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THYROID
MALIGNANCIES
+ LT COL VIPIN V NAIR
+ ASSO PROF AND PLASTIC SURGEON
+ AFMC PUNE
THYROID
MALIGNANCIES
Dr VIPIN V NAIR
ASSO PROF SURGERY AND PLASTIC SURGEON
AFMC PUNE
INTRODUCTION
 Most common endocrine tumor (95%)
 Female to male ratio- 3:1
 Differentiated
carcinomas peak in 3rd
and 4th decade.
 Medullary Ca thyroid
peaks in 5th and 6th
decade.
 Anaplastic carcinomas
peak in 7th decade.
Long term
survival.
EPIDEMIOLOGY
 Indian population - thyroid cancer forms 1.5%
of all malignant tumours
 Papillary thyroid carcinoma: Iodine sufficient
areas
 Follicular thyroid carcinoma: Iodine deficient
areas
DUNHILL CLASSIFICATION
DIFFERENTIATED – arise from Follicular cells
• Papillary carcinoma (60 - 70%)
• Follicular carcinoma (10%)
• Papillo-follicular variant
• Hurthle cell carcinoma
UNDIFFERENTIATED
Anaplastic carcinoma (10%) – arise from
undifferentiated follicular cells
CLASSIFICATION
• MEDULLARY CARCINOMA (5%) –
arise from parafollicular cells
• MALIGNANT LYMPHOMA (5%) –
arise from lymphoid cells
• SECONDARIES TO THYROID (RARE) –
kidney, breast, direct invasion from
aero-digestive tract squamous cell
carcinoma
WHO Classification
Adenomas
A. Follicular
1. Colloid variant
2. Embryonal
3. Fetal
4. Hurthle cell variant
B. Papillary (probably malignant)
C. Teratoma
Malignant
Malignant
A)Differentiated
1.Papillarycarcinoma(and variants)
2.Follicularcarcinoma(variants)
a.Minimallyinvasive b.Extensivelyinvasive
B)Medullary carcinoma
C)Undifferentiated
1.Giantcell 2.Carcinosarcoma
D)Miscellaneous
1.Lymphoma,sarcoma 4.Mucoepithelialcarcinoma
2.Squamouscellepidermoidcarcinoma 5.Metastatictumor
3.Fibrosarcoma
AGE RELATED PREVALENCE
Carcinoma Age group
a) Papillary Thyroid carcinoma
b) Medullary thyroid carcinoma associated with
MEN type 2
Children
a) Follicular thyroid carcinoma
b) Anaplastic carcinoma
c) Sporadic Medullary thyroid carcinoma
Elderly
THYROID CANCERS IN YOUNG AGE
 Papillary carcinoma: most common
 Radiation related
 More chances of multifocality
 More aggressive ??
 Extra-thyroid extension: more likely
 60%-80%: lymph node metastasis
 Lung metastasis(10%)
 Recurrence risk: 10% to 35%
 Mortality rate: 3 to 5 %
ETIOLOGY
Thyroid lymphomas: Intra-thyroid lymphoid tissue
Sarcomas: Connective tissue of thyroid gland
Endodermally derived
Follicular cells
• Papillary
• Follicular
• Anaplastic
Neuroendocrine derived
calcitonin producing C cells
• Medullary
Thyroid cancers arise from 2 types of cells
1) Radiation Exposure
 Papillary Carcinoma
Differentiated carcinoma – Irradiation under 5 years of age
 Prior neck irradiation early in life
 Treatment for acne, tonsillitis (200-150 cGy)
 Treatment for malignancies: Hodgkin’s (4000 cGy)
 Nuclear holocausts/ accidents
 Chernobyl incident (Ukraine 1986): 100 times increase
 Long latency period: 20 to 30 yrs
2) Pre-existing
Thyroid Lesions
 Pre-existing MNG: Follicular carcinoma
 SNT (esp. old age, males and in extremes of
age)
 Hashimoto’s thyroiditis: Papillary thyroid
carcinoma
 Any solitary nodule ~ 5% chances of
malignancy
 Solitary nodules with definite h/o radiation
exposure: 30 % chances of malignancy
FAMILIAL CANCER SYNDROMES
• Medullary carcinoma: Multiple
endocrine neoplasia (MEN) 2A or
2B syndrome, as well as familial
MTC (FMTC) syndrome
 4-10 times increased risk in 1st degree relatives
SYNDROMES
THYROID CANCERS
Cowden’s syndrome FTC and rarely PTC and
Hurthle cell tumors
FAP PTC
Werner’s syndrome PTC, FTC, Anaplastic Cancer
Carney complex type 1 PTC, FTC
McCune Albright
syndrome
PTC Clear cell
CLINICAL
PRESENTATION
 Commonest
presentation: painless
thyroid swelling
Patients with MTC may
complain of a dull
aching sensation
Presentation s/o malignancy –
Recent onset pain
Recent rapid enlargement in a long
standing nodule
Dysphagia
Stridor
Hemoptysis
Hoarseness
WORKUP
 H/o risk factors (radiation, family history)
 Examination findings
 Firmness (hard, gritty usually s/o
malignancy)
 Mobility/ adherence to surrounding
structures
 Presence of LNpathy
 Berry’s sign
 IDL for vocal cord assessment
 USG Neck followed by FNAC
LABORATORY
INVESTIGATIONS
Serum TSH levels
 Low TSH - autonomously functioning nodule
(usually benign)
 Does not rule out malignancy (1% risk)
Serum calcitonin levels (MTC or MEN 2)
 Highly suggestive of MTC if raised
PCR assays for germline mutations in the RET proto-
oncogene
 Diagnostic in Familial MTC
Serum CEA level
 Increased in MTC but nonspecific
 Better indicator of prognosis than Calcitonin
IMAGING STUDIES
ULTRASONOGRAPHY
 Highly sensitive for
thyroid nodules
 Can detect sub-
clinical/small nodules
 Differentiate solid from
cystic
 Detect sub-clinical
cervical
lymphadenopathy
TI-RADS
BETHESDA CRITERIA
 Accuracy of FNAC: 70 – 97 %
 False Negatives: 1 – 6 %
 Chances of malignancy in:
i. FLUS – 10 – 35 %
ii. AUS – 60 – 75 %
 Suspicious for malignancy : 60 %
turn out to be malignant
 Malignant : 97 % are malignant
Despite negative aspirate
thyroidectomy indicated if
large, hard nodule fixed to
surrounding structures
FROZEN SECTION
Lobectomy ???
