英文药名：ARRANON/Atriance(nelarabine Injection)

中文药名：奈拉滨注射剂

生产厂家：葛兰素史克
药品介绍
奈拉滨(Nekarabine，美国上市的商品名：Arranon，欧洲上市的商品名：Atriance 公司：葛兰素史克)是一种嘌呤类似物抗代谢药，其批准上市日期为2005年10月28日。
【适应症】
奈拉滨主要用于曾经接受过至少两种化疗方案治疗但仍无应答，或病情出现复发的急性T细胞型淋巴母细胞白血病及T细胞型淋巴母细胞淋巴瘤患者。
【药理及药代动力学】
奈拉滨是脱氧鸟苷类似物9-b-D-阿糖呋喃糖鸟嘌呤(ara-G)的前体药物。奈拉滨在腺苷脱氨酶(ADA)的作用下脱去甲基转变为ara-G，随后，又在脱氧鸟苷激酶和脱氧胞苷激酶的作用下，经单磷酸化作用途径转变为具有活性的ara-G三磷酸盐(ara-GTP)。ara-GTP可在白血病原始细胞(keukemic bkast cekk)中逐渐积聚，并与DNA相结合，从而起到抑制DNA合成，促进白血病细胞死亡的作用。此外，奈拉滨的抗癌机制可能还与其细胞毒性和全身毒性作用有关。
复发性白血病或淋巴瘤患者的药代动力学研究发现，奈拉滨和ara-G在血浆中的消除迅速，在给予1500mg/m2剂量的奈拉滨后，两者半衰期分别为30分钟和3小时。研究还发现，ara-G通常在奈拉滨给药完毕时达到峰浓度，而且其峰浓度数值通常也大于奈拉滨的峰浓度，表明奈拉滨可在体内迅速、完全地转化为ara-G。奈拉滨和ara-G部分经肾脏消除，28名成年患者在给予奈拉滨后24小时测得的奈拉滨和ara-G的平均肾排泄率分别为6.6±4.7%和27±15%。
【注意事项】
 奈拉滨所致的神经毒性属于剂量限制性毒性反应。患者在用药期间应密切留意是否出现意识模糊、嗜睡、惊厥、共济失调、感觉异常和感觉减退等症状。曾经接受过鞘内化疗或颅脊放疗的患者应用奈拉滨后出现神经毒性反应的风险将增大。
奈拉滨还有可能引起白细胞减少症、血小板减少症、贫血和中性粒细胞减少症(包括发热性中性粒细胞减少症)，因此应用奈拉滨的患者应常规进行全血细胞计数(包括血小板计数)。
根据标准治疗方案，正在应用奈拉滨的肿瘤溶解综合征患者并发高尿酸血症时，可通过静脉水合方式加以缓解；存在高尿酸血症风险的患者还可考虑服用别嘌醇进行治疗。应用奈拉滨的免疫缺陷患者应避免注射活疫苗。
【药物相互作用】
迄今尚未见有关奈拉滨和ara-G药物相互作用的报道。体内实验发现，奈拉滨和ara-G不会明显抑制人细胞色素P450同功酶1A2、2A6、2B6、2C8、2C9、2C19、2D6或3A4的活性。
【不良反应】
儿童患者应用奈拉滨后最常见的是血液系统不良事件(如贫血、白细胞减少、中性粒细胞减少和血小板减少)。在非血液系统不良事件中，最常见的是头痛、转氨酶水平升高、血钾水平降低、血白蛋白水平降低、血胆红素水平升高和呕吐。
成年患者应用奈拉滨后最常见的不良事件为疲劳、胃肠道不适(如恶心、腹泻、呕吐和便秘)、血液系统不良事件(如贫血、中性粒细胞减少和血小板减少)、呼吸系统不良事件(咳嗽和呼吸困难)、神经系统不良事件(嗜睡和头晕)以及发热。
【剂量及用药】奈拉滨注射剂为澄清、无色、无菌溶液，其规格为50mk∶250mg，储存在聚氯乙烯(PVC)输液袋或玻璃瓶中。奈拉滨注射剂经静脉给药，无需再进行稀释，成人患者每次静脉输注时间为2小时，儿童患者则为1小时。给予奈拉滨注射剂前，护士或药师应目测检查制剂产品中是否含有微粒物质或是否发生颜色改变。
奈拉滨的成人推荐剂量为1500mg/m2，分别在治疗开始第1天、第3天和第5天给药，每21天重复给药一次。奈拉滨的儿童推荐剂量为650 mg/m2，在治疗开始第1至第5天连续5天给药，每21天重复给药一次。成人及儿童患者用奈拉滨治疗的推荐疗程尚未建立。在临床试验中，受试者通常一直用药，直到出现以下情况：患者病情出现进展，患者不能耐受毒性反应，患者有望接受骨髓移植或者患者通过药物治疗不能再获得更多的好处。
【用药提示】
由于患者应用奈拉滨后可能出现嗜睡，因此患者在用药期间应避免操作具有危险性的机械，包括驾驶机动车。当患者出现新的周围神经病症状或原有症状加重时，应告知医师加以处理，这些体征和症状包括：手指、手部、脚趾和足部出现麻刺或麻木感；精细运动协调功能(如扣钮扣)出现障碍；走路不稳；从位置较低的椅子上起立时感到无力；上楼梯时感到无力；以及在不平坦地面上走路时容易跌倒等等。
应告知患者应用奈拉滨后可能会出现癫痫发作。因此，如果出现癫痫发作，患者应立即通知医生进行处理。此外，患者在用药过程中若出现发烧或感染症状，也应立即告知医生。
ARRANON - nelarabine injection 
GlaxoSmithKline LLC
ARRANON®(nelarabine) Injection
FOR INTRAVENOUS USE

WARNING

ARRANON (nelarabine) is a pro-drug of the cytotoxic deoxyguanosine analogue, 9-β-D-arabinofuranosylguanine (ara-G).

