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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02178475
Other study ID # 20120214
Secondary ID
Status Completed
Phase
First received
Last updated
Start date July 18, 2014
Est. completion date October 28, 2016

Study information

Verified date October 2017
Source Amgen
Contact n/a
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

To estimate the incidence of febrile neutropenia in patients with breast cancer and non-Hodgkin's lymphoma receiving high (> 20%) FN-risk chemotherapy and pegfilgrastim primary prophylaxis.


Recruitment information / eligibility

Status Completed
Enrollment 943
Est. completion date October 28, 2016
Est. primary completion date October 28, 2016
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Age = 18 years old.

- Any stage NHL or breast cancer and received the first cycle of a new chemotherapy course.

- Received the first cycle of a permitted standard dose chemotherapy regimens with an estimated high (> 20%) FN risk according to published data or guidelines (dose modifications +/-10% in Cycle 1 are allowable).

- Initiated treatment in Cycle 1 with pegfilgrastim according to the pegfilgrastim summary of product characteristics. (SmPC). Enrolment must occur after the first pegfilgrastim dosing in Cycle 1 and before the second day of Cycle 2.

Exclusion Criteria:

- Ongoing or planned concurrent participation in any clinical study involving Investigational Product that has not been approved by the national competent authorities for any indication.

- Ongoing or planned concurrent participation in any clinical study where the administration of Colony Stimulating Factor (CSF) is determined by the protocol (clinical trials on an approved drug and observational trials are permitted as long as these do not mandate how neutropenia should be treated).

Study Design


Locations

Country Name City State
Austria Research Site Eggenburg
Austria Research Site Graz
Austria Research Site Leoben
Austria Research Site Schwarzach im Pongau
Austria Research Site Wien
Austria Research Site Wien
Belgium Research Site Arlon
Belgium Research Site Liege
Belgium Research Site Liège
Bulgaria Research Site Pleven
Bulgaria Research Site Sofia
Czechia Research Site Chomutov
Czechia Research Site Horovice
Czechia Research Site Novy Jicin
Czechia Research Site Plzen
Czechia Research Site Praha 10
Czechia Research Site Praha 2
France Research Site Aix en Provence
France Research Site Amiens
France Research Site Beuvry
France Research Site Marseille
France Research Site Marseille cedex 5
France Research Site Meaux Cedex
France Research Site Nancy
France Research Site Nimes cedex 09
France Research Site Orleans Cedex
France Research Site Périgueux cedex
France Research Site Perpignan
France Research Site Pierre Benite Cedex
France Research Site Saint Priest en Jarez Cedex
France Research Site Sarcelles
France Research Site Strasbourg
Germany Research Site Bonn
Germany Research Site Dresden
Germany Research Site Fulda
Germany Research Site Hildesheim
Germany Research Site Kassel
Germany Research Site Stolberg
Germany Research Site Troisdorf
Germany Research Site Velbert
Germany Research Site Westerstede
Greece Research Site Athens
Greece Research Site Athens
Greece Research Site Athens
Greece Research Site Chania
Greece Research Site Kalamata
Greece Research Site Larissa
Greece Research Site Nea Kifissia, Athens
Greece Research Site Papagou
Greece Research Site Piraeus
Greece Research Site Thessaloniki
Greece Research Site Thessaloniki
Greece Research Site Thessaloniki
Greece Research Site Thessaloniki
Poland Research Site Bialystok
Poland Research Site Gdynia
Poland Research Site Koszalin
Poland Research Site Krakow
Poland Research Site Krakow
Poland Research Site Poznan
Poland Research Site Walbrzych
Poland Research Site Warszawa
Poland Research Site Warszawa
Romania Research Site Baia Mare
Romania Research Site Braila
Romania Research Site Bucharest
Romania Research Site Bucharest
Romania Research Site Bucharest
Romania Research Site Bucuresti
Romania Research Site Bucuresti
Romania Research Site Campina
Romania Research Site Cluj-Napoca
Romania Research Site Iasi
Romania Research Site Oradea
Romania Research Site Ploiesti