RADIO IODINE STUDIES
 Recommended in patients having
Follicular neoplasm on FN and
suppressed TSH
 Determine functional status of a nodule
Based on radioisotope studies nodule
can be
 Hot - Autonomous toxic nodule
 Warm - Normally functioning
 Cold - Non functioning nodule (likely
malignant but not always)
Thyroid scintigraphy Indium-111 octreotide scan for MTC
X-rays : CXR and X-ray skull to rule out metastatic deposits
COLD NODULE
THYROID SCANS
STAGING
PAPILLARY THYROID
CARCINOMA
CHARACTERISTIC
FEATURES
 60%-80% of all thyroid malignancies
 Found in iodine-sufficient areas
 Predominant in children and radiation exposed cases
 Females : Males = 2:1 (most euthyroid)
 Mean age at presentation 30-40 yrs
 Lymphatic spread commoner (mode of presentation in
many)
 Distant mets: upto 20 % cases (lungs > bone > liver > brain)
 Lateral aberrant thyroid: metastatic spread to cervical LN
 Multifocality common (upto 85%)
DIAGNOSIS
AND PRE-OP
WORK UP
 ORPHAN ANNIE NUCLEI: intra-nuclear cytoplasmic
inclusions
 Papillary projections: characteristic
 Mixed pattern/ follicular pattern (follicular variant)
 Follicular variant: behave biologically like papillary
 Psammoma bodies
 BRAF mutations
DIAGNOSIS AND PRE-OP WORK UP
 Basis of diagnosis: FNAC of thyroid mass/ LN mass
 Complete USG Neck:
 Contralateral lobe
 LN stations
 If suspected clinically: metastatic workup
 Prognostic scores
PROGNOSTIC MARKERS
LN involvement does not alter the
prognosis/survival rates
Predicts local recurrence All scoring systems categorize the
patient as
High risk
Low risk
SURGICAL MANAGEMENT
 CURRENT GUIDELINES: Near- total or total thyroidectomy for primary cancers >1 cm
(Unless surgery is contraindicated)
 Reduced recurrence rates
 Improved survival rates
 MRND type III: in case of proven lateral lymph node involvement
 No role of prophylactic lateral neck node dissection, micro-mets can be addressed by
RAI therapy
ARGUMENTS IN
FAVOR OF TOTAL
THYROIDECTOMY
SURGICAL MANAGEMENT
 Hemithyroidectomy is considered sufficient in cases of:
 Small tumours (<1 cm)
 Incidentally discovered/ low-risk/ unifocal/ intrathyroidal papillary ca
 Absence of prior head and neck irradiation
 Absence of radiologically/clinically involved cervical LN mets
 FNAC suspicious for papillary Ca: Hemithyroidectomy + removal of adjacent nodes
 If frozen-section of lymph node or tumor confirms carcinoma:
 Completion total or near-total thyroidectomy is performed
 Completion thyroidectomy can be performed at a later setting based on HPE
SURGICAL MANAGEMENT
Large/ Locally aggressive/ Metastatic tumours
 Total thyroidectomy + excision of adjacent involved structures + appropriate nodal
surgery
 Followed by radio-ablation
 Along with long term TSH suppression
LOW RISK GROUP
MICROPAPILLARY OR OCCULT MICRO CA
 “Micropapillary carcinoma is a tumour, clinically not detectable or less than 1cm with no
evidence of local invasion through the thyroid capsule or angioinvasion”
 Size criterion < 1.0 cm
 Usually clinically silent, more indolent than macro type
 Most are found incidentally at HPE/ autopsy
 25 % associated with occult LN mets
VARIANTS
1. Follicular variant
2. Encapsulated
3. Diffuse Sclerosing
4. Diffuse Follicular
5. Tall cell
6. Columnar cell
7. Oxyphilic (Oncocytic, Hürthle Cell)
8. Warthin Tumor-like
9. Cribriform-Morular Variant
10. Trabecular
11. Adenoid Cystic Carcinoma–like
12. Macrofollicular
13. Clear cell
14. Hobnail
15. Micropapillary
16. Variant with Spindle Cell Metaplasia.
17. Variant with Exuberant Nodular
Fasciitis–like Stroma
18. Papillary Carcinoma with
Lipomatous Stroma
19. Dedifferentiated Papillary
FOLLICULAR VARIANT
 Lindsay tumor
 Psammoma bodies and sclerosis may be present
 Diagnosis rests on identification of the typical nuclear features of papillary carcinoma
 Further divided into two subtypes:
 Infiltrative (non-encapsulated)
 Encapsulated
FOLLICULAR THYROID
CARCINOMA
Follicular Carcinoma vs Follicular Adenoma
 Unequivocal vascular and/or capsular invasion: follicular carcinoma
 Examination of the tumor-thyroid interface
 Histologic examination features favoring follicular Ca:
 Thick fibrous capsule
 High cellularity, with solid or trabecular growth pattern
 Diffuse nuclear atypia
 Readily identified mitotic figures
CHARACTERISTIC FEATURES
 10% of all thyroid ca
 More common in iodine deficient areas
 Female : Male = 3:1
 Presentation at older age: 5th decade
 Cervical LN uncommon at presentation
 Haematogenous spread more common
CHARACTERISTIC
FEATURES
 Usual presentation:
 SNTs: recent rapid increase in size
 Long standing MNG
 Rarely present as thyrotoxicosis (hyper-functioning
nodule)
 Indicators of malignancy in cases with FNAC
showing follicular features
 Distant mets
 Large tumours >4 cm in old males
 Bony mets: typically vascular/warm/pulsatile.