The chemical name for nelarabine is 2-amino-9-β-D-arabinofuranosyl-6-methoxy-9H-purine. It has the molecular formula C11H15N5O5 and a molecular weight of 297.27. Nelarabine has the following structural formula:

Nelarabine is slightly soluble to soluble in water and melts with decomposition between 209° and 217° C.

ARRANON Injection is supplied as a clear, colorless, sterile solution in glass vials. Each vial contains 250 mg of nelarabine (5 mg nelarabine per mL) and the inactive ingredient sodium chloride (4.5 mg per mL) in 50 mL Water for Injection, USP. ARRANON is intended for intravenous infusion.

Hydrochloric acid and sodium hydroxide may have been used to adjust the pH. The solution pH ranges from 5.0 to 7.0.

CLINICAL PHARMACOLOGY

Mechanism of Action

Nelarabine is a pro-drug of the deoxyguanosine analogue 9-β-D-arabinofuranosylguanine (ara-G). Nelarabine is demethylated by adenosine deaminase (ADA) to ara-G, mono-phosphorylated by deoxyguanosine kinase and deoxycytidine kinase, and subsequently converted to the active 5’-triphosphate, ara-GTP. Accumulation of ara-GTP in leukemic blasts allows for incorporation into deoxyribonucleic acid (DNA), leading to inhibition of DNA synthesis and cell death. Other mechanisms may contribute to the cytotoxic and systemic toxicity of nelarabine.

Pharmacokinetics

Pharmacokinetic studies in adult patients with refractory leukemia or lymphoma have demonstrated that nelarabine and ara-G are rapidly eliminated from plasma with a half-life of approximately 30 minutes and 3 hours, respectively, after a 1,500 mg/m2 nelarabine dose. No pharmacokinetic data are available in pediatric patients at the once daily 650 mg/m2 nelarabine dose. Plasma ara-G Cmax values generally occurred at the end of the nelarabine infusion and were generally higher than nelarabine Cmax values, suggesting rapid and extensive conversion of nelarabine to ara-G. Mean plasma nelarabine and ara-G Cmax values were 5.0 ± 3.0 μg/mL and 31.4 ± 5.6 μg/mL, respectively, after a 1,500 mg/m2 nelarabine dose infused over 2 hours in adult patients. Exposure to ara-G (AUC) is 37 times higher than that for nelarabine on Day 1 after nelarabine IV infusion of 1,500 mg/m2 dose (162 ± 49 μg.h/mL versus 4.4 ± 2.2 μg.h/mL, respectively). Comparable Cmax and AUC were obtained for nelarabine between Days 1 and 5 at the proposed nelarabine adult dosage of 1,500 mg/m2, indicating that the pharmacokinetics of nelarabine after multiple-dosing are predictable from single dosing. There are not enough data for ara-G to make a comparison between Day 1 and Day 5. After a nelarabine adult dosage of 1,500 mg/m2, a mean intracellular Cmax for ara-GTP appeared within 3 to 25 hours on Day 1. Exposure (AUC) to intracellular ara-GTP was 532 times higher than that for nelarabine and 14 times higher than that for ara-G (2,339 ± 2,628 μg.h/mL versus 4.4 ± 2.2 μg.h/mL and 162 ± 49 μg.h/mL, respectively). Because the intracellular levels of ara-GTP were so prolonged, its elimination half-life could not be accurately estimated.

Combined Phase 1 pharmacokinetic data at nelarabine doses of 104 to 2,900 mg/m2 indicate that the mean clearance (CL) of nelarabine is about 30% higher in pediatric patients than in adult patients (259 ± 409 L/h/m2 versus 197 ± 189 L/h/m2, respectively) (n = 66 adults, n = 22 pediatric patients) on Day 1. The apparent clearance of ara-G (CL/F) is comparable between the two groups (10.5 ± 4.5 L/h/m2 in adult patients and 11.3 ± 4.2 L/h/m2 in pediatric patients) on Day 1.

Nelarabine and ara-G are extensively distributed throughout the body. Specifically, for nelarabine, VSS values were 197 ± 216 L/m2 and 213 ± 358 L/m2 in adult and pediatric patients, respectively. For ara-G, VSS/F values were 50 ± 24 L/m2 and 33 ± 9.3 L/m2 in adult and pediatric patients, respectively.

Nelarabine and ara-G are not substantially bound to human plasma proteins (<25%) in vitro, and binding is independent of nelarabine or ara-G concentrations up to 600 μM.

