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TOTAL BODY
IRRADIATION
BASIL PAUL SUNNY
RADIOTHERAPIST
INTRODUCTION
• TBI started using in 1956 by Dr. Donnall
Thomas to treat patients with end stage
leukemia
• He was awarded Nobel prize for medicine in
1990
• Rationale for use of TBI not changed
• Tremendous change in
 Delivery of TBI
 Radiation sources used – Co^60 / LINAC
 Dose measure techniques- more reliable and accurate rather
than erythema dose for determination of dose delivered
INTRODUCTION
• One of main component in interdisciplinary
treatment of hematological malignancies-
leukemia, lymphoma, rarely solid tumors
• Enables myeloablative high dose therapy
(HDT) & immunoablative conditioning therapy
prior to stem cell transplantation
TASKS OF TBI
• Eradicating diseased marrow
• Reducing tumor burden
• Immunosuppression- lymphocyte elimination to
allow grafting of donor bone marrow
• Deplete the BM to allow physical space for
engraftment of healthy donor marrow
• Eradication of cells with genetic disorders-
Fanconi’s anemia, thalassemia major, Wiskott- Aldrich
syndrome
TBI IN CONDITIONING REGIMENS
MALIGNANT
1. LUKEMIAS,
ACUTE MYELOID LUKEMIA (AML)
ACUTE LYMPHOBLASTIC LUKEMIA (ALL)
CHRONIC MYELOID LUKEMIA (CML)
HAIRY CELL LUKEMIA
2. LYMPHOMAS/ MYELOPROLIFERATIVE DISORDERS
NON HODGKINS LYMPHOMAS
REFRACTORY HODGKINS DISEASES
MYELODYSPLASIA
MULTIPLE MYELOMA
TBI IN CONDITIONING REGIMENS
• PEDIATRIC SOLID TUMORS
NEUROBLASTOMA
EWINGS SARCOMA
• ADULT SOLID TUMORS
SMALL CELL OF LUNG
TESTICULAR CARCINOMA
TBI IN CONDITIONING REGIMENS
• NON MALIGNANT CONDITIONS
IMMUNE DISORDERS
APLASTIC ANEMIA
GENETIC DISORDERS
WISKOTT AIDRICH SYNDROME
OSTEOPETEROSIS
TAR SYD
FANCONI ANEMIA
CURRENT INDICATIONS
• HIGH RISK AML/CML IN FIRST REMISSION
• SECOND REMISSION AML
• SECOND REMISSION ALL IF THERE IS HLA COMPATIBLE SIBLING
DONOR
• FIRST REMISSION ALL WITH CNS INVOLVEMENT / PH
CHROMOSOME POSTIVITY
• LOW GRADE LYMPHOMA AFTER CHEMO FAILURE
• CHILDHOOD AML/ ALL IN SECOND / SUBSEQUENT
REMISSIONS
ADVANTAGES
• No sparing of sanctuary sites (testis, brain)
• Dose homogeneity regardless of blood supply
• Independent of hepatic & renal functions
• No problems with excretion or detoxification
• Ability to tailor the dose distribution by
shielding specific organs or by boosting sites
DISADVANTAGES
• Potential late side effects
Sterility
Cataract
Growth retardation
Neurological toxicity
• Patient body contour irregularities causes
adding of compensators
PRE- REQUISITES FOR TBI
• Medical history and evaluation
• Interdisciplinary approach from doctors and
health professionals
• RT & BM transplantation facility must be in
same center
• Conditions with a low risk of infections is
recommended
PHYSICAL EXAMINATION
• Evaluation of oral cavity and dentition
• Neurological evaluation
• PS
• Organ function analysis
CCT> 60 ml/min
AST / ALT < twice the upper level of normal
PFT
EF> 40%
• Infectious disease evaluation
• Sperm banking
TECHNIQUES OF TBI
• Patient comfort and Reproducibility
• Position of patient and stability
• The common factor in the different techniques of TBI
is to deliver the prescribed dose of radiation to the
entire body in uniformity of +/-10% of the
prescription dose. +/-5% considered as the best.
IMPORTANT CRITERIAS
BILATERAL TBI
BILATERAL TBI
• Designed by Khan et al
• Patient sitting or lying down on a couch
Good Patient comfort
Less homogeneous dose distribution due to variable body
thickness, needs compensating blocks.