Commonly in skull, long bones, ribs
DISTANT METS IN FOLLICULAR CA
PATHOLOGICAL FEATURES
 Usually solitary lesions
 Majority are encapsulated
 Minimally invasive tumours: microscopic capsular invasion, no parenchymal invasion
 Widely invasive tumours – widespread capsular invasion, e/o large vessel invasion
 Tumor thrombi a characteristic feature
 Due to limitations of FNAC: Novel genetic markers
BRAF, RAS, RET/PTC, MicroRNA 197, 346
SURGICAL MANAGEMENT
 Follicular lesion on FNAC:Hemithyroidectomy (80% adenomas)
 If HPE shows follicular Ca: Completion thyroidectomy
 Total thyroidectomy indications:
 Older patients
 Lesion >4cm ( cancer risk is 50%)
 Atypia on FNAC
 Family history of thyroid cancer
 History of radiation exposure
 Total thyroidectomy advocated mainly because RAI can be used to eliminate residual/
metastatic disease
NECK DISSECTION
 Occasional spread to cervical lymph nodes (10%)
 Prophylactic nodal dissection not indicated
 Proven nodal metastases: therapeutic neck dissection recommended
 Prophylactic central neck dissection may be considered in patients
with large tumors >4 cm
PROGNOSIS: FOLLICULAR CA
 The approximate cumulative mortality
 15% at 10 years
 30% at 20 years
 Poor long-term prognosis predicted by:
1. Age >50 years at presentation
2. Tumor size >4 cm
3. Higher tumor grade
4. Marked vascular invasion
5. Extra-thyroidal invasion
6. Distant metastases at time of diagnosis
HÜRTHLE CELL VARIANT
 Oncocytic, Oxyphilic, Ashkenazy cell neoplasms (3%)
 Subtype of follicular Ca, cannot be diagnosed on FNAC
 Differs from classical Follicular Ca:
 More often multifocal and bilateral (about 30%)
 Usually does not take up RAI (about 5%)
 More likely to metastasize to local nodes (25%) and have distant mets at
presentation
 Higher mortality rate (about 20% at 10 years)
HÜRTHLE CELL VARIANT
 Routine central neck node dissection recommended
 MRND if lateral neck nodes are positive (palpable/ USG)
 Radio-iodine scanning & ablation usually ineffective
 Should still be considered to ablate residual thyroid tissue and
occasionally ablate tumors as there is no other good therapy
POST OPERATIVE MANAGEMENT OF DTC
RADIOIODINE THERAPY
RAI ablation indications:
 All patients with stage III and IV disease
 All Patients with stage II disease <45 years
 Stage I disease with aggressive histology or size >1.5 cm
 Nodal mets
 Multifocal disease
 Extra-thyroidal or vascular invasion
RADIOIODINE THERAPY
 More sensitive than X-ray/ CT in detecting metastatic/ residual ca
 6 weeks after thyroidectomy, hypothyroid can be induced by discontinuing replacement to obtain
high serum TSH levels (30mU/L)
 Diagnostic dose of I131 or I123 is given initially (1-3 mCi)
 Whole-body scanning is performed to detect uptake of radioiodine
 If any normal thyroid remnant or metastatic disease detected, therapeutic dose of I131 is
administered to ablate the tissue
 Low-dose ablation (OPD Basis) - <30mCi (low risk cases)
 High doses (100 – 200 mCi) for high risk, old age, incomplete resection
RADIOIODINE THERAPY
FOLLOW-UP
Unstimulated - cut-off 0.5 ng
TSH SUPPRESSION THERAPY
 High risk patients maintained at serum TSH level <0.1 mU/L
 Low risk cases 0.1 – 0.5 mU/L (equivocal opinion based on recent trials)
 Suppressive dose is 0.3 mg OD lifelong (titration required)
 Reduces tumoral growth and recurrence rates
MEDULLARY CARCINOMA THYROID
MEDULLARY CARCINOMA
 Para-follicular C-cell derivative
 UB bodies, neuro-ectodermal origin (4th pharyngeal pouch)
 5% of all thyroid ca
 Concentrated supero-laterally on thyroid lobes
 Most MTCs: sporadic
 25 % - syndromic (MEN2A, MEN2B, familial MTC)
 Hereditary forms - germline mutation of the RET proto-oncogene
 C cell hyperplasia (pre-malignant): familial cases
FEATURES OF
MEDULLARY
THYROID
CANCER
SYNDROMES
Syndrome Manifestations
MEN2A MTC, pheochromocytoma, primary
hyperparathyroidism, lichen planus
amyloidosis
MEN2B (MOST
AGGRESSIVE)
MTC, pheochromocytoma, Marfanoid
habitus,
mucocutaneous ganglioneuromatosis
Familial MTC MTC
MEN2A and
Hirschsprung’s
disease
MTC, pheochromocytoma, primary
hyperparathyroidism, Hirschsprung's
disease
MEDULLARY
CARCINOMA
Presentation-
1. Thyroid mass with palpable cervical LN (~20%)
2. Aching type pain
3. Locally invasive symptoms - dysphagia, hoarseness,
dyspnoea
4. Diarrhea (40%)
 Hematogenous metastases (liver, bone), late feature
 Female : Male = 1.5 : 1
 Secrete Calcitonin, CEA, serotonin, PG, other peptides
 Sporadic cases – 80 % unilateral
 Familial cases – 90 % multicentric / Bilateral
MTC –
DIAGNOSIS
Histological feature – marked heterogeneity, amyloid
(diagnostic)
IHC – Calcitonin/ CEA / Calcitonin-gene related peptide
All fresh cases – screened for PHT, phaeochromocytoma,
RET point mutations
Provocative tests – pentagastrin-stimulated calcitonin
level
Calcitonin & CEA – markers for persistence/recurrence
Calcitonin – more sensitive marker
CEA – better predictor of prognosis
NECK USG – central/ lateral neck compartments, superior
mediastinum
MTC –
METASTATIC
WORK-UP
Metastatic work-up indicated in cases with:
Palpable/ USG proven positive node
Calcitonin level >400ng/mL
CECT Neck + Chest
Triple-phase CT for liver metastases
MTC – MANAGEMENT
 Total thyroidectomy + bilateral central neck node dissection treatment of choice because:
 Radio-Iodine ablation usually ineffective
 High incidence of multicentricity