Metabolism: The principal route of metabolism for nelarabine is O-demethylation by adenosine deaminase to form ara-G, which undergoes hydrolysis to form guanine. In addition, some nelarabine is hydrolyzed to form methylguanine, which is O-demethylated to form guanine. Guanine is N-deaminated to form xanthine, which is further oxidized to yield uric acid. Ring opening of uric acid followed by further oxidation results in the formation of allantoin.

Excretion: Nelarabine and ara-G are partially eliminated by the kidneys. Mean urinary excretion of nelarabine and ara-G was 6.6 ± 4.7% and 27 ± 15% of the administered dose, respectively, in 28 adult patients over the 24 hours after nelarabine infusion on Day 1. Renal clearance averaged 24 ± 23 L/h for nelarabine and 6.2 ± 5.0 L/h for ara-G in 21 adult patients.

Special Populations

Gender: Gender has no effect on nelarabine or ara-G pharmacokinetics.

Race: Most patients enrolled in Phase 1 studies were Whites. In general, nelarabine mean clearance and volume of distribution values tend to be higher in Whites (n = 63) than in Blacks (by about 10%) (n = 15). The opposite is true for ara-G; mean apparent clearance and volume of distribution values tend to be lower in Whites than in Blacks (by about 15-20%). No differences in safety or effectiveness were observed between these groups.

Geriatrics: Age has no effect on the pharmacokinetics of nelarabine or ara-G. Decreased renal function, which is more common in the elderly, may reduce ara-G clearance (see PRECAUTIONS, Geriatric Use).

Pediatrics: No pharmacokinetic data are available in pediatric patients at the once daily 650 mg/m2 nelarabine dosage. Combined Phase 1 pharmacokinetic data at nelarabine doses of 104 to 2,900 mg/m2 indicate that the mean clearance (CL) of nelarabine is about 30% higher in pediatric patients than in adult patients (259 ± 409 L/h/m2 versus 197 ± 189 L/h/m2, respectively) (n = 66 adults, n = 22 pediatric patients) on Day 1. The apparent clearance of ara-G (CL/F) is comparable between the two groups (10.5 ± 4.5 L/h/m2 in adult patients and 11.3 ± 4.2 L/h/m2 in pediatric patients) on Day 1.

Nelarabine and ara-G are extensively distributed throughout the body. Specifically, for nelarabine, VSS values were 197 ± 216 L/m2 and 213 ± 358 L/m2 in adult and pediatric patients, respectively. For ara-G, VSS/F values were 50 ± 24 L/m2 and 33 ± 9.3 L/m2 in adult and pediatric patients, respectively.

Renal Impairment: The pharmacokinetics of nelarabine and ara-G have not been specifically studied in renally impaired or hemodialyzed patients. Nelarabine is excreted by the kidney to a small extent (5 to 10% of the administered dose). Ara-G is excreted by the kidney to a greater extent (20 to 30% of the administered nelarabine dose). Patients were categorized into 3 groups: normal with CLcr >80 mL/min (n = 67), mild with CLcr = 50-80 mL/min (n = 15), and moderate with CLcr<50 mL/min (n = 3). The mean apparent clearance (CL/F) of ara-G was about 15% and 40% lower in patients with mild and moderate renal impairment, respectively, than in patients with normal renal function (see PRECAUTIONS and DOSAGE AND ADMINISTRATION). No differences in safety or effectiveness were observed.

Hepatic Impairment: The influence of hepatic impairment on the pharmacokinetics of nelarabine has not been evaluated.

Drug Interactions

Nelarabine and ara-G did not significantly inhibit the activities of the human hepatic cytochrome P450 isoenzymes 1A2, 2A6, 2B6, 2C8, 2C9, 2C19, 2D6, or 3A4 in vitro at concentrations of nelarabine and ara-G up to 100 μM.

Administration of fludarabine 30 mg/m2 as a 30-minute infusion 4 hours before a 1,200 mg/m2 infusion of nelarabine did not affect the pharmacokinetics of nelarabine, ara-G, or ara-GTP in 12 patients with refractory leukemia.

CLINICAL STUDIES

The safety and efficacy of ARRANON were evaluated in two open-label, single-arm, multicenter studies.

Pediatric Clinical Study

The safety and efficacy of ARRANON in pediatric patients were studied in a clinical trial conducted by the Children’s Oncology Group (COG P9673). This study included patients 21 years of age and younger, who had relapsed or refractory T-cell acute lymphoblastic leukemia (T-ALL) or T-cell lymphoblastic lymphoma (T-LBL). Eighty-four (84) patients, 39 of whom had received two or more prior induction regimens, were treated with 650 mg/m2/day of ARRANON administered intravenously over 1 hour daily for 5 consecutive days repeated every 21 days (see Table 1). Patients who experienced signs or symptoms of grade 2 or greater neurologic toxicity on therapy were to be discontinued from further therapy with ARRANON.

Table 1. Pediatric Clinical Study - Patient Allocation

Patient Population	N
Patients treated at 650 mg/m2/day x 5 days every 21 days.	84
Patients with T-ALL or T-LBL with two or more prior induction treated at 650 mg/m2/day x 5 days every 21 days.	39
Patients with T-ALL or T-LBL with one prior induction treated at 650 mg/m2/day x 5 days every 21 days.	31

The 84 patients ranged in age from 2.5-21.7 years (overall mean, 11.9 years), 52% were 3 to 12 years of age and most were male (74%) and Caucasian (62%). The majority (77%) of patients had a diagnosis of T-ALL.