AP-PA TBI
AP-PA TBI
• Irradiated anteroposteriorly by parallel opposed
fields while positioned upright several meters from
the source
• More homogeneous dose distribution
• The principle of the technique is that the standing
TBI allows shielding of certain critical organs from
photons and boosting of superficial tissues in the
shadow of the blocks with electrons
OTHER TBI TECHNIQUES
MODIFIED CONVENTIONAL MACHINES
• Large stationary Beam , stationary patient
Extended SSD technique
Collimator removal method
• Moving techniques
Translational beam method
Sweeping beam method
McGill UNIVERSITY
SWEEPING BEAM TECHNIQUE
TBI: McGill TECHNIQUE
TBI-IRRADIATION METHODS
TRANSLATIONAL COUCH
Computer controlled
POSITION
• Patient lies supine
Length of patient - not more than 140 cm
 If length greater than 140 cm – legs folded
with pillow tucked b/n both legs
• Arms flexed and placed near to chestwall
• Knees adjoined together, wrapped
• Positioned at extended SSD of 300 cm
40 x 40 cm FieldSize,
Gantry 90, Collimation 45
Measurements
Skull
Neck
Shoulder
Chest
Abdomen
Thigh
Knee
Calf
Ankle
TARGET VOLUME
• All malignant cells including those circulating
• whole cellular immune system
• The Whole Body, including Skin
DOSE PRESCRIPTION
• High Dose TBI – 13.2 Gy in 6 fractions over 3 days
• Standard dose TBI – 12 Gy in 6 fractions over 3
days
• Low dose TBI – 2 Gy in single fraction
• Lung is the dose-limiting organ (maximum 10 Gy).
DOSE REFERENCE POINTS
• The dose reference point is defined
at mid abdomen at the height of the umbilicus
according to an international consensus
TREATMENT DELIVERY
• Delivered in the position which measurements
are taken
• Under sterile conditions
OPTIMIZATION OF DOSE
• The homogeneity of dose in the target volume
• The effective sparing the lungs
DOSE VERIFICATION
• In vivo dosimetry is done with Semiconductor
diodes, mosfet, LiF TLD chips
• It is placed for skull, H&N , mediastinal regions
1. COMPENSATORS
• Influences of irregular body contours have
to be compensated.
• Tissue compensators are used in
Head and neck region
Lower extremities and
Lungs (Not required usually as effective thickness at
mid mediastinum is greater than at umbilicals. Arms positioned
inline with lungs and increase total thickness)
TBI AAPM Report 17
2. BEAM SPOILER
Skin/ surface doses in
Megavoltage beams is less
than D max
Beam spoiler has to be
positioned close to the
patient, For build-up the
surface dose up to at least
90% of the prescribed dose
1-2 cm thick acrylic is
sufficient to meet these
requirements
.
3. DOSE HOMOGENIZATION in parts of the
target volume with reduced dose :
• Thoracic wall receives a lower dose due to
lung shielding.
• Additional irradiation however is not used
• Electron boost can be given if necessary
ACUTE COMPLICATIONS
• Nausea& Vomiting
• Headache
• Fatigue
• Ocular dryness
• Esophagitis
• Loss of apetite
• Erythema/hyperpigmentation
• Mucositis
• Diarrhea
• Fever
CHRONIC COMPLICATIONS
• Ocular – Cataract, dryness, keratitis
• Salivary glands – Xerostomia, dental caries, tooth
abnormalities
• Pneumonitis or pulmonary fibrosis
• Hepatotoxicity
• Radiation nephropathy
• Growth abnomalities in children
• Sterility and endocrine abnormalities
• Secondary mets
Targeted TBI – TMI and TMLI
• Total marrow irradiation - skeletal bone.
Conditioning regimen for multiple myeloma
• Total marrow and lymphoid irradiation (TMLI)
- bone, major lymph node chains, liver,
spleen, and sanctuary sites, such as brain.