Sponsors (1)

Lead Sponsor Collaborator
Amgen

Countries where clinical trial is conducted

Austria,  Belgium,  Bulgaria,  Czechia,  France,  Germany,  Greece,  Poland,  Romania, 

Outcome

Type Measure Description Time frame Safety issue
Primary Percentage of Participants With Febrile Neutropenia Febrile neutropenia (FN) was defined as an absolute neutrophil count (ANC) of < 0.5 x 10^9/L, or < 1.0 x 10^9/L predicted to fall below 0.5 x 10^9/L within 48 hours with fever or clinical signs of sepsis; fever and ANC were measured the same day or within ± 1 calendar day. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Participants Who Discontinued Pegfilgrastim Prophylaxis Participants who discontinued pegfilgrastim prophylaxis was defined as participants who received at least one cycle of chemotherapy (cycle 2 or later) in which pegfilgrastim prophylaxis was not administered, but other granulocyte colony-stimulating factor (G-CSF) prophylaxis was administered. Participants in this group received either pegfilgrastim or other G-CSF prophylaxis in all chemotherapy cycles.
Discontinuation was categorized as either temporary (participant received pegfilgrastim prophylaxis in at least one subsequent cycle) or permanent (participant had at least one cycle of chemotherapy following the cycle in which no pegfilgrastim prophylaxis was administered, and other G-CSF prophylaxis (i.e. not pegfilgrastim) was administered in all subsequent cycles, OR participant did not receive pegfilgrastim prophylaxis in the last cycle of chemotherapy, and other G-CSF prophylaxis was administered).
Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Participants Who Discontinued G-CSF Prophylaxis Participants who discontinued G-CSF prophylaxis was defined as participants who received at least one cycle of chemotherapy (cycle 2 or later) in which no G-CSF prophylaxis was administered.
Discontinuation was categorized as either temporary (participant received G-CSF prophylaxis in at least one subsequent cycle) or permanent (participant had at least one cycle of chemotherapy following the cycle in which no G-CSF prophylaxis was administered, and no G-CSF prophylaxis was administered in any subsequent cycle, OR participant did not receive G-CSF prophylaxis in the last cycle of chemotherapy).
Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Characteristics of Participants Who Discontinued Pegfilgrastim Prophylaxis Participants who discontinued pegfilgrastim prophylaxis are participants who received at least one cycle of chemotherapy (cycle 2 or later) in which pegfilgrastim prophylaxis was not administered, but other G-CSF prophylaxis was administered in this cycle. Participants in this group received either pegfilgrastim or other G-CSF prophylaxis in all chemotherapy cycles.
Data includes both temporary and permanent pegfilgrastim discontinuation.
Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Characteristics of Participants Who Discontinued G-CSF Prophylaxis Participants who discontinued G-CSF prophylaxis are participants who received at least one cycle of chemotherapy (cycle 2 or later) in which no G-CSF prophylaxis was administered.
Data includes both temporary and permanent discontinuation of G-CSF prophylaxis.
Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Cycles With No Pegfilgrastim Prophylaxis A cycle of chemotherapy (cycle 2 or later) in which pegfilgrastim prophylaxis was not administered, but other G-CSF prophylaxis was administered in this cycle. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Cycles With no G-CSF Prophylaxis A cycle of chemotherapy (cycle 2 or later) in which no G-CSF prophylaxis was administered. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Reasons for Discontinuation of Pegfilgrastim Prophylaxis Participants who discontinued pegfilgrastim prophylaxis are participants who received at least one cycle of chemotherapy (cycle 2 or later) in which pegfilgrastim prophylaxis was not administered, but other G-CSF prophylaxis was administered in this cycle. Participants in this group received either pegfilgrastim or other G-CSF prophylaxis in all chemotherapy cycles.
Data includes both temporary and permanent pegfilgrastim discontinuation.
Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Reasons for Discontinuation of G-CSF Prophylaxis Participants who discontinued G-CSF prophylaxis are participants who received at least one cycle of chemotherapy (cycle 2 or later) in which no G-CSF prophylaxis was administered.
Data includes both temporary and permanent discontinuation of G-CSF prophylaxis. Participants may have more than 1 discontinuation reason.
Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Percentage of Participants Who Experienced Complications of Febrile Neutropenia Complications of febrile neutropenia were defined as FN-related hospitalizations and death, and neutropenia-related chemotherapy dose delays and dose reductions. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Febrile Neutropenia Events That Occurred During Cycles With No G-CSF Prophylaxis The number of febrile neutropenia events that occurred during a cycle of chemotherapy (cycle 2 or later) in which no G-CSF prophylaxis was administered. Febrile neutropenia was defined as an ANC of < 0.5 x 10^9/L, or < 1.0 x 10^9/L predicted to fall below 0.5 x 10^9/L within 48 hours with fever or clinical signs of sepsis; fever and ANC were measured the same day or within ± 1 calendar day. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Participants Who Experienced Febrile Neutropenia During Cycles With No G-CSF Prophylaxis The number of participants who received at least one cycle of chemotherapy in which no G-CSF prophylaxis was administered who experienced febrile neutropenia during a cycle of chemotherapy in which no G-CSF prophylaxis was administered. Febrile neutropenia was defined as an ANC of < 0.5 x 10^9/L, or < 1.0 x 10^9/L predicted to fall below 0.5 x 10^9/L within 48 hours with fever or clinical signs of sepsis; fever and ANC were measured the same day or within ± 1 calendar day. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Participants Who Experienced Complications of Febrile Neutropenia During Cycles With No G-CSF Prophylaxis The number of participants who received at least one cycle of chemotherapy in which no G-CSF prophylaxis was administered who experienced complications of febrile neutropenia during a cycle of chemotherapy in which no G-CSF prophylaxis was administered. Complications of febrile neutropenia were defined as FN-related hospitalizations and death, and neutropenia-related chemotherapy dose delays and dose reductions. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Cycles With No G-CSF Prophylaxis in Which Febrile Neutropenia Events Occurred The number of chemotherapy cycles during which an event of febrile neutropenia occurred in which no G-CSF prophylaxis was administered. Febrile neutropenia was defined as an ANC of < 0.5 x 10^9/L, or < 1.0 x 10^9/L predicted to fall below 0.5 x 10^9/L within 48 hours with fever or clinical signs of sepsis; fever and ANC were measured the same day or within ± 1 calendar day. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Cycles With No G-CSF Prophylaxis in Which Complications of Febrile Neutropenia Occurred The number of chemotherapy cycles during which complications of febrile neutropenia occurred in which no G-CSF prophylaxis was administered. Complications of febrile neutropenia were defined as FN-related hospitalizations and death, and neutropenia-related chemotherapy dose delays and dose reductions. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Number of Participants Who Permanently Switched From Pegfilgrastim Prophylaxis to Other G-CSF Prophylaxis The number of participants who received pegfilgrastim prophylaxis from cycle 1 until a cycle when other G-CSF prophylaxis was administered, and this G-CSF or a different G-CSF agent (not pegfilgrastim) was received as prophylaxis at each remaining cycle of the chemotherapy course. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
Secondary Characteristics of Participants Who Received On-schedule Pegfilgrastim Primary Prophylaxis On-schedule pegfilgrastim primary prophylaxis was defined as participants who received pegfilgrastim in cycle 1 and continued to receive pegfilgrastim across all cycles, administered 1-3 days after the end of cytotoxic chemotherapy in each cycle. Participants were followed for up to 8 cycles of chemotherapy; the average observation time was 4.1 months.
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