Complete response (CR) in this study was defined as bone marrow blast counts ≤5%, no other evidence of disease, and full recovery of peripheral blood counts. Complete response without full hematologic recovery (CR*) was also assessed as a meaningful outcome in this heavily pretreated population. Duration of response is reported from date of response to date of relapse, and may include subsequent stem cell transplant. Efficacy results are presented in Table 2.

Table 2. Efficacy Results in Patients 21 Years of Age and Younger at Diagnosis With ≥2 Prior Inductions Treated with 650 mg/m 2 of ARRANON Administered Intravenously Over 1 Hour Daily for 5 Consecutive Days Repeated Every 21 Days

	N = 39
CR plus CR* % (n) [95% CI]	23% (9) [11%, 39%]
CR % (n) [95% CI]	13% (5) [4%, 27%]
CR* % (n) [95% CI]	10% (4) [3%, 24%]
Duration of CR plus CR* (range in weeks)1	3.3 to 9.3
Median overall survival (weeks) [95% CI]	13.1 [8.7, 17.4]

CR = Complete response

CR* = Complete response without hematologic recovery

1 Does not include 5 patients who were transplanted or had subsequent systemic chemotherapy (duration of response in these 5 patients was 4.7 to 42.1 weeks).

The mean number of days on therapy was 46 days (range of 7 to 129 days). Median time to CR plus CR* was 3.4 weeks (95% CI: 3.0, 3.7).

Adult Clinical Study

The safety and efficacy of ARRANON in adult patients were studied in a clinical trial conducted by the Cancer and Leukemia Group B (CALGB). This study included 39 treated patients, 28 who had T-cell acute lymphoblastic leukemia (T-ALL) or T-cell lymphoblastic lymphoma (T-LBL) that had relapsed following or was refractory to at least two prior induction regimens. ARRANON 1,500 mg/m2 was administered intravenously over 2 hours on days 1, 3 and 5 repeated every 21 days. Patients who experienced signs or symptoms of grade 2 or greater neurologic toxicity on therapy were to be discontinued from further therapy with ARRANON. Seventeen patients had a diagnosis of T-ALL and 11 had a diagnosis of T-LBL. For patients with ≥2 prior inductions, the age range was 16-65 years (mean 34 years) and most patients were male (82%) and Caucasian (61%). Patients with central nervous system (CNS) disease were not eligible.

Complete response (CR) in this study was defined as bone marrow blast counts ≤5%, no other evidence of disease, and full recovery of peripheral blood counts. Complete response without complete hematologic recovery (CR*) was also assessed. The results of the study for patients who had received ≥2 prior inductions are shown in Table 3.

Table 3. Efficacy Results in Adult Patients With ≥2 Prior Inductions Treated with 1,500 mg/m 2 of ARRANON Administered Intravenously Over 2 Hours on Days 1, 3, and 5 Repeated Every 21 Days

	N = 28
CR plus CR* % (n) [95% CI]	21% (6) [8%, 41%]
CR % (n) [95% CI]	18% (5) [6%, 37%]
CR* % (n) [95% CI]	4% (1) [0%, 18%]
Duration of CR plus CR* (range in weeks)1	4 to 195+
Median overall survival (weeks) [95% CI]	20.6 weeks [10.4, 36.4]

CR = Complete response

CR* = Complete response without hematologic recovery

1 Does not include 1 patient who was transplanted (duration of response was 156+ weeks).

The mean number of days on therapy was 56 days (range of 10 to 136 days). Time to CR plus CR* ranged from 2.9 to 11.7 weeks.

INDICATIONS AND USAGE

ARRANON is indicated for the treatment of patients with T-cell acute lymphoblastic leukemia and T-cell lymphoblastic lymphoma whose disease has not responded to or has relapsed following treatment with at least two chemotherapy regimens. This use is based on the induction of complete responses. Randomized trials demonstrating increased survival or other clinical benefit have not been conducted.

CONTRAINDICATIONS

ARRANON is contraindicated in patients who have a history of hypersensitivity to nelarabine or any other components of ARRANON.

WARNINGS

ARRANON should be administered under the supervision of a physician experienced in the use of antineoplastic therapy.

Neurologic Events (see boxed WARNING)

ARRANON is a potent antineoplastic agent with potentially significant toxic side effects. Neurotoxicity is the dose-limiting toxicity of nelarabine. Patients undergoing therapy with ARRANON should be closely observed for signs and symptoms of neurologic toxicity.

Common signs and symptoms of nelarabine-related neurotoxicity include somnolence, confusion, convulsions, ataxia, paresthesias, and hypoesthesia. Severe neurologic toxicity can manifest as coma, status epilepticus, craniospinal demyelination, or ascending neuropathy similar in presentation to Guillain-Barré syndrome.

Patients treated previously or concurrently with intrathecal chemotherapy or previously with craniospinal irradiation may be at increased risk for neurologic adverse events. See DOSAGE AND ADMINISTRATION.