Conditioning regimen for myeloid and
lymphoid leukemia
TOMOTHERAPY
• Desirable to deliver radiation only to immune
organs and bone marrow spaces sparing
sensitive structures like brain, lens, lungs,
kidneys
• IMRT planning could accomplish this, but
most systems are limited by field size issues
• Accurate IMRT depends on reproducible
patient position, which is complicated when
considering treating the entire marrow spaces
TOMOTHERAPY
• Tomotherapy - linear accelerator mounted in
head of a spiral CT unit
• IMRT delivered as beams spiral down axis of
patient supine on treatment couch
• The beams can be planned to deliver dose to
bones and bone marrow, liver and spleen as
well as major nodal groups and to relatively
spare the lungs and kidneys
TOMOTHERAPY ISODOSE
DISTRIBUTION
THANK YOU

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Total body irradiation

  • 1. TOTAL BODY IRRADIATION BASIL PAUL SUNNY RADIOTHERAPIST
  • 2. INTRODUCTION • TBI started using in 1956 by Dr. Donnall Thomas to treat patients with end stage leukemia • He was awarded Nobel prize for medicine in 1990 • Rationale for use of TBI not changed • Tremendous change in  Delivery of TBI  Radiation sources used – Co^60 / LINAC  Dose measure techniques- more reliable and accurate rather than erythema dose for determination of dose delivered
  • 3. INTRODUCTION • One of main component in interdisciplinary treatment of hematological malignancies- leukemia, lymphoma, rarely solid tumors • Enables myeloablative high dose therapy (HDT) & immunoablative conditioning therapy prior to stem cell transplantation
  • 4. TASKS OF TBI • Eradicating diseased marrow • Reducing tumor burden • Immunosuppression- lymphocyte elimination to allow grafting of donor bone marrow • Deplete the BM to allow physical space for engraftment of healthy donor marrow • Eradication of cells with genetic disorders- Fanconi’s anemia, thalassemia major, Wiskott- Aldrich syndrome
  • 5. TBI IN CONDITIONING REGIMENS MALIGNANT 1. LUKEMIAS, ACUTE MYELOID LUKEMIA (AML) ACUTE LYMPHOBLASTIC LUKEMIA (ALL) CHRONIC MYELOID LUKEMIA (CML) HAIRY CELL LUKEMIA 2. LYMPHOMAS/ MYELOPROLIFERATIVE DISORDERS NON HODGKINS LYMPHOMAS REFRACTORY HODGKINS DISEASES MYELODYSPLASIA MULTIPLE MYELOMA
  • 6. TBI IN CONDITIONING REGIMENS • PEDIATRIC SOLID TUMORS NEUROBLASTOMA EWINGS SARCOMA • ADULT SOLID TUMORS SMALL CELL OF LUNG TESTICULAR CARCINOMA
  • 7. TBI IN CONDITIONING REGIMENS • NON MALIGNANT CONDITIONS IMMUNE DISORDERS APLASTIC ANEMIA GENETIC DISORDERS WISKOTT AIDRICH SYNDROME OSTEOPETEROSIS TAR SYD FANCONI ANEMIA
  • 8. CURRENT INDICATIONS • HIGH RISK AML/CML IN FIRST REMISSION • SECOND REMISSION AML • SECOND REMISSION ALL IF THERE IS HLA COMPATIBLE SIBLING DONOR • FIRST REMISSION ALL WITH CNS INVOLVEMENT / PH CHROMOSOME POSTIVITY • LOW GRADE LYMPHOMA AFTER CHEMO FAILURE • CHILDHOOD AML/ ALL IN SECOND / SUBSEQUENT REMISSIONS
  • 9. ADVANTAGES • No sparing of sanctuary sites (testis, brain) • Dose homogeneity regardless of blood supply • Independent of hepatic & renal functions • No problems with excretion or detoxification • Ability to tailor the dose distribution by shielding specific organs or by boosting sites
  • 10. DISADVANTAGES • Potential late side effects Sterility Cataract Growth retardation Neurological toxicity • Patient body contour irregularities causes adding of compensators
  • 11. PRE- REQUISITES FOR TBI • Medical history and evaluation • Interdisciplinary approach from doctors and health professionals • RT & BM transplantation facility must be in same center • Conditions with a low risk of infections is recommended
  • 12. PHYSICAL EXAMINATION • Evaluation of oral cavity and dentition • Neurological evaluation • PS • Organ function analysis CCT> 60 ml/min AST / ALT < twice the upper level of normal PFT EF> 40% • Infectious disease evaluation • Sperm banking
  • 13. TECHNIQUES OF TBI • Patient comfort and Reproducibility • Position of patient and stability • The common factor in the different techniques of TBI is to deliver the prescribed dose of radiation to the entire body in uniformity of +/-10% of the prescription dose. +/-5% considered as the best. IMPORTANT CRITERIAS
  • 14.
