KIT+ GIST

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KIT+ GIST

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Response rates for KIT+ GIST

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GLEEVEC^® significantly improves recurrence-free survival^1,2,*

9 out of 10 patients remained recurrence free with GLEEVEC^2,*

Adjuvant therapy with GLEEVEC demonstrated a significant difference in recurrence-free survival (RFS) versus placebo (P<0.0001).¹

*With a median follow-up of 14 months (range, 0 to ~54 months).^1,2

Evaluate and discuss the risk of recurrence in your patients with KIT–positive gastrointestinal stromal tumors (KIT+ GIST) to make an informed treatment decision
Level of risk tolerance will vary by patient
Note that the adjuvant GLEEVEC clinical trial examined tumors ≥3 cm in size¹

Cytopenias have been reported. Complete blood counts should be performed weekly for the first month, biweekly for the second month, and periodically thereafter as clinically indicated (eg, every 2-3 months). Dose reduction, treatment interruption, or in rare cases discontinuation of treatment may be required for severe neutropenia or thrombocytopenia (see full Prescribing Information for dose adjustment recommendations).

Serious adverse reactions to GLEEVEC^® (imatinib mesylate)
Fluid retention and edema Patients should be weighed and monitored regularly for signs and symptoms of edema or serious fluid retention. Severe fluid retention was reported in 9% to 13.1% of patients with KIT+ GIST. If severe fluid retention occurs, manage with diuretic therapy and withhold GLEEVEC until the event has resolved and then resume depending on the initial severity of the event
Hematologic toxicity Cytopenias, including anemia, neutropenia, and thrombocytopenia, have been reported. Complete blood counts should be performed as indicated
Severe congestive heart failure and left ventricular dysfunction Patients with cardiac disease or risk factors for cardiac failure should be monitored carefully. Patients with signs or symptoms should be evaluated and treated
Hepatotoxicity Severe hepatotoxicity, including fatalities, may occur with both short-term and long-term use. Assess liver function before initiation of treatment and monitor monthly thereafter or as clinically indicated. Dose adjustments or drug interruption may be required
Hemorrhage In Phase 3 unresectable or metastatic GIST studies, 12.9% of patients reported NCI Grades 3/4 hemorrhage at any site. In the Phase 2 unresectable or metastatic GIST study, 5% of patients reported severe gastrointestinal (GI) and/or intratumoral bleeds. GI tumor sites may have been the source of GI bleeds
Gastrointestinal disorders GLEEVEC should be taken with food and a large glass of water to minimize possible GI irritation. There have been rare reports, including fatalities, of GI perforation
Hypereosinophilic cardiac toxicity In patients with hypereosinophilic syndrome and cardiac involvement, cardiogenic shock and left ventricular dysfunction have been associated with initiation of GLEEVEC. The condition was reported to be reversible with the administration of systemic steroids, circulatory support measures, and temporary withholding of GLEEVEC
Dermatologic toxicities Bullous dermatologic reactions, including erythema multiforme and Stevens-Johnson syndrome, have been reported
Hypothyroidism Hypothyroidism has been reported in thyroidectomy patients undergoing levothyroxine replacement during treatment with GLEEVEC. TSH levels should be closely monitored
Toxicities from long-term use Consider potential toxicities-specifically liver, kidney, and cardiac toxicity-and immunosuppression
Growth retardation in children and pre-adolescents Growth retardation has been reported. Long-term effects on growth are unknown, therefore monitoring is recommended
Tumor lysis syndrome Cases of tumor lysis syndrome (TLS), including fatal cases, have been reported. Patients with tumors having a high proliferative rate or high tumor burden prior to treatment should be monitored closely for TLS and appropriate precautions taken

More than double the number of recurrence events occurred in the placebo arm compared with the GLEEVEC arm (HR=0.398 [95% CI: 0.259, 0.610], P<0.0001)^1,2

Only 30 events (8.4%) occurred in the GLEEVEC arm (n=359)^1,2
70 events (19.8%) occurred in the placebo arm (n=354)^1,2

