilgrastim supportJ Clin Oncol2006241523922394
  • PotoskyALMalinJLKimBUse of colony-stimulating factors with chemotherapy: opportunities for cost savings and improved outcomesJ Natl Cancer Inst20111031297998221670423
  • HadjiPKostevKSchröder-BernhardiDZillerVCost comparison of outpatient treatment with granulocyte colony-stimulating factors (G-CSF) in GermanyInt J Clin Pharmacol Ther201250428128922456299
  • PfannkucheMSGlaeskeGNeyeHKostenvergleiche für Arzneimittel auf der Basis von DDD im Rahmen der Vertragsärztlichen Versorgung. [Advantages and Limitations of the DDD System in the Context of the German statutory Health Insurance System]Gesundh Ökon Qual Manag20091411723 German
Download PDF

Related research

People also read lists articles that other readers of this article have read.

Recommended articles lists articles that we recommend and is powered by our AI driven recommendation engine.

Cited by lists all citing articles based on Crossref citations.
Articles with the Crossref icon will open in a new tab.