 Palpable cervical lymph nodes: MRND
 Tumour >1.5 cm: Ipsilateral prophylactic MRND
 If node positive then contralateral node dissection
 If phaeochromocytoma present: operated first
MTC – MANAGEMENT
 In unresectable/ metastatic/ locally recurrent disease
tumour debulking surgery indicated to alleviate symptoms:
 Pain
 Flushing
 Diarhhoea
 Protective from death due to central neck/ mediastinal disease
 External beam radiation: role in unresectable residual or recurrent tumour mass or
symptomatic bony mets
PALLIATION – METASTATIC MTC
 Palliation for Liver mets (usually multiple, >1.5 cm):
 Laparoscopic RF ablation
 Chemoembolization
TARGET THERAPIES:
 Vandetanib (FDA approved) – inhibits VEGFR, multikinase & EGFR
 Anti-CEA monoclonal anti-body – Labetuzumab (CEA-Cide)
 Multikinase inhibitors – sorafenib, sunitinib
MANAGEMENT IN
MEN SYNDROMES
 If PTH raised and hypercalcemia present,
at thyroidectomy, only obviously enlarged
parathyroid gland is removed
 Other PTH glands should be marked and
preserved (20 % in MEN 2A develop HPT)
 If devascularized PTH gland, auto-
transplantation to be done
 Non-dominant forearm
 SCM
PROPHYLACTIC
THYROIDECTOMY
 Family members to be evaluated
with calcitonin level / RET
mutation screening, if positive
prophylactic total thyroidectomy
indicated
 Prophylactic central neck node
dissection:
1. Avoided in calcitonin negative
and normal USG neck
2. To be done - If calcitonin
positive + USG s/o cancer
SCREENING CHARACTERISTICS AGE AT
SURGERY
Less aggressive mutations, normal annual
serum calcitonin, less aggressive family
history, normal neck USG
>5 yrs
Mutations at codon 634 <5 yrs
MEN-2B related mutations <1 yrs
FOLLOW-UP
&
PROGNOSIS
 Annual monitoring:
 Clinical examination
 Calcitonin & CEA levels
 USG Neck/ higher imaging if suspicion
 FGD PET scan: Superior to other radionuclide
based studies for MTC
10 yr survival rate :
 80 % - LN negative cases
 45 % - LN involved
 35 % - MEN2B worst prognosis
MANAGEMENT OF
RECURRENCE - MTC
Local recurrence:
surgical excision
Non localized
– I131 radioablation
– External beam
radiotherapy
ANAPLASTIC CARCINOMA
(UNDIFFERENTIATED TYPE)
CHARACTERISTIC FEATURES
 Very aggressive, one of the most lethal malignancy
 Median survival: 4 to 5 months from diagnosis
 1-3 % of total thyroid malignancies (on a decline)
 Median age 63-74 yrs
 Female to male ratio = 1.5:1
CHARACTERISTIC FEATURES
Commonly related to prior/ concurrent well-differentiated thyroid ca or
benign thyroid disease which suggests:
 Risk factors are similar
 De-differentiation of well-differentiated thyroid cancer tissue, eventually
replaces all well-differentiated tissue
UNDIFFERENTIATED (ANAPLASTIC)
CARCINOMA
Presentation
 Recent rapid enlargement in a long-standing goiter (commonest)
 Recent growth with rapid increase in size
 Regional invasion into trachea, larynx, RLN Palsy
 Distant mets (most commonly lungs, bones & liver)
Mortality
 Aggressive loco-regional invasion e.g. upper airway invasion/ obliteration
ATC - MANAGEMENT
 Aggressive local therapy warranted
 I131 ablation has no role
 Doxorubicin + platinum based chemo: more effective than doxorubicin alone. No other
agent has a role
 Best management strategy:
 Early diagnosis + aggressive surgical resection + EBRT followed by doxorubicin based
chemo
 Recent trials – Paclitaxel may have a role
 Tracheostomy/ isthmusectomy: Relieve airway obstruction in unresectable cases
THYRIOD LYMPHOMA
THYRIOD LYMPHOMA
 Relatively rare disease
 <1 % of thyroid malignancies
 2 % of extra-nodal non-Hodgkin’s lymphoma
 Most common: Non-Hodgkin B cell lymphomas
 Majority are intermediate grade (70-90%)
 Many are considered MALToma
 May be associated with similar lesions in extra-nodal sites e.g. GI tract
THYROID
LYMPHOMA
 Commonly arises from chronic
lymphocytic thyroiditis
 Chronic antigenic lymphocyte
stimulation: lymphocyte
transformation
 Radiosensitive
 Good prognosis
THYRIOD
LYMPHOMA
 Strong female preponderance 3:1 to 8:1
 Age at diagnosis – 7th decade commonest
 Presentation:-
 F/s/o local invasion
 Frequently have features of hypothyroidism
 Correct diagnosis -
 FNAC – may have f/o autoimmune or Hashimoto’s
thyroiditis
 IHC crucial for correct identification (vs Anaplastic Ca)
MANAGEMENT
Optimal therapy possible due to:
 Combination chemo + ability to obtain correct
diagnosis without surgery (Trucut Biopsy)
 Ideal treatment – EBRT + combination
chemotherapy based on the histopathological
subtype
 Most authors support rapid initiation of EBRT +
chemotherapy over surgical excision as it has lower
morbidity
CHOP regime (Cyclophosphamide, Doxorubicin,
Vincristine, and Prednisolone)
METASTASES TO THYROID
 <1 % of all thyroid malignancies
 Common sources:
 Commonest: RCC (23%)
 Breast (16%)
 Lungs (15 %)
 Melanoma (5 %)
 Colon (5%)
 Larynx (5%)
METASTASES TO THYROID
Occasional presentation
– thyroid mass from
occult primary
FNAC helps in
identification
Thyroid mets may grow
rapidly to cause airway
obstruction
Some patients may
require thyroidectomy to
control local symptoms
THANK YOU

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THYROID MALIGNANCIES

  • 1. THYROID MALIGNANCIES + LT COL VIPIN V NAIR + ASSO PROF AND PLASTIC SURGEON + AFMC PUNE THYROID MALIGNANCIES Dr VIPIN V NAIR ASSO PROF SURGERY AND PLASTIC SURGEON AFMC PUNE
  • 2. INTRODUCTION  Most common endocrine tumor (95%)  Female to male ratio- 3:1
  • 3.