Pregnancy Category D

ARRANON may cause fetal harm when administered to a pregnant woman. There are no studies of ARRANON in pregnant women. When compared to controls, nelarabine administration during the period of organogenesis caused increased incidences of fetal malformations, anomalies, and variations in rabbits at doses ≥360 mg/m2/day (8-hour IV infusion; approximately ¼ the adult dose compared on a mg/m2 basis), which was the lowest dose tested. Cleft palate was seen in rabbits given 3,600 mg/m2/day (approximately 2-fold the adult dose), absent pollices (digits) in rabbits given ≥1,200 mg/m2/day (approximately ¾ the adult dose), while absent gall bladder, absent accessory lung lobes, fused or extra sternebrae and delayed ossification was seen at all doses. Maternal body weight gain and fetal body weights were reduced in rabbits given 3,600 mg/m2/day (approximately 2-fold the adult dose), but could not account for the increased incidence of malformations seen at this or lower administered doses. If this drug is used during pregnancy, or if the patient becomes pregnant while taking this drug, the patient should be warned of the potential hazard to the fetus. Women of child-bearing potential should be advised to avoid becoming pregnant while receiving treatment with ARRANON.

PRECAUTIONS

Hematologic

Leukopenia, thrombocytopenia, anemia, and neutropenia, including febrile neutropenia have been associated with nelarabine therapy. Complete blood counts including platelets should be monitored regularly (see ADVERSE REACTIONS and DOSAGE AND ADMINISTRATION).

General

Patients receiving ARRANON should receive intravenous hydration according to standard medical practice for the management of hyperuricemia in patients at risk for tumor lysis syndrome. Consideration should be given to the use of allopurinol in patients at risk of hyperuricemia.

Administration of live vaccines to immunocompromised patients should be avoided.

Information for Patients

Since patients receiving nelarabine therapy may experience somnolence, they should be cautioned about operating hazardous machinery, including automobiles.

Patients should be instructed to contact their physician if they experience new or worsening symptoms of peripheral neuropathy (see WARNINGS and DOSAGE AND ADMINISTRATION). These signs and symptoms include: tingling or numbness in fingers, hands, toes, or feet; difficulty with the fine motor coordination tasks such as buttoning clothing; unsteadiness while walking; weakness arising from a low chair; weakness in climbing stairs; increased tripping while walking over uneven surfaces.

Patients should be instructed that seizures have been known to occur in patients who receive nelarabine. If a seizure occurs, the physician administering ARRANON should be promptly informed.

Patients who develop fever or signs of infection while on therapy should notify their physician promptly.

Patients should be advised to use effective contraceptive measures to prevent pregnancy and to avoid breast feeding during treatment with ARRANON.

Drug Interactions

Nelarabine and ara-G did not significantly inhibit the activities of the human hepatic cytochrome P450 isoenzymes 1A2, 2A6, 2B6, 2C8, 2C9, 2C19, 2D6, or 3A4 in vitro at concentrations of nelarabine and ara-G up to 100 μM.

There is in vitro evidence that pentostatin is a strong inhibitor of adenosine deaminase. This may result in a reduction in the conversion of the pro-drug nelarabine to its active moiety and consequently in a reduction in efficacy of nelarabine and/or change in adverse event profile of either drug. Administration of nelarabine in combination with adenosine deaminase inhibitors, such as pentostatin, is not recommended.

Carcinogenesis, Mutagenesis, Impairment of Fertility

Carcinogenicity testing of nelarabine has not been done. However, nelarabine was mutagenic when tested in vitro in L5178Y/TK mouse lymphoma cells with and without metabolic activation. No studies have been conducted in animals to assess genotoxic potential or effects on fertility. The effect on human fertility is unknown.

Pregnancy

Pregnancy Category D. (See WARNINGS.)

Nursing Mothers

It is not known whether nelarabine or ara-G are excreted in human milk. Because many drugs are excreted in human milk and because of the potential for serious adverse reactions in nursing infants from ARRANON, nursing should be discontinued in women who are receiving therapy with ARRANON.

Pediatric Use

(See CLINICAL STUDIES, Pediatric Clinical Study).

Geriatric Use

Clinical studies of ARRANON did not include sufficient numbers of patients aged 65 and over to determine whether they respond differently from younger patients. In an exploratory analysis, increasing age, especially age 65 years and older, appeared to be associated with increased rates of neurologic adverse events.

Use in Renally Impaired Patients

Ara-G clearance decreased as renal function decreased (see CLINICAL PHARMACOLOGY). Because the risk of adverse reactions to this drug may be greater in patients with severe renal impairment (CLcr<30 mL/min), these patients should be closely monitored for toxicities when treated with ARRANON (see DOSAGE AND ADMINISTRATION).

Use in Hepatically Impaired Patients

The influence of hepatic impairment on the pharmacokinetics of nelarabine has not been evaluated. Because the risk of adverse reactions to this drug may be greater in patients with severe hepatic impairment (bilirubin >3.0 mg/dL), these patients should be closely monitored for toxicities when treated with ARRANON.

ADVERSE REACTIONS

ARRANON was studied in 459 patients in Phase I and Phase II clinical trials. The safety profile for the recommended dosages of ARRANON is based on data from 103 adult patients enrolled and treated in the CALGB 19801 and an adult chronic lymphocytic leukemia study (PGAA2003) who were treated with the recommended dose and schedule. The safety profile for children is based on data from 84 pediatric patients enrolled and treated in the COG P9673 study who were treated with the recommended dose and schedule.