400 mg/day is the recommended dose for adjuvant therapy.¹

In the adjuvant treatment of GIST trials (GLEEVEC; placebo), severe (NCI Grades 3 and above) lab abnormalities—increase in liver enzymes (ALT) (3%; 0%), (AST) (2%; 0%), decreased neutrophil count (3%; 1%), and decrease in hemoglobin (1%; 0%)—and severe adverse reactions (NCI Grades 3 and above), including abdominal pain (3%; 1%), diarrhea (3%; 1%), rash (3%; 0%), fatigue (2%; 1%), nausea (2%; 1%), vomiting (2%; 1%), white blood cell count decreased (1%; 0%), and periorbital edema (1%; 0%) were reported among patients receiving adjuvant treatment with GLEEVEC.

The rate of tumor recurrence increased after stopping adjuvant therapy with GLEEVEC³

GLEEVEC may be continued in the absence of progression or unacceptable toxicity¹

There is no treatment restriction based on tumor size¹
The optimal treatment duration with GLEEVEC in the adjuvant setting is unknown¹
In the adjuvant clinical study, GLEEVEC was administered for 1 year in patients with tumor size ≥3 cm¹
Ongoing trials in the adjuvant setting are focusing on duration of benefit for continuing GLEEVEC

Provide proven efficacy with GLEEVEC^®¹

The majority of patients achieved a response in phase 3 metastatic trials¹

*Two open-label, randomized, multinational phase 3 studies (SWOG [Southwest Oncology Group] Study S0033 and EORTC [European Organisation for Research and Treatment of Cancer] Study STSBG62005) were designed to compare response rates, progression-free survival (PFS), and overall survival (OS) between 400 mg/day and 800 mg/day imatinib in patients with unresectable and/or metastatic malignant KIT–positive gastrointestinal stromal tumors (KIT+ GIST) (N=1640). Response rate included complete response (CR) and partial response (PR).¹

Adequate time must be allowed for response to GLEEVEC¹

Median time to response was 12 weeks (range, 3-98 weeks).

GLEEVEC provides durable responses with up to 2 years of progression-free survival (PFS) at the 800-mg/day dose¹

About 80% of patients benefited from treatment when administered a starting dose of 400 mg/day^4,*
Dose escalation to 800 mg/day is permitted in patients with unresectable and/or metastatic KIT+ GIST showing clear signs or symptoms of disease progression at a lower dose¹
Adverse reactions were similar across both dosages in the metastatic trials with the exception of edema and rash/related terms¹
- Incidence of both was higher in the 800-mg/day arm versus the 400-mg/day arm (86% vs 77% for edema and 50% vs 38% for rash/related terms)
Patients who tolerated the 400-mg dose prior to dose escalation were less likely to require dose reductions at the 800-mg level than patients initiated at the higher dose⁴

Three hundred forty-seven patients (42.4%) crossed over to the 800-mg/day arm following disease progression in phase 3 trials; these patients had a 3.4-month median and 7.7-month mean exposure to GLEEVEC following crossover¹
Long-term median OS was observed even in patients who crossed over to 800 mg/day due to disease progression⁴
Doses of 400 mg should be administered once daily, whereas a dose of 800 mg should be administered as 400 mg twice a day¹

Prematurely switching patients to another targeted therapy is not recommended by the NCCN³

Switching from GLEEVEC is recommended in the primary treatment of KIT+ GIST only if life-threatening side effects occur that cannot be managed by maximum supportive care³
Continuing GLEEVEC treatment at the same or an increased dose as tolerated is recommended in cases of limited or generalized progression³
Please note that in some cases, dose adjustments, drug interruptions, or drug discontinuation may be necessary due to hematologic adverse reactions, hepatotoxicity, and other nonhematologic adverse events¹

Fight disease progression with GLEEVEC 800 mg/day¹

Continuing GLEEVEC treatment at same or increased dose as tolerated is recommended in cases of limited or generalized progression³

Dose escalation to GLEEVEC 800 mg daily is the standard of care for patients experiencing focal and multifocal progression on 400-mg therapy^3,5

Review dosing for KIT+ GIST

Adverse reactions were similar across both dosages in the metastatic trials with the exception of edema and rash/related terms¹
- Incidence of both was higher in the 800-mg/day arm versus the 400-mg/day arm (86% vs 77% for edema and 50% vs 38% for rash/related terms)
Patient noncompliance and drug interactions should be ruled out as causes of progression⁶

Please see Important Safety Information and full Prescribing Information.