  • 16. BILATERAL TBI • Designed by Khan et al • Patient sitting or lying down on a couch Good Patient comfort Less homogeneous dose distribution due to variable body thickness, needs compensating blocks.
  • 18. AP-PA TBI • Irradiated anteroposteriorly by parallel opposed fields while positioned upright several meters from the source • More homogeneous dose distribution • The principle of the technique is that the standing TBI allows shielding of certain critical organs from photons and boosting of superficial tissues in the shadow of the blocks with electrons
  • 19. OTHER TBI TECHNIQUES MODIFIED CONVENTIONAL MACHINES • Large stationary Beam , stationary patient Extended SSD technique Collimator removal method • Moving techniques Translational beam method Sweeping beam method
  • 24. POSITION • Patient lies supine Length of patient - not more than 140 cm  If length greater than 140 cm – legs folded with pillow tucked b/n both legs • Arms flexed and placed near to chestwall • Knees adjoined together, wrapped • Positioned at extended SSD of 300 cm
  • 25. 40 x 40 cm FieldSize, Gantry 90, Collimation 45
  • 27. TARGET VOLUME • All malignant cells including those circulating • whole cellular immune system • The Whole Body, including Skin
  • 28. DOSE PRESCRIPTION • High Dose TBI – 13.2 Gy in 6 fractions over 3 days • Standard dose TBI – 12 Gy in 6 fractions over 3 days • Low dose TBI – 2 Gy in single fraction • Lung is the dose-limiting organ (maximum 10 Gy).
  • 29. DOSE REFERENCE POINTS • The dose reference point is defined at mid abdomen at the height of the umbilicus according to an international consensus
  • 30. TREATMENT DELIVERY • Delivered in the position which measurements are taken • Under sterile conditions
  • 31. OPTIMIZATION OF DOSE • The homogeneity of dose in the target volume • The effective sparing the lungs
  • 32. DOSE VERIFICATION • In vivo dosimetry is done with Semiconductor diodes, mosfet, LiF TLD chips • It is placed for skull, H&N , mediastinal regions
  • 33. 1. COMPENSATORS • Influences of irregular body contours have to be compensated. • Tissue compensators are used in Head and neck region Lower extremities and Lungs (Not required usually as effective thickness at mid mediastinum is greater than at umbilicals. Arms positioned inline with lungs and increase total thickness)
  • 35. 2. BEAM SPOILER Skin/ surface doses in Megavoltage beams is less than D max Beam spoiler has to be positioned close to the patient, For build-up the surface dose up to at least 90% of the prescribed dose 1-2 cm thick acrylic is sufficient to meet these requirements .
  • 36. 3. DOSE HOMOGENIZATION in parts of the target volume with reduced dose : • Thoracic wall receives a lower dose due to lung shielding. • Additional irradiation however is not used • Electron boost can be given if necessary
  • 37. ACUTE COMPLICATIONS • Nausea& Vomiting • Headache • Fatigue • Ocular dryness • Esophagitis • Loss of apetite • Erythema/hyperpigmentation • Mucositis • Diarrhea • Fever
  • 38. CHRONIC COMPLICATIONS • Ocular – Cataract, dryness, keratitis • Salivary glands – Xerostomia, dental caries, tooth abnormalities • Pneumonitis or pulmonary fibrosis • Hepatotoxicity • Radiation nephropathy • Growth abnomalities in children • Sterility and endocrine abnormalities • Secondary mets
  • 39. Targeted TBI – TMI and TMLI • Total marrow irradiation - skeletal bone. Conditioning regimen for multiple myeloma • Total marrow and lymphoid irradiation (TMLI) - bone, major lymph node chains, liver, spleen, and sanctuary sites, such as brain. Conditioning regimen for myeloid and lymphoid leukemia
  • 40. TOMOTHERAPY • Desirable to deliver radiation only to immune organs and bone marrow spaces sparing sensitive structures like brain, lens, lungs, kidneys • IMRT planning could accomplish this, but most systems are limited by field size issues • Accurate IMRT depends on reproducible patient position, which is complicated when considering treating the entire marrow spaces
  • 41. TOMOTHERAPY • Tomotherapy - linear accelerator mounted in head of a spiral CT unit • IMRT delivered as beams spiral down axis of patient supine on treatment couch • The beams can be planned to deliver dose to bones and bone marrow, liver and spleen as well as major nodal groups and to relatively spare the lungs and kidneys