1. Special Populations:�Clinical Trials and Elderly Cancer Patients Stuart M. Lichtman, MD, FACP
Associate Attending
Memorial Sloan-Kettering Cancer Center
3. Cancer Leading Cause of Death-Jan 05
4. Age Specific Cancer Incidence Rates
5. Cancer Mortality and Mortality Rates
6. Incidence of 10 Major Cancers in Patients Over 65 years (73-95)
7. % US Population 65 and older
8. Life Expectancy: Woman
9. Life Expectancy: Woman
10. Life Expectancy: Woman
11. The facts 60% of cancer is in people greater than 65 years of age
70% of cancer mortality is in people greater than 65 years of age
12. Therefore More older patients
Living longer
Living healthier
More indications for anticancer therapy
Many more patients in need of getting more therapy
13. Geriatric Oncology How is cancer treatment studied?
Primarily middle aged patients; minimal inclusion of older patients
Minimal comorbidity; patients with other medical problems excluded
Caucasian
Cancer center based; little community involvement
20. How is cancer treatment studied? Primarily middle aged patients; minimal inclusion of older patients
Minimal comorbidity; patients with other medical problems excluded
Caucasian
Cancer center based
21. Elderly and Registration Trials
22. Elderly and Registration Trials
23. NCI Sponsored Trials by Age
24. NCI Sponsored Trials
25. Topics Pharmacology
Design Issues
Clinical Trials Reporting
26. Pharmacology Absorption
Distribution
Metabolism
Excretion
27. Absorption Factors that may affect absorption
Controllable
Concomitant medication, ie. H2 blockers, antacids
Compliance
Not Controllable
Reduced gastric secretion, gastric emptying, gastrointestinal motility
Diminished splanchnic blood flow
Decreased absorption surface
28. Distribution Changes in body composition
fat content doubles
decreased intracellular water
albumin concentrations reduced (etopside, taxanes are highly protein bound)
anemia
Increase in volume of distribution
Lower peak concentration and prolonged terminal t
29. Hepatic Metabolism and Age: P450 Liver flow reduced
Liver size decreases
Age related changes in P450 microsomal systems
Polypharmacy*
P450 inhibitors: grapefruit juice
P450 inducers: phenobarbital
30. Medications
31. Metabolism and P450 Drug interactions extremely important issue in elderly
Increases risk of hospitalization and dependency
Emphasizes the importance of minimizing concomitant medications
?Role of different isoenzymes: genetic influences
?Role of nonP450 medications
32. Chemotherapy P450 Metabolism
33. Excretion Decline in glomerular filtration rate (GFR) is one of the most predictable changes associated with aging
Additional effect of comorbid conditions on renal function
34. Renal Excretion Drugs completely excreted through the kidneys:
Methotrexate
Carboplatin
Drugs partially excreted through the kidneys:
Epipodophyllotoxins
Fludarabine
Capecitabine
Pemetrexed
Drugs producing active or toxic metabolites excreted through the kidneys:
Cytarabine (high doses)
35. Sample CrCl Calculations �Cockcroft-Gault: Female
36. Sample CrCl Calculations Using Cockcroft-Gault:Female
37. CrCl: Which formula? Cockcroft-Gault
Jelliffe
Levey: MDRD or aMDRD
Wright
Clinical Consequences
May alter clinical trial eligibility or exclude patient from standard therapy
Misperception of drug safety, I.e. cisplatin
38. Pharmacology Pharmacokinetics
Little evidence of PK changes based on age alone
Changes (variability) are result of:
Comorbidity
Endorgan dysfunction
Physical factors: fat, anemia, albumin, etc.
Polypharmacy
Gender, ethnicity, genotype
39. Influence of pharmacokinetics
40. Pharmacodynamic Heterogeneity of Effect
Tremendous variability in toxicity
Increased susceptibility
Myelosuppression
Mucositis
Cardiac toxicity
Nervous system toxicity
41. Design Issues
42. Design Issues Patient Selection
Endpoints
Dose Limiting Toxicity
Toxicity Evaluation
43. Patient Selection Which older patient?
Comorbidity
Endorgan dysfunction: renal, hepatic
Cardiac disease
Neuropathy
Prior malignancy, i.e. prior chemotherapy, radiotherapy
44. Which Older Patient?: Stages of Aging
45. Patient Selection: Stages of Aging
46. Comorbidity and Function Comorbidity evaluation
Prevalent in elderly
Can predict survival
Various scales: Charlson, Cumulative Illness Rating Scale-Geriatric (CIRS-G)
Function
Can predict survival
ADL, IADL
Physical function: gait speed, get-up-and-go, etc.
Dependency
Should we or can we evaluate the frail patient?
47. Design Issues: Endpoints Survival
Is the patient going to die of or with cancer?