¹GLEEVEC^® (imatinib mesylate) tablets prescribing information. East Hanover, NJ: Novartis Pharmaceuticals Corporation; April 2011.

²DeMatteo RP, Ballman KV, Antonescu CR, et al; American College of Surgeons Oncology Group (ACOSOG) Intergroup Adjuvant GIST Study Team. Adjuvant imatinib mesylate after resection of localised, primary gastrointestinal stromal tumour: a randomised, double-blind, placebo-controlled trial. Lancet. 2009;373(9669):1097-1104.

³The NCCN Soft Tissue Sarcoma Clinical Practice Guidelines in Oncology (Version 1.2011). National Comprehensive Cancer Network Web site. http://www.nccn.org. Accessed April 1, 2011.

⁴Patel S, Zalcberg JR. Optimizing the dose of imatinib for treatment of gastrointestinal stromal tumours: lessons from the phase 3 trials. Eur J Cancer. 2008;44(4):501-509.

⁵Reichardt P, Blay JY, Mehren M. Towards global consensus in the treatment of gastrointestinal stromal tumor. Expert Rev Anticancer Ther. 2010;10(2):221-232.

⁶Casali PG, Jost L, Reichardt P, Schlemmer M, Blay JY; ESMO Guidelines Working Group. Gastrointestinal stromal tumours: ESMO clinical recommendations for diagnosis, treatment and follow-up. Ann Oncol. 2009;(20 suppl 4):64-67.

Serious adverse reactions to GLEEVEC^® (imatinib mesylate)
Fluid retention and edema Patients should be weighed and monitored regularly for signs and symptoms of edema or serious fluid retention. Severe fluid retention was reported in 9% to 13.1% of patients with KIT+ GIST. If severe fluid retention occurs, manage with diuretic therapy and withhold GLEEVEC until the event has resolved and then resume depending on the initial severity of the event
Hematologic toxicity Cytopenias, including anemia, neutropenia, and thrombocytopenia, have been reported. Complete blood counts should be performed as indicated
Severe congestive heart failure and left ventricular dysfunction Patients with cardiac disease or risk factors for cardiac failure should be monitored carefully. Patients with signs or symptoms should be evaluated and treated
Hepatotoxicity Severe hepatotoxicity, including fatalities, may occur with both short-term and long-term use. Assess liver function before initiation of treatment and monitor monthly thereafter or as clinically indicated. Dose adjustments or drug interruption may be required
Hemorrhage In Phase 3 unresectable or metastatic GIST studies, 12.9% of patients reported NCI Grades 3/4 hemorrhage at any site. In the Phase 2 unresectable or metastatic GIST study, 5% of patients reported severe gastrointestinal (GI) and/or intratumoral bleeds. GI tumor sites may have been the source of GI bleeds
Gastrointestinal disorders GLEEVEC should be taken with food and a large glass of water to minimize possible GI irritation. There have been rare reports, including fatalities, of GI perforation
Hypereosinophilic cardiac toxicity In patients with hypereosinophilic syndrome and cardiac involvement, cardiogenic shock and left ventricular dysfunction have been associated with initiation of GLEEVEC. The condition was reported to be reversible with the administration of systemic steroids, circulatory support measures, and temporary withholding of GLEEVEC
Dermatologic toxicities Bullous dermatologic reactions, including erythema multiforme and Stevens-Johnson syndrome, have been reported
Hypothyroidism Hypothyroidism has been reported in thyroidectomy patients undergoing levothyroxine replacement during treatment with GLEEVEC. TSH levels should be closely monitored
Toxicities from long-term use Consider potential toxicities—specifically liver, kidney, and cardiac toxicity—and immunosuppression
Growth retardation in children and pre-adolescents Growth retardation has been reported. Long-term effects on growth are unknown, therefore monitoring is recommended
Tumor lysis syndrome Cases of tumor lysis syndrome (TLS), including fatal cases, have been reported. Patients with tumors having a high proliferative rate or high tumor burden prior to treatment should be monitored closely for TLS and appropriate precautions taken