  • 4.  Differentiated carcinomas peak in 3rd and 4th decade.  Medullary Ca thyroid peaks in 5th and 6th decade.  Anaplastic carcinomas peak in 7th decade.
  • 6. EPIDEMIOLOGY  Indian population - thyroid cancer forms 1.5% of all malignant tumours  Papillary thyroid carcinoma: Iodine sufficient areas  Follicular thyroid carcinoma: Iodine deficient areas
  • 7. DUNHILL CLASSIFICATION DIFFERENTIATED – arise from Follicular cells • Papillary carcinoma (60 - 70%) • Follicular carcinoma (10%) • Papillo-follicular variant • Hurthle cell carcinoma UNDIFFERENTIATED Anaplastic carcinoma (10%) – arise from undifferentiated follicular cells
  • 8. CLASSIFICATION • MEDULLARY CARCINOMA (5%) – arise from parafollicular cells • MALIGNANT LYMPHOMA (5%) – arise from lymphoid cells • SECONDARIES TO THYROID (RARE) – kidney, breast, direct invasion from aero-digestive tract squamous cell carcinoma
  • 9. WHO Classification Adenomas A. Follicular 1. Colloid variant 2. Embryonal 3. Fetal 4. Hurthle cell variant B. Papillary (probably malignant) C. Teratoma Malignant
  • 10. Malignant A)Differentiated 1.Papillarycarcinoma(and variants) 2.Follicularcarcinoma(variants) a.Minimallyinvasive b.Extensivelyinvasive B)Medullary carcinoma C)Undifferentiated 1.Giantcell 2.Carcinosarcoma D)Miscellaneous 1.Lymphoma,sarcoma 4.Mucoepithelialcarcinoma 2.Squamouscellepidermoidcarcinoma 5.Metastatictumor 3.Fibrosarcoma
  • 11. AGE RELATED PREVALENCE Carcinoma Age group a) Papillary Thyroid carcinoma b) Medullary thyroid carcinoma associated with MEN type 2 Children a) Follicular thyroid carcinoma b) Anaplastic carcinoma c) Sporadic Medullary thyroid carcinoma Elderly
  • 12. THYROID CANCERS IN YOUNG AGE  Papillary carcinoma: most common  Radiation related  More chances of multifocality  More aggressive ??  Extra-thyroid extension: more likely  60%-80%: lymph node metastasis  Lung metastasis(10%)  Recurrence risk: 10% to 35%  Mortality rate: 3 to 5 %
  • 13. ETIOLOGY Thyroid lymphomas: Intra-thyroid lymphoid tissue Sarcomas: Connective tissue of thyroid gland Endodermally derived Follicular cells • Papillary • Follicular • Anaplastic Neuroendocrine derived calcitonin producing C cells • Medullary Thyroid cancers arise from 2 types of cells
  • 14. 1) Radiation Exposure  Papillary Carcinoma Differentiated carcinoma – Irradiation under 5 years of age  Prior neck irradiation early in life  Treatment for acne, tonsillitis (200-150 cGy)  Treatment for malignancies: Hodgkin’s (4000 cGy)  Nuclear holocausts/ accidents  Chernobyl incident (Ukraine 1986): 100 times increase  Long latency period: 20 to 30 yrs
  • 15. 2) Pre-existing Thyroid Lesions  Pre-existing MNG: Follicular carcinoma  SNT (esp. old age, males and in extremes of age)  Hashimoto’s thyroiditis: Papillary thyroid carcinoma  Any solitary nodule ~ 5% chances of malignancy  Solitary nodules with definite h/o radiation exposure: 30 % chances of malignancy
  • 16. FAMILIAL CANCER SYNDROMES • Medullary carcinoma: Multiple endocrine neoplasia (MEN) 2A or 2B syndrome, as well as familial MTC (FMTC) syndrome  4-10 times increased risk in 1st degree relatives SYNDROMES THYROID CANCERS Cowden’s syndrome FTC and rarely PTC and Hurthle cell tumors FAP PTC Werner’s syndrome PTC, FTC, Anaplastic Cancer Carney complex type 1 PTC, FTC McCune Albright syndrome PTC Clear cell
  • 18. Patients with MTC may complain of a dull aching sensation
  • 19. Presentation s/o malignancy – Recent onset pain Recent rapid enlargement in a long standing nodule Dysphagia Stridor Hemoptysis Hoarseness
  • 20.
  • 21. WORKUP  H/o risk factors (radiation, family history)  Examination findings  Firmness (hard, gritty usually s/o malignancy)  Mobility/ adherence to surrounding structures  Presence of LNpathy  Berry’s sign  IDL for vocal cord assessment  USG Neck followed by FNAC
  • 22. LABORATORY INVESTIGATIONS Serum TSH levels  Low TSH - autonomously functioning nodule (usually benign)  Does not rule out malignancy (1% risk) Serum calcitonin levels (MTC or MEN 2)  Highly suggestive of MTC if raised PCR assays for germline mutations in the RET proto- oncogene  Diagnostic in Familial MTC Serum CEA level  Increased in MTC but nonspecific  Better indicator of prognosis than Calcitonin
  • 23. IMAGING STUDIES ULTRASONOGRAPHY  Highly sensitive for thyroid nodules  Can detect sub- clinical/small nodules  Differentiate solid from cystic  Detect sub-clinical cervical lymphadenopathy
  • 25. BETHESDA CRITERIA  Accuracy of FNAC: 70 – 97 %  False Negatives: 1 – 6 %  Chances of malignancy in: i. FLUS – 10 – 35 % ii. AUS – 60 – 75 %  Suspicious for malignancy : 60 % turn out to be malignant  Malignant : 97 % are malignant Despite negative aspirate thyroidectomy indicated if large, hard nodule fixed to surrounding structures FROZEN SECTION Lobectomy ???