The most common adverse events in pediatric patients, regardless of causality, were hematologic disorders (anemia, leukopenia, neutropenia, and thrombocytopenia). Of the non-hematologic adverse events in pediatric patients, the most frequent events reported were headache, increased transaminase levels, decreased blood potassium, decreased blood albumin, increased blood bilirubin, and vomiting.

The most common adverse events in adults, regardless of causality, were fatigue; gastrointestinal (GI) disorders (nausea, diarrhea, vomiting, and constipation); hematologic disorders ( anemia, neutropenia, and thrombocytopenia); respiratory disorders (cough and dyspnea); nervous system disorders (somnolence and dizziness); and pyrexia.

The most common adverse events by System Organ Class, regardless of causality, including severe or life threatening events (NCI Common Toxicity Criteria grade 3 or grade 4) and fatal events (grade 5) are shown in Table 4 for pediatric patients and Table 5 for adult patients.

Table 4. Most Commonly Reported (≥5% Overall) Adverse Events Regardless of Causality in Pediatric Patients Treated with 650 mg/m 2 of ARRANON Administered Intravenously Over 1 Hour Daily for 5 Consecutive Days Repeated Every 21 Days

System Organ Class Preferred Term	Percentage of Patients: 650 mg/m2; N = 84
	Toxicity Grade
	Grade 3 %	Grade 4+ %	All Grades %
Blood and Lymphatic System Disorders
Anemia	45	10	95
Neutropenia	17	62	94
Thrombocytopenia	27	32	88
Leukopenia	14	7	38
Hepatobiliary Disorders
Transaminases increased	4	0	12
Blood albumin decreased	5	1	10
Blood bilirubin increased	7	2	10
Metabolic/Laboratory
Blood potassium decreased	4	2	11
Blood calcium decreased	1	1	8
Blood creatinine increased	0	0	6
Blood glucose decreased	4	0	6
Blood magnesium decreased	2	0	6
Nervous System Disorders (see Table 6)
Gastrointestinal Disorders
Vomiting	0	0	10
General Disorders & Administration Site Conditions
Asthenia	1	0	6
Infections& Infestations
Infection	2	1	5

Grade 4+ = Grade 4 and Grade 5

Three (3) patients had a fatal event. Fatal events included neutropenia and pyrexia (n = 1), status epilepticus/seizure (n = 1), and fungal pneumonia (n = 1). The status epilepticus was thought to be related to treatment with ARRANON. All other fatal events were unrelated to treatment with ARRANON.

Table 5. Most Commonly Reported (≥5% Overall) Adverse Events Regardless of Causality in Adult Patients Treated with 1,500 mg/m 2 of ARRANON Administered Intravenously Over 2 Hours on Days 1, 3, and 5 Repeated Every 21 Days

System Organ Class Preferred Term	Percentage of Patients; N = 103
	Toxicity Grade
	Grade 3 %	Grade 4+ %	All Grades %
Blood and Lymphatic System Disorders
Anemia	20	14	99
Thrombocytopenia	37	22	86
Neutropenia	14	49	81
Febrile neutropenia	9	1	12
Cardiac Disorders
Sinus tachycardia	1	0	8
Gastrointestinal Disorders
Nausea	0	0	41
Diarrhea	1	0	22
Vomiting	1	0	22
Constipation	1	0	21
Abdominal pain	1	0	9
Stomatitis	1	0	8
Abdominal distension	0	0	6
General Disorders and Administration Site Conditions
Fatigue	10	2	50
Pyrexia	5	0	23
Asthenia	0	1	17
Edema, peripheral	0	0	15
Edema	0	0	11
Pain	3	0	11
Rigors	0	0	8
Gait, abnormal	0	0	6
Chest pain	0	0	5
Non-cardiac chest pain	0	1	5
Infections
Infection	2	1	9
Pneumonia	4	1	8
Sinusitis	1	0	7
Hepatobiliary Disorders
AST increased	1	1	6
Metabolism and Nutrition Disorders
Anorexia	0	0	9
Dehydration	3	1	7
Hyperglycemia	1	0	6
Musculoskeletal and Connective Tissue Disorders
Myalgia	1	0	13
Arthralgia	1	0	9
Back pain	0	0	8
Muscular weakness	5	0	8
Pain in extremity	1	0	7
Nervous System Disorders (see Table 7)
Psychiatric Disorders
Confusional state	2	0	8
Insomnia	0	0	7
Depression	1	0	6
Respiratory, Thoracic, and Mediastinal Disorders
Cough	0	0	25
Dyspnea	4	2	20
Pleural effusion	5	1	10
Epistaxis	0	0	8
Dyspnea, exertional	0	0	7
Wheezing	0	0	5
Vascular Disorders
Petechiae	2	0	12
Hypotension	1	1	8

Grade 4+ = Grade 4 and Grade 5

Five (5) patients had a fatal event. Fatal events included hypotension (n = 1), respiratory arrest (n = 1), pleural effusion/pneumothorax (n = 1), pneumonia (n = 1), and cerebral hemorrhage/coma/leukoencephalopathy (n = 1). The cerebral hemorrhage/coma/leukoencephalopathy was thought to be related to treatment with ARRANON. All other fatal events were unrelated to treatment with ARRANON.