Serious adverse events may occur with GLEEVEC

Fetal harm can occur when administered to a pregnant woman. Therefore, women of reproductive potential should be advised not to become pregnant while taking GLEEVEC tablets and to avoid breastfeeding while taking GLEEVEC because of the potential for serious adverse reactions in nursing infants. Sexually active female patients taking GLEEVEC should use highly effective contraception. If the patient does become pregnant while taking GLEEVEC, the patient should be advised of the potential hazard to the fetus
Motor vehicle accidents involving patients receiving imatinib have been reported. Caution should be recommended when driving a car or operating machinery

Low discontinuation rate due to adverse reactions

Crossover from 400 mg/day to 800 mg/day is feasible, particularly in patients able to tolerate the standard dose
Only 5.4% of patients at both dosage levels (400 mg/day and 800 mg/day) discontinued due to adverse reactions
Edema, fatigue, nausea, abdominal pain, diarrhea, rash, vomiting, myalgia, anemia, and anorexia were the most frequently reported adverse reactions

Adverse events were similar across both dosages with the exception of edema and rash/related terms

Patients with adverse reactions where frequency was ≥15% in any one group (full analysis set) in the Phase 3 unresectable and/or metastatic malignant GIST clinical trials.

Click here for the full GLEEVEC Prescribing Information and for complete list of adverse reactions.

Help your patients manage mild-to-moderate adverse events

Supportive care may help reduce the severity of some adverse reactions, whereas other adverse reactions require discontinuation or dosage adjustment

GLEEVEC^® (imatinib mesylate) tablets are indicated for:

Newly diagnosed adult and pediatric patients with Philadelphia chromosome-positive chronic myeloid leukemia (Ph+ CML) in the chronic phase
Patients with Ph+ CML in blast crisis (BC), accelerated phase (AP), or in the chronic phase (CP) after failure of interferon-alpha therapy
Adult patients with relapsed or refractory Philadelphia chromosome–positive acute lymphoblastic leukemia (Ph+ ALL)
Adult patients with myelodysplastic/myeloproliferative diseases (MDS/MPD) associated with PDGFR (platelet-derived growth factor receptor) gene rearrangements
Adult patients with aggressive systemic mastocytosis (ASM) without the D816V c-KIT mutation or c-KIT mutational status unknown
Adult patients with hypereosinophilic syndrome (HES) and/or chronic eosinophilic leukemia (CEL) who have FIP1L1-PDGFRα fusion kinase (mutational analysis or FISH demonstration of CHIC2 allele deletion) and for patients with HES and/or CEL who are FIP1L1-PDGFRα fusion kinase negative or unknown
Adult patients with unresectable, recurrent, and/or metastatic dermatofibrosarcoma protuberans (DFSP)
Patients with KIT (CD117)-positive unresectable and/or metastatic malignant gastrointestinal stromal tumors (GIST)
Adjuvant treatment of adult patients following complete gross resection of KIT (CD117)- positive GIST