  • 26. RADIO IODINE STUDIES  Recommended in patients having Follicular neoplasm on FN and suppressed TSH  Determine functional status of a nodule Based on radioisotope studies nodule can be  Hot - Autonomous toxic nodule  Warm - Normally functioning  Cold - Non functioning nodule (likely malignant but not always)
  • 27.
  • 28.
  • 29.
  • 30. Thyroid scintigraphy Indium-111 octreotide scan for MTC X-rays : CXR and X-ray skull to rule out metastatic deposits COLD NODULE THYROID SCANS
  • 31.
  • 33.
  • 34.
  • 35.
  • 37. CHARACTERISTIC FEATURES  60%-80% of all thyroid malignancies  Found in iodine-sufficient areas  Predominant in children and radiation exposed cases  Females : Males = 2:1 (most euthyroid)  Mean age at presentation 30-40 yrs  Lymphatic spread commoner (mode of presentation in many)  Distant mets: upto 20 % cases (lungs > bone > liver > brain)  Lateral aberrant thyroid: metastatic spread to cervical LN  Multifocality common (upto 85%)
  • 38. DIAGNOSIS AND PRE-OP WORK UP  ORPHAN ANNIE NUCLEI: intra-nuclear cytoplasmic inclusions  Papillary projections: characteristic  Mixed pattern/ follicular pattern (follicular variant)  Follicular variant: behave biologically like papillary  Psammoma bodies  BRAF mutations
  • 39. DIAGNOSIS AND PRE-OP WORK UP  Basis of diagnosis: FNAC of thyroid mass/ LN mass  Complete USG Neck:  Contralateral lobe  LN stations  If suspected clinically: metastatic workup  Prognostic scores
  • 40. PROGNOSTIC MARKERS LN involvement does not alter the prognosis/survival rates Predicts local recurrence All scoring systems categorize the patient as High risk Low risk
  • 41. SURGICAL MANAGEMENT  CURRENT GUIDELINES: Near- total or total thyroidectomy for primary cancers >1 cm (Unless surgery is contraindicated)  Reduced recurrence rates  Improved survival rates  MRND type III: in case of proven lateral lymph node involvement  No role of prophylactic lateral neck node dissection, micro-mets can be addressed by RAI therapy
  • 42. ARGUMENTS IN FAVOR OF TOTAL THYROIDECTOMY
  • 43. SURGICAL MANAGEMENT  Hemithyroidectomy is considered sufficient in cases of:  Small tumours (<1 cm)  Incidentally discovered/ low-risk/ unifocal/ intrathyroidal papillary ca  Absence of prior head and neck irradiation  Absence of radiologically/clinically involved cervical LN mets  FNAC suspicious for papillary Ca: Hemithyroidectomy + removal of adjacent nodes  If frozen-section of lymph node or tumor confirms carcinoma:  Completion total or near-total thyroidectomy is performed  Completion thyroidectomy can be performed at a later setting based on HPE
  • 44. SURGICAL MANAGEMENT Large/ Locally aggressive/ Metastatic tumours  Total thyroidectomy + excision of adjacent involved structures + appropriate nodal surgery  Followed by radio-ablation  Along with long term TSH suppression
  • 46. MICROPAPILLARY OR OCCULT MICRO CA  “Micropapillary carcinoma is a tumour, clinically not detectable or less than 1cm with no evidence of local invasion through the thyroid capsule or angioinvasion”  Size criterion < 1.0 cm  Usually clinically silent, more indolent than macro type  Most are found incidentally at HPE/ autopsy  25 % associated with occult LN mets
  • 47. VARIANTS 1. Follicular variant 2. Encapsulated 3. Diffuse Sclerosing 4. Diffuse Follicular 5. Tall cell 6. Columnar cell 7. Oxyphilic (Oncocytic, Hürthle Cell) 8. Warthin Tumor-like 9. Cribriform-Morular Variant 10. Trabecular 11. Adenoid Cystic Carcinoma–like 12. Macrofollicular 13. Clear cell 14. Hobnail 15. Micropapillary 16. Variant with Spindle Cell Metaplasia. 17. Variant with Exuberant Nodular Fasciitis–like Stroma 18. Papillary Carcinoma with Lipomatous Stroma 19. Dedifferentiated Papillary
  • 48. FOLLICULAR VARIANT  Lindsay tumor  Psammoma bodies and sclerosis may be present  Diagnosis rests on identification of the typical nuclear features of papillary carcinoma  Further divided into two subtypes:  Infiltrative (non-encapsulated)  Encapsulated
  • 50. Follicular Carcinoma vs Follicular Adenoma  Unequivocal vascular and/or capsular invasion: follicular carcinoma  Examination of the tumor-thyroid interface  Histologic examination features favoring follicular Ca:  Thick fibrous capsule  High cellularity, with solid or trabecular growth pattern  Diffuse nuclear atypia  Readily identified mitotic figures
  • 51. CHARACTERISTIC FEATURES  10% of all thyroid ca  More common in iodine deficient areas  Female : Male = 3:1  Presentation at older age: 5th decade  Cervical LN uncommon at presentation  Haematogenous spread more common
  • 52. CHARACTERISTIC FEATURES  Usual presentation:  SNTs: recent rapid increase in size  Long standing MNG  Rarely present as thyrotoxicosis (hyper-functioning nodule)  Indicators of malignancy in cases with FNAC showing follicular features  Distant mets  Large tumours >4 cm in old males  Bony mets: typically vascular/warm/pulsatile. Commonly in skull, long bones, ribs
  • 53. DISTANT METS IN FOLLICULAR CA
  • 54. PATHOLOGICAL FEATURES  Usually solitary lesions  Majority are encapsulated  Minimally invasive tumours: microscopic capsular invasion, no parenchymal invasion  Widely invasive tumours – widespread capsular invasion, e/o large vessel invasion  Tumor thrombi a characteristic feature  Due to limitations of FNAC: Novel genetic markers BRAF, RAS, RET/PTC, MicroRNA 197, 346