Response
Overall response
Freedom from progression
Time without symptoms
Functional and clinical benefit, quality of life
48. Design Issues: DLT Hematologic
Modulated by growth factors
Nonhematologic
Predominating
Are our toxicity scales adequate for older patients?
Function
49. Non-hematologic
50. Toxicity Evaluation-CTC v2
51. Toxicity Evaluation: Functional
52. Toxicity Evaluation-Frail
53. Proposed Toxicity Assessment Peripheral sensory neuropathy
Oxaliplatin, vinca alkaloids, paclitaxel
Sequelae of neuropathy in older patients
Falls, social isolation (not driving), chronic impairment
Incorporate other measures
Hand grip
Get up and go; gait speed
54. Functional Assessment as Endpoint Alterations in:
ADL
IADL
Geriatric syndromes
Falls, delirium, incontinence, nutrition
Maintain independence/avoid further dependence
55. Comprehensive Geriatric Assessment Is Highly Sensitive to Common Problems in Elderly There is a high prevalence of problems that could adversely affect course of cancer and its treatment; the CGA is the best tool for detecting such problems.
Findings in 200 consecutive elderly patients (age =70) at H. Lee Moffitt Cancer Center and Research Institute, screened by CGA:1
18% dependent in ADL (dressing, eating, use of toilet, etc)
72% dependent in IADL (driving, shopping, meal preparation, etc)
36% with serious comorbidity on Charlson scale (short list of selected diseases)
94% with serious comorbidity on CIRS-G scale (Cumulative Illness Rating Scale-Geriatric; comprehensive listing of diseases)
22% with memory disorder
19% with poor nutritional status
41% with polypharmacy
Conclusions:
High prevalence of problems in elderly patients
CGA is highly sensitive in revealing these problems
CGA is indicated in all patients age =70 (or younger if signs of aging are present, such as falls, memory loss, loss of independence)
Balducci L, Extermann M. Management of cancer in the older patient: a practical approach. Oncologist. 2000;5:224237.
There is a high prevalence of problems that could adversely affect course of cancer and its treatment; the CGA is the best tool for detecting such problems.
Findings in 200 consecutive elderly patients (age =70) at H. Lee Moffitt Cancer Center and Research Institute, screened by CGA:1
18% dependent in ADL (dressing, eating, use of toilet, etc)
72% dependent in IADL (driving, shopping, meal preparation, etc)
36% with serious comorbidity on Charlson scale (short list of selected diseases)
94% with serious comorbidity on CIRS-G scale (Cumulative Illness Rating Scale-Geriatric; comprehensive listing of diseases)
22% with memory disorder
19% with poor nutritional status
41% with polypharmacy
Conclusions:
High prevalence of problems in elderly patients
CGA is highly sensitive in revealing these problems
CGA is indicated in all patients age =70 (or younger if signs of aging are present, such as falls, memory loss, loss of independence)
Balducci L, Extermann M. Management of cancer in the older patient: a practical approach. Oncologist. 2000;5:224237.
56. Comprehensive Geriatric Assessment Is Highly Sensitive to Common Problems in Elderly There is a high prevalence of problems that could adversely affect course of cancer and its treatment; the CGA is the best tool for detecting such problems.
Findings in 200 consecutive elderly patients (age =70) at H. Lee Moffitt Cancer Center and Research Institute, screened by CGA:1
18% dependent in ADL (dressing, eating, use of toilet, etc)
72% dependent in IADL (driving, shopping, meal preparation, etc)
36% with serious comorbidity on Charlson scale (short list of selected diseases)
94% with serious comorbidity on CIRS-G scale (Cumulative Illness Rating Scale-Geriatric; comprehensive listing of diseases)
22% with memory disorder
19% with poor nutritional status
41% with polypharmacy
Conclusions:
High prevalence of problems in elderly patients
CGA is highly sensitive in revealing these problems
CGA is indicated in all patients age =70 (or younger if signs of aging are present, such as falls, memory loss, loss of independence)
Balducci L, Extermann M. Management of cancer in the older patient: a practical approach. Oncologist. 2000;5:224237.
There is a high prevalence of problems that could adversely affect course of cancer and its treatment; the CGA is the best tool for detecting such problems.
Findings in 200 consecutive elderly patients (age =70) at H. Lee Moffitt Cancer Center and Research Institute, screened by CGA:1
18% dependent in ADL (dressing, eating, use of toilet, etc)
72% dependent in IADL (driving, shopping, meal preparation, etc)
36% with serious comorbidity on Charlson scale (short list of selected diseases)
94% with serious comorbidity on CIRS-G scale (Cumulative Illness Rating Scale-Geriatric; comprehensive listing of diseases)
22% with memory disorder
19% with poor nutritional status
41% with polypharmacy
Conclusions:
High prevalence of problems in elderly patients
CGA is highly sensitive in revealing these problems
CGA is indicated in all patients age =70 (or younger if signs of aging are present, such as falls, memory loss, loss of independence)
Balducci L, Extermann M. Management of cancer in the older patient: a practical approach. Oncologist. 2000;5:224237.