Important Safety Information

GLEEVEC is often associated with edema and, occasionally, serious fluid retention. Severe fluid retention was reported in 9%-13.1% and 2.5%-11% of patients taking GLEEVEC for GIST and CML, respectively. Patients should be weighed and monitored regularly for signs and symptoms of fluid retention, which can be serious or life threatening, and be advised to report any rapid, unexpected weight gain. The probability of edema tended to be increased among older patients (>65 years) or those taking higher doses of GLEEVEC. Severe edema and superficial edema was observed in 182 (11.1%) GIST patients and 1.5%-6% in CML patients, respectively. If severe fluid retention occurs, manage with diuretic therapy and withhold GLEEVEC until the event has resolved, and then resume depending on the initial severity of the event
Cytopenias have been reported. Complete blood counts should be performed weekly for the first month, biweekly for the second month, and periodically thereafter as clinically indicated (eg, every 2-3 months). Dose reduction, treatment interruption, or in rare cases discontinuation of treatment may be required for severe neutropenia or thrombocytopenia (see full Prescribing Information for dose adjustment recommendations)
Severe congestive heart failure and left ventricular dysfunction have been reported. Most of the patients with reported cardiac events have had other comorbidities and risk factors, including advanced age and previous medical history of cardiac disease. Patients with cardiac disease or risk factors for cardiac disease or history of renal failure should be monitored carefully, and any patient with signs or symptoms consistent with cardiac or renal failure should be evaluated and treated
Hepatotoxicity, occasionally severe, may occur. Cases of fatal liver failure and severe liver injury requiring liver transplants have been reported with both short-term and long-term use of GLEEVEC. Assess liver function before initiation of treatment and monthly thereafter, or as clinically indicated. A 25% decrease in the recommended dose should be used for patients with severe hepatic impairment. If severe hepatotoxicity occurs, GLEEVEC should be withheld until the event has resolved and then resumed depending on the initial severity of the event
When GLEEVEC is combined with chemotherapy, liver toxicity in the form of transaminase elevation and hyperbilirubinemia has been observed. Additionally, there have been reports of acute liver failure. Monitoring of hepatic function is recommended
In the newly diagnosed CML trial, 1.8% of patients had hemorrhage (NCI Grades 3/4)
In the Phase 3 unresectable or metastatic GIST studies, 13% of patients reported hemorrhage (NCI Grades 3/4) at any site. In the Phase 2 unresectable or metastatic GIST study, 5% of patients were reported to have severe gastrointestinal (GI) bleeds and/or intratumoral bleeds. GI tumor sites may have been the source of GI bleeds; therefore, GI symptoms should be monitored at the start of therapy
In patients with hypereosinophilic syndrome and cardiac involvement, cardiogenic shock and left ventricular dysfunction have been associated with initiation of GLEEVEC. The condition was reported to be reversible with the administration of systemic steroids, circulatory support measures, and temporarily withholding GLEEVEC. MDS /MPD disease and systemic mastocytosis may be associated with high eosinophil levels. Performance of an echocardiogram and determination of serum troponin should, therefore, be considered in patients with HES/CEL and in patients with MDS/MPD or ASM associated with high eosinophil levels. If either is abnormal, the prophylactic use of systemic steroids (1-2 mg/kg) for 1-2 weeks concomitantly with GLEEVEC should be considered at the initiation of therapy
Bullous dermatologic reactions (eg, erythema multiforme and Stevens-Johnson syndrome) have also been reported. In some cases, the reaction recurred upon rechallenge. Several postmarketing reports describe patients able to tolerate the reintroduction of GLEEVEC at a lower dose, with or without concomitant corticosteroids or antihistamines following resolution or improvement of the bullous reaction
Clinical cases of hypothyroidism have been reported in thyroidectomy patients undergoing levothyroxine replacement during treatment with GLEEVEC. TSH levels should be closely monitored in such patients
Consider potential toxicitiesspecifically liver, kidney, and cardiac toxicityand immunosuppression from long-term use
Fetal harm can occur when administered to a pregnant woman. Therefore, women of reproductive potential should be advised not to become pregnant while taking GLEEVEC tablets and to avoid breastfeeding while taking GLEEVEC because of the potential for serious adverse reactions in nursing infants. Sexually active female patients taking GLEEVEC should use highly effective contraception. If the patient does become pregnant while taking GLEEVEC, the patient should be advised of the potential hazard to the fetus