Other Adverse Events

Blurred vision was also reported in 4% of adult patients.

There was a single report of biopsy confirmed progressive multifocal leukoencephalopathy in the adult patient population.

There have been reports of sometimes fatal opportunistic infections in patients receiving ARRANON.

Neurologic Adverse Events

Nervous system events, regardless of drug relationship, were reported for 64% of patients across the Phase I and Phase II studies.

Pediatric: The most common neurologic adverse events (≥2%), regardless of causality, including all grades (NCI Common Toxicity Criteria) are shown in Table 6 for pediatric patients.

Table 6. Neurologic Adverse Events (≥2%) Regardless of Causality in Pediatric Patients Treated with 650 mg/m 2 of ARRANON Administered Intravenously Over 1 Hour Daily for 5 Consecutive Days Repeated Every 21 Days

Nervous System Disorders Preferred Term	Percentage of Patients; N = 84
	Grade 1 %	Grade 2 %	Grade 3 %	Grade 4+ %	All Grades %
Headache	8	2	4	2	17
Peripheral neurologic disorders, any event	1	4	7	0	12
Peripheral neuropathy	0	4	2	0	6
Peripheral motor neuropathy	1	0	2	0	4
Peripheral sensory neuropathy	0	0	6	0	6
Somnolence	1	4	1	1	7
Hypoesthesia	1	1	4	0	6
Seizures	0	0	0	6	6
Convulsions	0	0	0	3	4
Grand mal convulsions	0	0	0	1	1
Status epilepticus	0	0	0	1	1
Motor dysfunction	1	1	1	0	4
Nervous system disorder	1	2	0	0	4
Paresthesia	0	2	1	0	4
Tremor	1	2	0	0	4
Ataxia	1	0	1	0	2

Grade 4+ = Grade 4 and Grade 5

One (1) patient had a fatal neurologic event, status epilepticus. This event was thought to be related to treatment with ARRANON.

The other grade 3 event in pediatric patients, regardless of causality, was hypertonia reported in 1 patient (1%). The additional grade 4+ events, regardless of causality, were 3rd nerve paralysis, and 6th nerve paralysis, each reported in 1 patient (1%).

The other neurologic adverse events, regardless of causality, reported as grade 1, 2, or unknown in pediatric patients were dysarthria, encephalopathy, hydrocephalus, hyporeflexia, lethargy, mental impairment, paralysis, and sensory loss, each reported in 1 patient (1%).

Adults: The most common neurologic adverse events (≥2%), regardless of causality, including all grades (NCI Common Toxicity Criteria) are shown in Table 7 for adult patients.

Table 7. Neurologic Adverse Events (≥2%) Regardless of Causality in Adult Patients Treated with 1,500 mg/m 2 of ARRANON Administered Intravenously Over 2 Hours on Days 1, 3, and 5 Repeated Every 21 Days

Nervous System Disorders Preferred Term	Percentage of Patients; N =103
	Grade 1 %	Grade 2 %	Grade 3 %	Grade 4 %	All Grades %
Somnolence	20	3	0	0	23
Dizziness	14	8	0	0	21
Peripheral neurologic disorders, any event	8	12	2	0	21
Neuropathy	0	4	0	0	4
Peripheral neuropathy	2	2	1	0	5
Peripheral motor neuropathy	3	3	1	0	7
Peripheral sensory neuropathy	7	6	0	0	13
Hypoesthesia	5	10	2	0	17
Headache	11	3	1	0	15
Paresthesia	11	4	0	0	15
Ataxia	1	6	2	0	9
Depressed level of consciousness	4	1	0	1	6
Tremor	2	3	0	0	5
Amnesia	2	1	0	0	3
Dysgeusia	2	1	0	0	3
Balance disorder	1	1	0	0	2
Sensory loss	0	2	0	0	2

One (1) patient had a fatal neurologic event, cerebral hemorrhage/coma/leukoencephalopathy. This event was thought to be related to treatment with ARRANON.

Most nervous system events in the adult patients were evaluated as grade 1 or 2. The additional grade 3 events in adult patients, regardless of causality, were aphasia, convulsion, hemiparesis, and loss of consciousness, each reported in 1 patient (1%). The additional grade 4 events, regardless of causality, were cerebral hemorrhage, coma, intracranial hemorrhage, leukoencephalopathy, and metabolic encephalopathy, each reported in one patient (1%).

The other neurologic adverse events, regardless of causality, reported as grade 1, 2, or unknown in adult patients were abnormal coordination, burning sensation, disturbance in attention, dysarthria, hyporeflexia, neuropathic pain, nystagmus, peroneal nerve palsy, sciatica, sensory disturbance, sinus headache, and speech disorder, each reported in one patient (1%).

Other Neurologic Events

There have also been reports of events associated with demyelination and ascending peripheral neuropathies similar in appearance to Guillain-Barré syndrome.

Adverse Reactions from Other Clinical Programs

In addition to the safety data from the pivotal clinical trials, tumor lysis syndrome has been observed (see PRECAUTIONS, General).