57. Design Issues Polypharmacy
Beers list (Fick, et al. 2003)
Minimize ADR
Modulate effects of drug interactions
Sampling
Limited sampling strategies
Minimize visits
Increase compliance
58. Progressively Increasing Inclusion Criteria (PIIC) protocol design: Extermann Rationale
Older patients are underrepresented in cancer trials.
The selected healthy patients that are enrolled appear in most cases to do roughly as well as younger patients with their treatment.
Category of vulnerable elderly patients, but an evidence-based definition is still lacking in oncology.
59. Progressively Increasing Inclusion Criteria (PIIC) protocol design: Extermann Rationale (cont)
Studies focused on patients in poor condition (typically ECOG PS 2), accrue poorly, probably due to the low prevalence of such patients in the population seen in centers and reluctance to enter
Geriatric instruments such as IADL, GDS, comorbidity, etc appear to add prognostic information to ECOG PS, but cut-offs for chemotherapy modifications have not yet been determined.
60. Progressively Increasing Inclusion Criteria (PIIC) protocol design: Extermann Objective
Provide a study design that would allow establishing clinical cut offs for treatment modifications and response categories.
Eligibility
Age 70 and above
Stage IV NSCLC
No previous chemotherapy for metastatic disease
Cohort I: ECOG PS 0-1, independent in IADL (28-29), Charlson <2
Cohort II: ECOG PS 0-1, IADL 21-27 (mild dependence) or Charlson 2
Cohort III: IADL <21, Charlson > 2, or ECOG PS 2
61. Publications in Geriatric Oncology
62. Report of Clinical Trials Journals
Journal of Clinical Oncology
Journal of the National Cancer Institute
Cancer
Criteria
January 2005-December 2006
Prospective clinical trials
At least 50 patients
63. Data
Papers reviewed:
258 JCO, 58 Cancer, and 17 JNCI
The median number of patients enrolled per trial into these studies is
212 (JCO), 77.5 (Cancer), and 954 (JNCI).
Mean age: 59.4 years (range 16 to 93 years).
64. Data
65. Barriers to Participation Fewer trials available
Focus on aggressive therapy
Trial eligibility limits participation, ie. comorbidity, previous malignancy
Limited expectation of benefit
Physician reluctance to recruit older patients and recommend protocols
Complicate trials requiring large expenditure of time for patients and caregivers
66. Conclusions 1)Drugs, which will be primarily used by older patients, should be studied in older patients. These studies should involve pharmacokinetic analysis and oral medication should include measurements of compliance;
2) randomized phase II trials of new agents in groups of patients divided by age. These studies should involve pharmacokinetic analysis;
3)dose modify in a phase I fashion using progressive degrees of functional impairment and increasing comorbidity;
4)include functional independence as a clinical benefit of cancer treatment in older individuals;
67. Conclusions 5)consider studying long term functional and medical consequences of cancer treatment in long term older cancer survivors.
6)Journal editors should encourage the inclusion of age related analyses in the reporting of clinical trials to provide meaningful information for clinicians caring for older patients.
7)Clinical trial design of adult cancer patients should prospectively incorporate age analysis to maximize data generated
68. Thank You
69. Supplemental Slides
70. Comorbidity is Key Factor
71. Burden of Comorbidity�Yancik Variety of comorbidities
hypertension
heart disease
arthritis
gastrointestinal problems
anemia
eye problems
urinary tract problems
previous cancers
gall bladder problems
COPD
diabetes
thyroid/glandular
72. Burden of Comorbidity�Yancik Patients with >5 comorbid conditions
55-65 years 13%
66-74 years 24%
75+ years 39%
73. Burden of Comorbidity�Yancik Predictors of early mortality (24 months) with colon cancer
Disorder RR
heart disease 1.31
COPD 1.51
renal failure 1.73
liver disease 2.54
74. Effect of Comorbidity of 3 Year Survival with Breast Cancer��Mortality v. Comorbidity
75. Geriatric Syndromes Delirium
Dementia
Incontinence
Falls
Pressure ulcers
Malnutrition
Osteoporosis
Language
Hearing and vision
Sleep
76. Activities of Daily Living (ADL) Toilet
Feeding
Dressing
Grooming
Ambulation
Bathing
77. Instrumental ADL (IADL) Telephone
Shopping
Food preparation
Housekeeping
Laundry
Transportation
Medication
78. 8% if fully independent,
14% if dependent in IADL,
27% if dependent in ADL,
? 40% if institutionalized.