Growth retardation has been reported in children and preadolescents receiving GLEEVEC. The long-term effects of prolonged treatment with GLEEVEC on growth in children are unknown; therefore, monitoring of growth in children taking GLEEVEC is recommended
Cases of tumor lysis syndrome (TLS), including fatal cases, have been reported. The patients at risk of TLS are those with tumors having a high proliferative rate or high tumor burden prior to treatment. These patients should be monitored closely and appropriate precautions taken. Correction of clinically significant dehydration and treatment of high uric acid levels are recommended prior to initiation of GLEEVEC
Motor vehicle accidents involving patients receiving GLEEVEC have been reported. Patients should be advised that they may experience undesirable effects such as dizziness, blurred vision, or somnolence during treatment with GLEEVEC. Caution should be recommended when driving a car or operating machinery
In Ph+ CML trials,* severe (NCI Grades 3/4) lab abnormalitiesincluding neutropenia (3.6%-48%), anemia (1%-42%), thrombocytopenia (<1%-33%), and hepatotoxicity (~ 5%)—and severe (NCI Grades 3/4) adverse experiences, including hemorrhage (1.8%-19%), fluid retention (eg, pleural effusion, pulmonary edema, and ascites) (2.5%-11%) and superficial edema (1.5%-6%), and musculoskeletal pain (2%-9%) were reported among patients receiving GLEEVEC. Severe fluid retention appears to be dose related, was more common in the advanced phase studies (where the dosage was 600 mg/day), and is more common in the elderly
In HES/CEL patients, instances of Grade 3 leukopenia, neutropenia, lymphopenia, and anemia were reported
For DFSP, severe (NCI Grades 3/4) lab abnormalities included anemia (17%), thrombocytopenia (17%), neutropenia (8%), and increased creatinine (8%)
In the Phase 2 unresectable or metastatic GIST trial (400 mg/d; 600 mg/d), severe (NCI Grades 3/4) lab abnormalities—including anemia (3%; 9%) and neutropenia (10%; 11%)—were reported among patients receiving GLEEVEC. In Phase 3 unresectable or metastatic GIST trials (400 mg/day; 800 mg/day), the most frequently reported adverse reactions included abdominal pain (14%; 12%), edema (9%; 13%), fatigue (12%; 12%), nausea (9%; 8%), vomiting (9%; 8%), diarrhea (8%; 9%), rash (8%; 9%), myalgia (6%; 4%), anemia (5%; 6%), and anorexia (7%; 5%). The percentages listed represent NCI Grades 3 and above
In the adjuvant GIST study comparing 12 months of GLEEVEC vs placebo treatment (GLEEVEC; placebo), severe (NCI Grades 3 and above) lab abnormalities included increase in liver enzymes (ALT) (3%; 0%), (AST) (2%; 0%), decreased neutrophil count (3%; 1%), and decrease in hemoglobin (1%; 0%); severe (NCI Grades 3 and above reported at rates >1%) adverse reactions included abdominal pain (3%; 1%), diarrhea (3%; 1%), rash (3%; 0%), fatigue (2%; 1%), nausea (2%; 1%), vomiting (2%; 1%), decreased white blood cell count (1%; 0%), and periorbital edema (1%; 0%). The frequencies of these reported lab abnormalities and severe adverse reactions were similar in a study comparing 12 vs 36 months of GLEEVEC treatment (12 mo; 36 mo), except for liver enzyme AST (2%; 3%), decreased neutrophil count (5%; 5%), decreased white blood cell count (2%; 3%), pain (1%; 3%), infection (2%; 3%), and blurred vision (1%; 1%), which were higher among patients receiving 36 months of adjuvant treatment with GLEEVEC*
There have also been reports, including fatalities, of cardiac tamponade, cerebral edema, acute respiratory failure, and GI perforation
GLEEVEC is metabolized by the CYP3A4 isoenzyme and is an inhibitor of CYP3A4, CYP2D6, and CYP2C9. Significant reductions in imatinib concentrations may occur when GLEEVEC is administered concomitantly with agents that are strong CYP3A4 inducers such as rifampin, St. John's wort, and enzyme-inducing anti-epileptic drugs, eg, phenytoin. The concomitant use of strong CYP3A4 inducers should be avoided. If patients must be administered a strong CYP3A4 inducer, the dosage of GLEEVEC should be increased by at least 50%, and clinical response should be carefully monitored. Caution is recommended when GLEEVEC is administered with CYP3A4 inhibitors such as ketoconazole, with CYP2D6 substrates that have a narrow therapeutic window, or with CYP3A4 substrates that have a narrow therapeutic window. Other examples of commonly used drugs that may significantly interact with GLEEVEC include acetaminophen, warfarin, erythromycin, and metoprolol. Grapefruit juice should also be avoided in patients taking GLEEVEC. (Please see full Prescribing Information for other potential drug interactions)
Patients with moderate renal impairment (CrCL = 20-39 mL/min) should receive a 50% decrease in the recommended starting dose; future doses can be increased as tolerated. Doses greater than 600 mg are not recommended in patients with mild renal impairment (CrCL = 40-59 mL/min). For patients with moderate renal impairment, doses greater than 400 mg are not recommended. GLEEVEC should be used with caution in patients with severe renal impairment