OVERDOSAGE

There is no known antidote for overdoses of ARRANON. It is anticipated that overdosage would result in severe neurotoxicity (possibly including paralysis, coma), myelosuppression, and potentially death. In the event of overdose, supportive care consistent with good clinical practice should be provided.

Nelarabine has been administered in clinical trials up to a dose of 2,900 mg/m2 on days 1, 3, and 5 to 2 adult patients. At a dose of 2,200 mg/m2 given on days 1, 3, and 5 every 21 days, 2 patients developed a significant grade 3 ascending sensory neuropathy. MRI evaluations of the 2 patients demonstrated findings consistent with a demyelinating process in the cervical spine.

A single IV dose of 4,800 mg/m2 was lethal in monkeys, and was associated with CNS signs including reduced/shallow respiration, reduced reflexes, and flaccid muscle tone.

DOSAGE AND ADMINISTRATION

Preparation for Administration

ARRANON is not diluted prior to administration. The appropriate dose of ARRANON is transferred into polyvinylchloride (PVC) infusion bags or glass containers and administered as a two-hour infusion in adult patients and as a one-hour infusion in pediatric patients.

Prior to administration, inspect the drug product visually for particulate matter and discoloration.

Adult Dosage

The recommended adult dose of ARRANON is 1,500 mg/m2 administered intravenously over 2 hours on days 1, 3, and 5 repeated every 21 days. ARRANON is administered undiluted.

Pediatric Dosage

The recommended pediatric dose of ARRANON is 650 mg/m2 administered intravenously over 1 hour daily for 5 consecutive days repeated every 21 days. ARRANON is administered undiluted.

The recommended duration of treatment for adult and pediatric patients has not been clearly established. In clinical trials, treatment was generally continued until there was evidence of disease progression, the patient experienced unacceptable toxicity, the patient became a candidate for bone marrow transplant, or the patient no longer continued to benefit from treatment.

Supportive Care

Appropriate measures (e.g., hydration, urine alkalinization, and prophylaxis with allopurinol) must be taken to prevent hyperuricemia of tumor lysis syndrome.

Dose Modification

ARRANON should be discontinued for neurologic events of NCI Common Toxicity Criteria grade 2 or greater. Dosage may be delayed for other toxicity including hematologic toxicity.

Adjustment of Dose in Special Populations

ARRANON has not been studied in patients with hepatic or renal dysfunction (see PRECAUTIONS). No dose adjustment is recommended for patients with a CLcr≥50 mL/min (see CLINICAL PHARMACOLOGY, Renal Impairment). There are insufficient data to support a dose recommendation for CLcr<50 mL/min.

Precautions

ARRANON is a cytotoxic agent. Caution should be used during handling and preparation. Use of gloves and other protective clothing to prevent skin contact is recommended. Proper aseptic technique should be used.

Stability

Nelarabine Injection is stable in polyvinylchloride (PVC) infusion bags and glass containers for up to 8 hours at up to 30° C.

Handling and Disposal

Procedures for proper handling and disposal of anticancer drugs should be used. Several guidelines on this subject have been published.1-9

There is no general agreement that all of the procedures recommended in the guidelines are necessary or appropriate.

HOW SUPPLIED

ARRANON Injection is supplied as a clear, colorless, sterile solution in Type I, clear glass vials with a gray butyl rubber (latex-free) stopper and a red snap-off aluminum seal. Each vial contains 250 mg of nelarabine (5 mg nelarabine per mL) and the inactive ingredient sodium chloride (4.5 mg per mL) in 50 mL Water for Injection, USP. Vials are available in the following carton sizes:

NDC 0007-4401-01 (package of 1)

NDC 0007-4401-06 (package of 6)

Store at 25° C (77° F); excursions permitted to 15° to 30° C (59° to 86° F) [see USP Controlled Room Temperature].

http://www.kegg.jp/medicus-bin/japic_med_product?id=00053758
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【上市国家】美国
【原产地英文商品名】Arranon 250MG/VIAL 6VIALS/BOX
【原产地英文药品名】nelarabine
【中文参考商品译名】奈拉滨 250毫克/针剂 6针剂/盒
【中文参考药品译名】奈拉滨注射液
【曾用名】阿仑恩
【生产厂家中文参考译名】葛兰素史克
【生产厂家英文名】GlaxoSmithKline
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【上市国家】德国/英国
【原产地英文商品名】Atriance 250MG/VIAL 6VIALS/BOX
【原产地英文药品名】nelarabine
【中文参考商品译名】奈拉滨 250毫克/瓶 6瓶/盒
【中文参考药品译名】奈拉滨注射液
【曾用名】阿仑恩
【生产厂家中文参考译名】葛兰素史克
【生产厂家英文名】GlaxoSmithKline
--------------------------------------------
【上市国家】日本
【原产地英文商品名】ARRANON G Injection（アラノンジー静注用）250MG/VIAL 1VIALS/BOX
【原产地英文药品名】nelarabine
【中文参考商品译名】ARRANON G注射液（アラノンジー静注用）250毫克/瓶 1瓶/盒
【中文参考药品译名】奈拉滨
【曾用名】阿仑恩
【生产厂家中文参考译名】葛兰素史克
【生产厂家英文名】GlaxoSmithKline