Reuben Am J Med 1992;93:663 2-year mortality rate for persons aged 70 years and older D:
D:
79. Frailty Age =85
3+ comorbidity
1+ geriatric syndrome(s)
1+ ADL
Biologic markers: d-dimer, IL-6
80. Survival by Functioning
81. Guidelines for Management of the�Older Cancer Patient: The Assessment Function
Comorbidity
Cognition
Nutrition
Pharmacy
Socioeconomic status
Geriatric syndromes
82. Aging Physiology and Cancer
83. Metabolism and P450 Drug interactions extremely important issue in elderly
Increases risk of hospitalization and dependency
Emphasizes the importance of minimizing concomitant medications
?Role of different isoenzymes: genetic influences
?Role of nonP450 medications
?Any toxicity specificity
85. This slide demonstrates the change in clearance by age.This slide demonstrates the change in clearance by age.
86. Renal Excretion Drugs completely excreted through the kidneys:
Methotrexate (*use with extreme care)
Carboplatin
Drugs partially excreted through the kidneys:
Epipodophyllotoxins
Fludarabine
Capecitabine
Pemetrexed
Drugs producing active or toxic metabolites excreted through the kidneys:
Cytarabine (high doses)
87. Creatinine Clearance and Aging
88. Cockcroft-Gault formula
89. Sample CrCl Calculations �Cockcroft-Gault: Female
90. Sample CrCl Calculations Using Cockcroft-Gault:Female
91. Renal Dysfunction�National Kidney Foundation
92. International Society of Geriatric Oncology Renal Taskforce (prelim) Prior to drug therapy optimisation of hydration status and evaluation of renal function to establish any need for dose adjustment is required.
Serum creatinine alone is insufficient as a means of evaluating renal function.
More accurate tools, including creatinine clearance methods such as C-G are available and are generally good indices of renal function status of the patient.
93. International Society of Geriatric Oncology Renal Taskforce (prelim) In extremes of obesity and cachexia and at very high and low creatinine values, no single tool is really accurate.
Within each drug class, preference may be given to agents less likely to be toxic to the kidneys or for which appropriate methods of prevention for renal toxicity exist.
Co-administration of known nephrotoxic drugs such as bisphosphonates, NSAIDS or Cox-2 inhibitors should be avoided or minimised.
94. Are elderly cancer patients under treated?
Stuart M. Lichtman, MD
Memorial Sloan-Kettering Cancer Center
95. What is under treatment? Poor evaluation?
Poor treatment?
Surgery
Radiation
Chemotherapy
96. Under treatment Question needs to be answered in terms of:
Goal of therapy
Potential benefit of therapy-what is the best possible outcome?
97. Goal Palliative
No potential for cure
Curative therapy exists
Patient cannot tolerate potentially curable therapy
Who decides
How is this decided
self fulfilling prophesy
98. Curative therapy Adjuvant breast
Adjuvant colon
Advanced ovarian cancer
Large cell lymphoma
99. Adjuvant Treatment of Colon Cancer
100. SEER Database
From 1998-2002, the median age at diagnosis for cancer of the colon and rectum was 72 years of age.
Approximately 29.2% between 75 and 84; and 12.6% 85+ years of age.
101. Age-Specific SEER Incidence Rates by Sex for Colon and Rectum Cancer, 1998-2002�
102. Questions being asked Do older patients receive adjuvant chemotherapy?
Do older patients benefit from adjuvant therapy?
103. Age and Adjuvant Chemotherapy Use After Surgery for�Stage III Colon Cancer�
104. Questions being asked Do older patients receive adjuvant chemotherapy?
Do older patients benefit from adjuvant therapy?
106. Colon Cancer-Adjuvant�Age NOT A Factor
107. Phase III MOSAIC Trial:�Adjuvant Oxaliplatin This large, multicenter, multinational phase III study (de Gramont, et al) aimed to demonstrate a 25% decrease in the risk of recurrence at 3 years for patients receiving FOLFOX in stage II/III colon cancer. Since 1998, 2248 patients with completely resected stage II (40%) or III (60%) colorectal cancer were randomly assigned to receive LV5FU2 (leucovorin, fluorouracil, bolus and infusion), also known as the de Gramont schedule, or FOLFOX (LV5FU2 + oxaliplatin) bimonthly for 12 cycles. At the onset of the study, the expected 3-year disease free survival was assumed to be 73% in the control arm and 79% in the treatment arm. This large, multicenter, multinational phase III study (de Gramont, et al) aimed to demonstrate a 25% decrease in the risk of recurrence at 3 years for patients receiving FOLFOX in stage II/III colon cancer. Since 1998, 2248 patients with completely resected stage II (40%) or III (60%) colorectal cancer were randomly assigned to receive LV5FU2 (leucovorin, fluorouracil, bolus and infusion), also known as the de Gramont schedule, or FOLFOX (LV5FU2 + oxaliplatin) bimonthly for 12 cycles. At the onset of the study, the expected 3-year disease free survival was assumed to be 73% in the control arm and 79% in the treatment arm.