Common Side Effects of GLEEVEC Tablets

Almost all adult Ph+ CML patients who received GLEEVEC in clinical studies experienced adverse reactions at some time but most were mild to moderate in severity. The most frequently reported adverse reactions (all grades) and those with rates greater than 45% were superficial edema (60%-74%), nausea (50%-73%), diarrhea (43%-57%), hemorrhage (29%-57%), musculoskeletal pain (38%-49%), fatigue (39%-48%), rash and related terms (36%-47%), muscle cramps (28%-62%), and vomiting (23%-58%)^†
The adverse reactions and safety profile for Ph+ ALL, MDS/MPD, ASM, and HES/CEL were generally similar to the safety profile for Ph+ CML
The adverse reactions were similar for Ph+ ALL as for Ph+ CML. The most frequently reported drug-related adverse reactions in the Ph+ ALL studies were mild nausea, vomiting, diarrhea, myalgia, muscle cramps, and rash. Superficial edemas were also a common finding in all studies and were described primarily as periorbital or lower-limb edemas. However, these edemas were rarely severe and may be managed (severity reduced) with diuretics, other supportive measures, or in some patients by reducing the dose of GLEEVEC
Frequently reported adverse reactions (all grades) in the 7 MDS/MPD patients assessed were nausea (57%); diarrhea and muscle cramps (43% each); anemia, fatigue, arthralgia, and periorbital edema (29% each)
All ASM patients experienced at least 1 adverse reaction at some time. The most frequently reported adverse reactions were diarrhea, nausea, ascites, muscle cramps, dyspnea, fatigue, peripheral edema, anemia, pruritus, rash, and lower respiratory tract infection
All HES/CEL patients experienced at least 1 adverse reaction, the most common being GI, cutaneous, and musculoskeletal disorders. Hematologic abnormalities were also frequent, with instances of Grade 3 leukopenia, neutropenia, lymphopenia, and anemia
Frequently reported adverse reactions (all grades) in the 12 DFSP patients assessed included nausea and fatigue (42% each); periorbital, peripheral, and eye edema (33% each); diarrhea, vomiting, rash, lacrimation increased, and anemia (25% each); face edema, pyrexia, exertional dyspnea, rhinitis, and anorexia (17% each)
Almost all patients who received GLEEVEC in the Phase 3 unresectable or metastatic GIST studies experienced adverse reactions at some time. Overall, the incidence of all grades of adverse reactions and the incidence of severe (CTC Grade 3 and above) adverse reactions were similar between the 2 treatment arms, except for edema and rash/related terms, which were reported more frequently in the 800-mg group. The most frequently reported adverse reactions (400 mg/day; 800 mg/day) (all grades) were edema (77%; 86%), fatigue (69%; 75%), nausea (58%; 65%), abdominal pain (57%; 55%), diarrhea (56%; 58%), rash and related terms (56%; 70%), vomiting (37%; 41%), myalgia (32%; 30%), anemia (32%; 35%), anorexia (31%; 36%), and arthralgia (14%; 12%). Therapy with GLEEVEC was discontinued for adverse reactions in 5% of patients studied*
In the adjuvant treatment of GIST studies, almost all the GLEEVEC- and placebo-treated patients experienced adverse reactions at some time. The most frequently reported adverse reactions were similar to those reported in other clinical studies in other patient populations. In Study 1, comparing 12 months of GLEEVEC treatment vs placebo (all grades), these included (GLEEVEC; placebo) diarrhea (59%; 29%), fatigue (57%; 41%), nausea (53%; 28%), periorbital edema (47%; 15%), decreased hemoglobin (47%; 27%), peripheral edema (27%; 15%), rash (26%; 13%), vomiting (26%; 14%), abdominal pain (21%; 22%), anorexia (17%; 9%), muscle spasms (16%; 3%), white blood cell count decreased (15%; 4%), arthralgia (15%; 15%), and myalgia (12%; 12%).* The frequencies of these reported adverse reactions were similar in Study 2, comparing 12 vs 36 months of GLEEVEC treatment (12 mo; 36 mo), except for decreased hemoglobin (72%; 80%), periorbital edema (59%; 74%), muscle spasms (31%; 49%), decreased white blood cell count (35%; 47%), pain (26%; 46%), peripheral edema (33%; 41%), rash (29%; 39%), arthralgia (9%; 17%), and myalgia (9%; 15%), which were higher among patients receiving 36 months of adjuvant treatment with GLEEVEC. Adverse reactions listed represent the most frequently reported for Study 1 with the addition of adverse reactions with higher rates in Study 2*
In the adjuvant GIST study comparing GLEEVEC vs placebo, drug was discontinued for adverse events in 17% of GLEEVEC- and 3% of placebo-treated patients. Edema, GI disturbances (nausea, vomiting, abdominal distension, and diarrhea), fatigue, low hemoglobin, and rash were the most frequently reported adverse reactions at the time of discontinuation. In the adjuvant study comparing 12 vs 36 months of GLEEVEC treatment, drug was discontinued for adverse events in 8% of patients treated for 12 months and 14% of patients treated for 36 months*
Supportive care may help reduce the severity of some mild to moderate adverse reactions. However, in some cases, either a dose reduction or interruption of treatment with GLEEVEC may be necessary
Doses of 400 mg or 600 mg should be administered once daily, whereas a dose of 800 mg should be administered at 400 mg twice a day. For daily dosing of 800 mg and above, dosing should be accomplished using the 400-mg tablet to reduce exposure to iron
GLEEVEC tablets should be taken with food and a large glass of water to minimize GI irritation
Patients should be instructed to take GLEEVEC exactly as prescribed and not to change their dose or stop taking GLEEVEC unless they are told to do so by their doctor. If patients miss a dose, they should be advised to take their dose as soon as possible unless it is almost time for their next dose, in which case the missed dose should not be taken. A double dose should not be taken to make up for any missed dose