  • 55. SURGICAL MANAGEMENT  Follicular lesion on FNAC:Hemithyroidectomy (80% adenomas)  If HPE shows follicular Ca: Completion thyroidectomy  Total thyroidectomy indications:  Older patients  Lesion >4cm ( cancer risk is 50%)  Atypia on FNAC  Family history of thyroid cancer  History of radiation exposure  Total thyroidectomy advocated mainly because RAI can be used to eliminate residual/ metastatic disease
  • 56. NECK DISSECTION  Occasional spread to cervical lymph nodes (10%)  Prophylactic nodal dissection not indicated  Proven nodal metastases: therapeutic neck dissection recommended  Prophylactic central neck dissection may be considered in patients with large tumors >4 cm
  • 57. PROGNOSIS: FOLLICULAR CA  The approximate cumulative mortality  15% at 10 years  30% at 20 years  Poor long-term prognosis predicted by: 1. Age >50 years at presentation 2. Tumor size >4 cm 3. Higher tumor grade 4. Marked vascular invasion 5. Extra-thyroidal invasion 6. Distant metastases at time of diagnosis
  • 58. HÜRTHLE CELL VARIANT  Oncocytic, Oxyphilic, Ashkenazy cell neoplasms (3%)  Subtype of follicular Ca, cannot be diagnosed on FNAC  Differs from classical Follicular Ca:  More often multifocal and bilateral (about 30%)  Usually does not take up RAI (about 5%)  More likely to metastasize to local nodes (25%) and have distant mets at presentation  Higher mortality rate (about 20% at 10 years)
  • 59. HÜRTHLE CELL VARIANT  Routine central neck node dissection recommended  MRND if lateral neck nodes are positive (palpable/ USG)  Radio-iodine scanning & ablation usually ineffective  Should still be considered to ablate residual thyroid tissue and occasionally ablate tumors as there is no other good therapy
  • 60. POST OPERATIVE MANAGEMENT OF DTC RADIOIODINE THERAPY RAI ablation indications:  All patients with stage III and IV disease  All Patients with stage II disease <45 years  Stage I disease with aggressive histology or size >1.5 cm  Nodal mets  Multifocal disease  Extra-thyroidal or vascular invasion
  • 61. RADIOIODINE THERAPY  More sensitive than X-ray/ CT in detecting metastatic/ residual ca  6 weeks after thyroidectomy, hypothyroid can be induced by discontinuing replacement to obtain high serum TSH levels (30mU/L)  Diagnostic dose of I131 or I123 is given initially (1-3 mCi)  Whole-body scanning is performed to detect uptake of radioiodine  If any normal thyroid remnant or metastatic disease detected, therapeutic dose of I131 is administered to ablate the tissue  Low-dose ablation (OPD Basis) - <30mCi (low risk cases)  High doses (100 – 200 mCi) for high risk, old age, incomplete resection
  • 63. TSH SUPPRESSION THERAPY  High risk patients maintained at serum TSH level <0.1 mU/L  Low risk cases 0.1 – 0.5 mU/L (equivocal opinion based on recent trials)  Suppressive dose is 0.3 mg OD lifelong (titration required)  Reduces tumoral growth and recurrence rates
  • 65. MEDULLARY CARCINOMA  Para-follicular C-cell derivative  UB bodies, neuro-ectodermal origin (4th pharyngeal pouch)  5% of all thyroid ca  Concentrated supero-laterally on thyroid lobes  Most MTCs: sporadic  25 % - syndromic (MEN2A, MEN2B, familial MTC)  Hereditary forms - germline mutation of the RET proto-oncogene  C cell hyperplasia (pre-malignant): familial cases
  • 66. FEATURES OF MEDULLARY THYROID CANCER SYNDROMES Syndrome Manifestations MEN2A MTC, pheochromocytoma, primary hyperparathyroidism, lichen planus amyloidosis MEN2B (MOST AGGRESSIVE) MTC, pheochromocytoma, Marfanoid habitus, mucocutaneous ganglioneuromatosis Familial MTC MTC MEN2A and Hirschsprung’s disease MTC, pheochromocytoma, primary hyperparathyroidism, Hirschsprung's disease
  • 67. MEDULLARY CARCINOMA Presentation- 1. Thyroid mass with palpable cervical LN (~20%) 2. Aching type pain 3. Locally invasive symptoms - dysphagia, hoarseness, dyspnoea 4. Diarrhea (40%)  Hematogenous metastases (liver, bone), late feature  Female : Male = 1.5 : 1  Secrete Calcitonin, CEA, serotonin, PG, other peptides  Sporadic cases – 80 % unilateral  Familial cases – 90 % multicentric / Bilateral
  • 68. MTC – DIAGNOSIS Histological feature – marked heterogeneity, amyloid (diagnostic) IHC – Calcitonin/ CEA / Calcitonin-gene related peptide All fresh cases – screened for PHT, phaeochromocytoma, RET point mutations Provocative tests – pentagastrin-stimulated calcitonin level Calcitonin & CEA – markers for persistence/recurrence Calcitonin – more sensitive marker CEA – better predictor of prognosis NECK USG – central/ lateral neck compartments, superior mediastinum
  • 69. MTC – METASTATIC WORK-UP Metastatic work-up indicated in cases with: Palpable/ USG proven positive node Calcitonin level >400ng/mL CECT Neck + Chest Triple-phase CT for liver metastases
  • 70. MTC – MANAGEMENT  Total thyroidectomy + bilateral central neck node dissection treatment of choice because:  Radio-Iodine ablation usually ineffective  High incidence of multicentricity  Palpable cervical lymph nodes: MRND  Tumour >1.5 cm: Ipsilateral prophylactic MRND  If node positive then contralateral node dissection  If phaeochromocytoma present: operated first
  • 71. MTC – MANAGEMENT  In unresectable/ metastatic/ locally recurrent disease tumour debulking surgery indicated to alleviate symptoms:  Pain  Flushing  Diarhhoea  Protective from death due to central neck/ mediastinal disease  External beam radiation: role in unresectable residual or recurrent tumour mass or symptomatic bony mets