110. FOLFOX in > 70 Year Olds 3700 patients in 4 trials
493 older than age 70
No difference in overall survival
No difference in toxicity
No difference in 3rd and 6th cycle dose intensity
111. Results-FOLFOX and Age
112. Efficacy by Age �PFS/DFS
113. Adjuvant Therapy
114. Adjuvant Therapy Completion
115. Colon Cancer Definitive evidence of benefit and tolerance of adjuvant therapy
Older patients are untreated
Less adequate surgery
Lower incidence of chemotherapy
Less chemotherapy received
Leads to lower survival
116. Adjuvant Treatment of Breast Cancer with Chemotherapy
117. Age-Specific SEER Incidence Rates For Breast Cancer�SEER 13 Registries for 1998-2002�
118. SEER Data From 2000-2003, the median age at diagnosis was 61 years of age
Age Distribution
10.6% between 35 and 44
22.1% between 45 and 54
22.8% between 55 and 64
20.4% between 65 and 74
16.8% between 75 and 84
5.4% 85+ years of age.
123. Breast Cancer Evidence of benefit of adjuvant therapy-limited data
Older patients are untreated
Lower incidence of chemotherapy
Less chemotherapy received
Leads to lower survival
124. Advanced Ovarian Cancer
125. Ovary: Survival by Age-SEER
126. Literature Review
127. Variations in the Use of Chemotherapy for Elderly Patients�with Advanced Ovarian Cancer: A Population-Based Study�
129. Advanced Ovarian Cancer over 65 Years
130. Advanced Ovarian Cancer by Age No difference:
PFS
OS
Chemotherapy regimens
Chemotherapy dose administered
Chemotherapy toxicity
131. Ovarian Cancer Definitive evidence of benefit and tolerance of therapy for advanced disease
Older patients are untreated
Lower incidence of chemotherapy
Less chemotherapy received
Leads to lower survival
132. Malignant Lymphoma
133. Non-Hodgkins Lymphoma: SEER Incidence �1973-1975 vs. 1993-1995 The SEER data shows that the incidence of non-Hodgkins lymphoma rises with age. The recent database also indicates that the overall incidence of non-Hodgkins lymphoma has increased over the indicated twenty year period. The exact cause remains unknown. Speculation includes the AIDS epidemic, environmental factors and our increased ability to make specific diagnoses and an increased aggressiveness in pursing diagnoses in older patients.
Reference
Ries LAG, Eisner MP, Kosary CL, Hankey BF, Miller BA, Clegg L, Edwards BK (eds).
SEER Cancer Statistics Review, 1973-1998, National Cancer Institute. Bethesda, MD, 2001.
http://seer.cancer.gov/Publications/CSR1973_1998/The SEER data shows that the incidence of non-Hodgkins lymphoma rises with age. The recent database also indicates that the overall incidence of non-Hodgkins lymphoma has increased over the indicated twenty year period. The exact cause remains unknown. Speculation includes the AIDS epidemic, environmental factors and our increased ability to make specific diagnoses and an increased aggressiveness in pursing diagnoses in older patients.
Reference
Ries LAG, Eisner MP, Kosary CL, Hankey BF, Miller BA, Clegg L, Edwards BK (eds).
SEER Cancer Statistics Review, 1973-1998, National Cancer Institute. Bethesda, MD, 2001.
http://seer.cancer.gov/Publications/CSR1973_1998/
134. Standard-Dose CHOP Yields Comparable Response in Younger and Older NHL Patients On standard-dose CHOP regimen, older and younger lymphoma patients showed similar frequency and duration of complete response, and frequency of toxicity.
Classic study from Southwest Oncology Group:1 307 patients with advanced diffuse histiocytic lymphoma (a form of non-Hodgkins lymphoma).
Treatment: CHOP (cyclophosphamide, doxorubicin, vincristine, prednisone), with or without bleomycin, and with or without immunotherapy.
Population included 81 patients age 65 or over, in whom protocol ordered automatic 50% reduction in chemotherapy dosage:
58 received half-dose treatment (as per protocol)
23 received full-dose treatment (in violation of protocol)
For all patients (N = 307), complete response rate declined with age (P <0.001).
However, in patients who received full-dose chemotherapy (n = 212), no significant �age-related differences in:
Complete response rate
Duration of complete response (relative relapse rate)
Frequency of treatment-related complications
Conclusion: automatic reduction in chemotherapy dosage based on age contributed to poorer outcome in older patients.
Findings consistent with later research suggesting that older patients with aggressive �non-Hodgkins lymphoma derive benefit from treatment comparable to that achieved �in younger patients2 and should be treated with the intent of achieving cure.3
Dixon DO, Neilan B, Jones SE, et al. Effect of age on therapeutic outcome in advanced diffuse histiocytic lymphoma: the Southwest Oncology Group experience. J Clin Oncol. 1986;4:295-305.