*For more detailed study information, please see full Prescribing Information.

^†Numbers indicate the range of percentages in 4 studies among adult patients, with newly diagnosed Ph+ CML, patients in blast crisis, accelerated phase, and in the chronic phase after failure of interferon-alpha therapy.

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Gleevec

KIT+ GIST

Response rates for KIT+ GIST

GLEEVEC® significantly improves recurrence-free survival1,2,*

9 out of 10 patients remained recurrence free with GLEEVEC2,*

More than double the number of recurrence events occurred in the placebo arm compared with the GLEEVEC arm (HR=0.398 [95% CI: 0.259, 0.610], P<0.0001)1,2

The rate of tumor recurrence increased after stopping adjuvant therapy with GLEEVEC3

GLEEVEC may be continued in the absence of progression or unacceptable toxicity1

Provide proven efficacy with GLEEVEC®1

The majority of patients achieved a response in phase 3 metastatic trials1

Adequate time must be allowed for response to GLEEVEC1

GLEEVEC provides durable responses with up to 2 years of progression-free survival (PFS) at the 800-mg/day dose1

Prematurely switching patients to another targeted therapy is not recommended by the NCCN3

Fight disease progression with GLEEVEC 800 mg/day1

Continuing GLEEVEC treatment at same or increased dose as tolerated is recommended in cases of limited or generalized progression3

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