  • 72. PALLIATION – METASTATIC MTC  Palliation for Liver mets (usually multiple, >1.5 cm):  Laparoscopic RF ablation  Chemoembolization TARGET THERAPIES:  Vandetanib (FDA approved) – inhibits VEGFR, multikinase & EGFR  Anti-CEA monoclonal anti-body – Labetuzumab (CEA-Cide)  Multikinase inhibitors – sorafenib, sunitinib
  • 73. MANAGEMENT IN MEN SYNDROMES  If PTH raised and hypercalcemia present, at thyroidectomy, only obviously enlarged parathyroid gland is removed  Other PTH glands should be marked and preserved (20 % in MEN 2A develop HPT)  If devascularized PTH gland, auto- transplantation to be done  Non-dominant forearm  SCM
  • 74. PROPHYLACTIC THYROIDECTOMY  Family members to be evaluated with calcitonin level / RET mutation screening, if positive prophylactic total thyroidectomy indicated  Prophylactic central neck node dissection: 1. Avoided in calcitonin negative and normal USG neck 2. To be done - If calcitonin positive + USG s/o cancer SCREENING CHARACTERISTICS AGE AT SURGERY Less aggressive mutations, normal annual serum calcitonin, less aggressive family history, normal neck USG >5 yrs Mutations at codon 634 <5 yrs MEN-2B related mutations <1 yrs
  • 75. FOLLOW-UP & PROGNOSIS  Annual monitoring:  Clinical examination  Calcitonin & CEA levels  USG Neck/ higher imaging if suspicion  FGD PET scan: Superior to other radionuclide based studies for MTC 10 yr survival rate :  80 % - LN negative cases  45 % - LN involved  35 % - MEN2B worst prognosis
  • 76. MANAGEMENT OF RECURRENCE - MTC Local recurrence: surgical excision Non localized – I131 radioablation – External beam radiotherapy
  • 78. CHARACTERISTIC FEATURES  Very aggressive, one of the most lethal malignancy  Median survival: 4 to 5 months from diagnosis  1-3 % of total thyroid malignancies (on a decline)  Median age 63-74 yrs  Female to male ratio = 1.5:1
  • 79. CHARACTERISTIC FEATURES Commonly related to prior/ concurrent well-differentiated thyroid ca or benign thyroid disease which suggests:  Risk factors are similar  De-differentiation of well-differentiated thyroid cancer tissue, eventually replaces all well-differentiated tissue
  • 80. UNDIFFERENTIATED (ANAPLASTIC) CARCINOMA Presentation  Recent rapid enlargement in a long-standing goiter (commonest)  Recent growth with rapid increase in size  Regional invasion into trachea, larynx, RLN Palsy  Distant mets (most commonly lungs, bones & liver) Mortality  Aggressive loco-regional invasion e.g. upper airway invasion/ obliteration
  • 81. ATC - MANAGEMENT  Aggressive local therapy warranted  I131 ablation has no role  Doxorubicin + platinum based chemo: more effective than doxorubicin alone. No other agent has a role  Best management strategy:  Early diagnosis + aggressive surgical resection + EBRT followed by doxorubicin based chemo  Recent trials – Paclitaxel may have a role  Tracheostomy/ isthmusectomy: Relieve airway obstruction in unresectable cases
  • 83. THYRIOD LYMPHOMA  Relatively rare disease  <1 % of thyroid malignancies  2 % of extra-nodal non-Hodgkin’s lymphoma  Most common: Non-Hodgkin B cell lymphomas  Majority are intermediate grade (70-90%)  Many are considered MALToma  May be associated with similar lesions in extra-nodal sites e.g. GI tract
  • 84. THYROID LYMPHOMA  Commonly arises from chronic lymphocytic thyroiditis  Chronic antigenic lymphocyte stimulation: lymphocyte transformation  Radiosensitive  Good prognosis
  • 85. THYRIOD LYMPHOMA  Strong female preponderance 3:1 to 8:1  Age at diagnosis – 7th decade commonest  Presentation:-  F/s/o local invasion  Frequently have features of hypothyroidism  Correct diagnosis -  FNAC – may have f/o autoimmune or Hashimoto’s thyroiditis  IHC crucial for correct identification (vs Anaplastic Ca)
  • 86. MANAGEMENT Optimal therapy possible due to:  Combination chemo + ability to obtain correct diagnosis without surgery (Trucut Biopsy)  Ideal treatment – EBRT + combination chemotherapy based on the histopathological subtype  Most authors support rapid initiation of EBRT + chemotherapy over surgical excision as it has lower morbidity CHOP regime (Cyclophosphamide, Doxorubicin, Vincristine, and Prednisolone)
  • 87. METASTASES TO THYROID  <1 % of all thyroid malignancies  Common sources:  Commonest: RCC (23%)  Breast (16%)  Lungs (15 %)  Melanoma (5 %)  Colon (5%)  Larynx (5%)
  • 88. METASTASES TO THYROID Occasional presentation – thyroid mass from occult primary FNAC helps in identification Thyroid mets may grow rapidly to cause airway obstruction Some patients may require thyroidectomy to control local symptoms

Notas del editor

  1. Not with higher doses >2000 cGy Linear increase in risk from 6.5 – 2000 cGy
  2. Read : Thyroid paradox
  3. 24 hour Urinary VMA, metanephrine and catecholamine – to rule out coexisting Phaeochromocytoma in MTC
  4. Limitation • Difficult to differentiate between follicular adenoma and carcinoma on cytology as it depends upon capsular and angioinavision
  5. MTC (70 %sensitive)
  6. BRAF mutations – more aggressive tumour, extrathyroid extension more common Independent predictor of recurrence and tumour related mortality Warrants more extensive surgical excisions, higher doses of RAI, increased TSH suppression
  7. prognosis is so good in these patients, no added survival