Gaynor ER, Dahlberg S, Fisher RI. Factors affecting reduced survival of the elderly with intermediate and high-grade lymphoma: an analysis of SWOG-8516 (int 0067)the National High Priority Lymphoma Study: a randomized comparison of CHOP vs m-BACOD vs ProMACE-CytaBOM vs MACOP-B. Proc ASCO. 1994;13. Abstract 1250.
Tirelli U, Zagonel V, Errante D, et al. Treatment of non-Hodgkins lymphoma in the elderly: an update. Hematol Oncol. 1998;16:113. On standard-dose CHOP regimen, older and younger lymphoma patients showed similar frequency and duration of complete response, and frequency of toxicity.
Classic study from Southwest Oncology Group:1 307 patients with advanced diffuse histiocytic lymphoma (a form of non-Hodgkins lymphoma).
Treatment: CHOP (cyclophosphamide, doxorubicin, vincristine, prednisone), with or without bleomycin, and with or without immunotherapy.
Population included 81 patients age 65 or over, in whom protocol ordered automatic 50% reduction in chemotherapy dosage:
58 received half-dose treatment (as per protocol)
23 received full-dose treatment (in violation of protocol)
For all patients (N = 307), complete response rate declined with age (P <0.001).
However, in patients who received full-dose chemotherapy (n = 212), no significant age-related differences in:
Complete response rate
Duration of complete response (relative relapse rate)
Frequency of treatment-related complications
Conclusion: automatic reduction in chemotherapy dosage based on age contributed to poorer outcome in older patients.
Findings consistent with later research suggesting that older patients with aggressive non-Hodgkins lymphoma derive benefit from treatment comparable to that achieved in younger patients2 and should be treated with the intent of achieving cure.3
Dixon DO, Neilan B, Jones SE, et al. Effect of age on therapeutic outcome in advanced diffuse histiocytic lymphoma: the Southwest Oncology Group experience. J Clin Oncol. 1986;4:295-305.
Gaynor ER, Dahlberg S, Fisher RI. Factors affecting reduced survival of the elderly with intermediate and high-grade lymphoma: an analysis of SWOG-8516 (int 0067)the National High Priority Lymphoma Study: a randomized comparison of CHOP vs m-BACOD vs ProMACE-CytaBOM vs MACOP-B. Proc ASCO. 1994;13. Abstract 1250.
Tirelli U, Zagonel V, Errante D, et al. Treatment of non-Hodgkins lymphoma in the elderly: an update. Hematol Oncol. 1998;16:113.
135. International Non-Hodgkins Lymphoma (NHL) Prognostic Factors Projects Age > 60 years
Stage III/IV
Extranodal sites > 2
PS > 2
Lactate dehydrogenase (LDH) > normal This prognostic factor was based on adults with aggressive non-Hodgkin's lymphoma from 16 institutions and cooperative groups in the United States, Europe, and Canada who were treated between 1982 and 1987 with combination-chemotherapy regimens containing doxorubicin were evaluated for clinical features predictive of overall survival and relapse-free survival. Features that remained independently significant in step-down regression analyses of survival were incorporated into models that identified groups of patients of all ages and groups of patients no more than 60 years old with different risks of death.
In 2031 patients of all ages, the model, based on age, tumor stage, serum lactate dehydrogenase concentration, performance status, and number of extranodal disease sites, identified four risk groups with predicted five-year survival rates of 73 percent, 51 percent, 43 percent, and 26 percent. In 1274 patients 60 or younger, an age-adjusted model based on tumor stage, lactate dehydrogenase level, and performance status identified four risk groups with predicted five-year survival rates of 83 percent, 69 percent, 46 percent, and 32 percent. In both models, the increased risk of death was due to both a lower rate of complete responses and a higher rate of relapse from complete response. These two indexes, called the international index and the age-adjusted international index, were significantly more accurate than the Ann Arbor classification in predicting long-term survival.
Reference: A predictive model for aggressive non-Hodgkin's lymphoma. The International Non-Hodgkin's Lymphoma Prognostic Factors Project. N Engl J Med. 1993;329:987-994.
This prognostic factor was based on adults with aggressive non-Hodgkin's lymphoma from 16 institutions and cooperative groups in the United States, Europe, and Canada who were treated between 1982 and 1987 with combination-chemotherapy regimens containing doxorubicin were evaluated for clinical features predictive of overall survival and relapse-free survival. Features that remained independently significant in step-down regression analyses of survival were incorporated into models that identified groups of patients of all ages and groups of patients no more than 60 years old with different risks of death.
In 2031 patients of all ages, the model, based on age, tumor stage, serum lactate dehydrogenase concentration, performance status, and number of extranodal disease sites, identified four risk groups with predicted five-year survival rates of 73 percent, 51 percent, 43 percent, and 26 percent. In 1274 patients 60 or younger, an age-adjusted model based on tumor stage, lactate dehydrogenase level, and performance status identified four risk groups with predicted five-year survival rates of 83 percent, 69 percent, 46 percent, and 32 percent. In both models, the increased risk of death was due to both a lower rate of complete responses and a higher rate of relapse from complete response. These two indexes, called the international index and the age-adjusted international index, were significantly more accurate than the Ann Arbor classification in predicting long-term survival.
Reference: A predictive model for aggressive non-Hodgkin's lymphoma. The International Non-Hodgkin's Lymphoma Prognostic Factors Project. N Engl J Med. 1993;329:987-994.
136. 5-Year Survival vs Risk Category: �<60 Years vs ? 60 Years Risk categories in terms of number of factors present: Low-0,1; Low-Intermediate-2; High-Intermediate-3, High 4,5.
The table shows that there is a significant change in 5 year survival by risk category and age. It clearly demonstrates that prognosis for non-Hodgkins lymphoma in the older patient population can bary from 56% to 21% depending category.Risk categories in terms of number of factors present: Low-0,1; Low-Intermediate-2; High-Intermediate-3, High 4,5.
The table shows that there is a significant change in 5 year survival by risk category and age. It clearly demonstrates that prognosis for non-Hodgkins lymphoma in the older patient population can bary from 56% to 21% depending category.
137. Overall Survival in the Treatment Groups The curve shows that overall survival did not vary by treatment regimen.The curve shows that overall survival did not vary by treatment regimen.
138. CHOP-R Cyclophosphamide 750 mg/m2
Adriamycin 50 mg/m2
Vincristine 2 mg
Prednisone 100 mg/m2/day x 5 days
Rituximab 375 mg/m2
every 21 days for 6-8 cycles
139. Overall Survival Improved with Rituximab
140. Myeloid Growth Factors: Primary Prophylaxis in Elderly Patients Patients over 70 years at high risk of early morbidity and mortality
Myeloid growth factors reduce risk It is suggested that patients aged 70 and older who are receiving moderately toxic chemotherapy (cyclophosphamide, hydroxydaunorubicin, vincristine, and prednisone [CHOP] or CHOP-like) be specifically mentioned as a special high-risk group recommended to receive primary prophylactic treatment with growth factors starting up front with the first course of chemotherapy. The suggestion is based on the following considerations and data. In nine studies of older individuals with large-cell non-Hodgkins lymphoma, the risk of life-threatening neutropenia was higher than 40% in all studies. The risk of neutropenic infections varied between 21% and 47%, and the risk of infectious death varied between 5% and 30%. The majority of deaths and serious infections occurred in the first course of chemotherapy, before secondary prophylaxis with growth factors could even be considered. In the study of Gomez et al, there were 51 deaths (20%) among 260 patients receiving chemotherapy; 36 deaths occurred during the first two courses of chemotherapy, and 63% of these were after the first course. Generally the seriousness of neutropenic infections is increased, and so is the duration of hospitalization in older individuals, involving a substantially increased cost per infection. Furthermore, hospitalization of older individuals is associated with increased risk of functional dependence that may increase the cost of treatment due to expensive home care and rehabilitation. In at least four studies, hematopoietic growth factors reduced the risk of neutropenia and neutropenic infection by 32% to 83% in older patients with large-cell non-Hodgkins lymphomas. The National Comprehensive Cancer Network advisory panel for the guidelines for the management of older individuals has unanimously recommended that hematopoietic growth factors be used routinely in persons aged 70 and older who are receiving moderately toxic chemotherapy.
References
Balducci L, Lyman GH. Patients aged > or = 70 are at high risk for neutropenic infection and should receive hemopoietic growth factors when treated with moderately toxic chemotherapy. J Clin Oncol. 2001;19:1583-1585.
Gomez H, Hidalgo M, Casanova L, et al. Risk factors for treatment-related death in elderly patients with aggressive non-Hodgkin's lymphoma: results of a multivariate analysis. J Clin Oncol. 1998;16:2065-2069.
It is suggested that patients aged 70 and older who are receiving moderately toxic chemotherapy (cyclophosphamide, hydroxydaunorubicin, vincristine, and prednisone [CHOP] or CHOP-like) be specifically mentioned as a special high-risk group recommended to receive primary prophylactic treatment with growth factors starting up front with the first course of chemotherapy. The suggestion is based on the following considerations and data. In nine studies of older individuals with large-cell non-Hodgkins lymphoma, the risk of life-threatening neutropenia was higher than 40% in all studies. The risk of neutropenic infections varied between 21% and 47%, and the risk of infectious death varied between 5% and 30%. The majority of deaths and serious infections occurred in the first course of chemotherapy, before secondary prophylaxis with growth factors could even be considered. In the study of Gomez et al, there were 51 deaths (20%) among 260 patients receiving chemotherapy; 36 deaths occurred during the first two courses of chemotherapy, and 63% of these were after the first course. Generally the seriousness of neutropenic infections is increased, and so is the duration of hospitalization in older individuals, involving a substantially increased cost per infection. Furthermore, hospitalization of older individuals is associated with increased risk of functional dependence that may increase the cost of treatment due to expensive home care and rehabilitation. In at least four studies, hematopoietic growth factors reduced the risk of neutropenia and neutropenic infection by 32% to 83% in older patients with large-cell non-Hodgkins lymphomas. The National Comprehensive Cancer Network advisory panel for the guidelines for the management of older individuals has unanimously recommended that hematopoietic growth factors be used routinely in persons aged 70 and older who are receiving moderately toxic chemotherapy.
References
Balducci L, Lyman GH. Patients aged > or = 70 are at high risk for neutropenic infection and should receive hemopoietic growth factors when treated with moderately toxic chemotherapy. J Clin Oncol. 2001;19:1583-1585.
Gomez H, Hidalgo M, Casanova L, et al. Risk factors for treatment-related death in elderly patients with aggressive non-Hodgkin's lymphoma: results of a multivariate analysis. J Clin Oncol. 1998;16:2065-2069.
141. Older patients are at higher risk than younger patients for first-cycle FN Key Point:
Elderly patients are at a higher risk for FN in the first chemotherapy cycle than younger patients.
Background:
Lyman et al conducted a retrospective analysis of data from 577 patients with NHL who were treated with CHOP at 1 of 12 community or academic oncology practices between 1991 and 1999.
Twenty-eight percent of all patients in the analysis experienced an FN event.
Patients age ? 65 years represented 50% of all patients, but accounted for 62% of FN events.
Older patients with NHL had a greater risk of FN, even after adjustment for dose intensity and comorbidities.
The time to the first FN event was shorter in patients aged 65 years or older (P = 0.0002).
Lyman GH, Morrison VA, Dale DC, et al. Risk of first febrile neutropenia among patients receiving CHOP chemotherapy. �Proc Am Soc Clin Oncol. 2002;21:358a. Abstract 1430.Key Point:
Elderly patients are at a higher risk for FN in the first chemotherapy cycle than younger patients.
Background:
Lyman et al conducted a retrospective analysis of data from 577 patients with NHL who were treated with CHOP at 1 of 12 community or academic oncology practices between 1991 and 1999.
Twenty-eight percent of all patients in the analysis experienced an FN event.
Patients age ? 65 years represented 50% of all patients, but accounted for 62% of FN events.
Older patients with NHL had a greater risk of FN, even after adjustment for dose intensity and comorbidities.
The time to the first FN event was shorter in patients aged 65 years or older (P = 0.0002).
Lyman GH, Morrison VA, Dale DC, et al. Risk of first febrile neutropenia among patients receiving CHOP chemotherapy. Proc Am Soc Clin Oncol. 2002;21:358a. Abstract 1430.
142. Incidence of Febrile Neutropenia: Primary Prophylaxis Effective
The p-value for the incidence of FN in cycle 1 is significant and is 0.006.
Primary Endpoint
Over all cycles, the percentage of patients experiencing febrile neutropenia was statistically significantly lower for patients receiving pegfilgrastim in all cycles compared with patients receiving no pegfilgrastim in cycle 1
The p-value for the incidence of FN in cycle 1 is significant and is 0.006.
Primary Endpoint
Over all cycles, the percentage of patients experiencing febrile neutropenia was statistically significantly lower for patients receiving pegfilgrastim in all cycles compared with patients receiving no pegfilgrastim in cycle 1
143. Conclusion Society has treated the elderly poorly even when curative therapy exists
Less surgery
Lower use of chemotherapy
Less chemotherapy
Older patients can tolerate standard therapy
Under treatment results in lower benefit
Need to provide better supportive care
Improvements in patient assessment needed
144. Clinical Trials
145. Overcoming Barriers Focus trial on elderly
Reasonable regimens
Keep it simple
Relax eligibility: let Doctor/Patient decide
Make consent process easier
Arrange transportation
HCFA to pay for routine care on trial
Physician Education
146. Conclusion (I) Will the patient die of cancer or with cancer?
Will the patient suffer cancer-related morbidity?
What is the effectiveness of the therapy?
Is the patient able to handle the toxicity of treatment?
Will dependency be increased?
What is the goal?
147. Conclusion (II) Elderly specific cancer trials are needed
Avoid subset analysis in which elderly participation is minimal
148. Conclusion (III) Studies should include (cont):
Some form of geriatric assessment should be performed
Current standards time consuming
New methodology
Self-assessment
Comorbidity and functional assessment
Quality of life evaluation
149. Conclusion (IV) Studies should emphasize particular aspects of aging, i.e. frailty, vulnerable elderly, well elderly
Functional testing: VES-13
Predictive laboratory testing
Appropriate endpoints
Survival may not be most important
TTP, QOL, etc.
Pharmacology
