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Stomach Neoplasms

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Stomach Neoplasms Professor Ravi Kant FRCS (England), FRCS (Ireland), FRCS(Edinburgh), FRCS(Glasgow), MS, DNB, FAMS, FACS, FICS, Professor of Surgery – PowerPoint PPT presentation

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Title: Stomach Neoplasms

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Stomach Neoplasms

Professor Ravi Kant
FRCS (England), FRCS (Ireland), FRCS(Edinburgh),
FRCS(Glasgow), MS, DNB, FAMS, FACS, FICS,
Professor of Surgery

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Stomach Neoplasm

Maltoma
Lymphoma
GIST
CA stomach

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GASTRIC LYMPHOMA
4

Gastric Lymphoma
Most common primary GI Lymphoma .
Its increasing in frequency.
Presentation
Similar to gastric carcinoma.
May reveal peripheral adenopathy, abdominal
mass or splenomegaly.

Diagnosis
1.EGD 2.contrast GI x-ray.
3.CT guided fine needle biopsy.
Treatment
Gastric Lymphoma Rx is Surgery
(Other organs- preferred Rx of Lymphoma is
Chemotherapy or Radiotherapy)

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Maltoma

Mucosa associated lymphoid tumour

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MALTOMA

Aetiology H Pylori
Rx Rx of H Pylori
Triple drugs

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GIST
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What are GIST??

Gastrointestinal Stromal Tumors are uncommon
mesenchymal tumors that arise in the wall of the
gastrointestinal tract
It is believed to originate from an intestinal
pacemaker cell called the interstitial cell of
Cajal.

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Cajal cell

An intestinal pacemaker cell, has been proposed
the cellular origin of GISTs. It has
characteristics of both smooth muscle and neural
differentiation on ultrastructural examination

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KIT

role of the KIT and platelet-derived growth
factor receptor (PDGFR) tyrosine kinase receptors
KIT receptor tyrosine kinase (KIT RTK)

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KIT

approximately 5 of GIST cells show not
activation and aberrant signaling of the KIT
receptor, but rather mutational activation of a
structurally related kinase, PDGFR- (PDGFRA).
90 rate of mutations seen in a more recent
series searching for potential mutations in each
of exons 11, 9, 13, and 17

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CD117 CD34 Actin Desmin S-100
GIST - -
Desmoid tumor - - -
True leiomyosarcoma - - -
Schwanoma - - -

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Diagnosis

CT is the common mode of diagnosis
FDG PET is mandatory
?PET CT scan is ideal
MR

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GIST chemoresistance

? P-glycoprotein the product of the multidrug
resistance-1 (MDR-1) gene
? MDR protein

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Distribution

Stomach 50-60
Small bowel 20-30
Large bowel 10
Esophagus 5
Else where in abdomen 5

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Symptoms

Abdominal pain
Dysphagia
Gastrointestinal bleeding
Symptoms of bowel obstruction
Small tumors may be asymptomatic

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Cytologically

Spindle cell GISTs
Epithelioid cell GISTs
Although GISTs can differentiate along either or
both cell types, some show NO significant
differentiation at all

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Diagnosis

MUST BE DONE IMMUNOCHEMICALLY
The CD34 antigen (70-78)
The CD117 antigen (72-94)

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Malignant Versus Benign
Size Mitotic count
Very Low risk lt2 cm lt5/50 HPF
Low risk 2-5 cm lt5/50 HPF
Intermediate risk lt5 cm 5-10 cm 6-10/50 HPF lt5/50 HPF
High risk gt5 cm gt10 cm Any size gt5/50 HPF Any count gt10/50 HPF
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predictors of survival

Male sex,
Tumor size gt 5cm
Incomplete resection

significant on multivariate analysis
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Treatment

Surgical excision is primary treatment option but
recurrence rates are high
Resistant to standard chemotherapy regimens due
to over-expression of efflux pumps
Radiation therapy limited by large tumor sizes
and sensitivity of adjacent bowel

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IMATINIB

Since activation of Kit played a crucial role in
the pathogenesis of GIST, inhibition of Kit would
be therapeutic ?

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IMATINIB

Orally bioactive tyrosine kinase inhibitor
Shown to be effective against GIST tumors in two
trials in the US and Europe reported in 2001
2002

Gastrointestinal Stromal Tumor GIST
Previously leiomyoma leiomyosarcoma.
lt1
Rarely cause bleeding or obstruction.
The origin Intestinal Cells of Cajal ICCs
autonomic nervous system.
The distinction b\w benign malignant is
unclear. In general terms, the larger the tumor
greater mitotic activity, the more likely to
metastases.
The stomach is the most common site of GIST.

Usually are discovered incidentally on endoscopy
or barium meal
The endoscopic biopsies may be uninformative as
the overlying mucosa is usually normal
Small tumors?wedge resection
Larger ones?gastrectomy

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GIST

Case history-submucosal
Cajal Cell
Gene KIT
PGDRF
Diagnosis
CT
PET

Rx
Surgery
Chemoresistance
Imatininb
Sumanitib
Prognosis
Predictor factors

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GASTRIC CARCINOMA
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GASTRIC NEOPLASM
Benign
Malignant

Epithelial
Mesenchymal

1.Primary Adenocarcinoma Gastrointestinal stromal
tumors GIST Lymphoma
2. Secondary invasion from adjacent tumors.
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GASTRIC CA
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Gastric Carcinoma
Epidemiology Risk Factors
DEFINITION
Malignant lesion of the stomach.

55 year old Japanese male who is living in Japan
working in industry.

Incidence of Gastric Carcinoma Japan 70
in100,000/year Europe 40 in 100,000/year UK 15 in
100,000/year USA 10 in 100,000/year It is
decreasing worldwide.
Can occur at any age But Peak incidence Is 50-70
years old. It is more aggressive In younger ages.
Twice more common In male than in female
Studies have confirmed that incidence decline
in Japanese immigrant to America.
Japan has the world highest Rate of gastric
cancer.
dust ingestion from a variety of industrial
processes may be a risk.
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Gastric Carcinoma

Risk Factors

Environmental 1.H.pylori infection
Sero()patients have 6-9 folds risk 2.low
socioeconomic Status 3. nationality
(JAPAN) 4. Diet (prevention)
Predisposing 1. Pernicious anaemia
atrophic gastritis (achlorhydra) 2.
Previous gastric resection 3. Chronic peptic
ulcer (give rise to 1) 4. Smoking. 5.
Alcohol.
Genetic 1.Blood group A 2.HNPCC Hereditary
non-polyposis colon cancer.
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Clinical Presentation

Most patients present with advanced stage..
why?
They are often asymptomatic in early stages.

Common clinical Presentation
The patient complained of loss of appetite that
was followed by weight loss of 10Kg in 4 weeks.
He had notice epigastric discomfort
postprandial fullness. He presented to the ER
complaining of vomiting of large quantities of
undigested food epigastric distension.
epigastric pain Bloating early satiety nausea
vomiting dysphagia anorexia weight loss
upper GI bleeding (hematemesis, melena, iron
deficiency anemia)
Dyspepsia
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signs

-Anemia.
-Wt. loss ( cachexia)
-Epigastric mass, Hepatomegaly, Ascitis
-Jaundice.
-Blumers shelf
-Virchow's node
-Sister Mary Joseph node
-Krukenberg tumor
-Irish node

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Pathology DIO Classification

Lauren Classification
1. Intestinal Gastric ca.
It arises in areas of intestinal metaplasia
to form polypoid tumors or ulcers.
2. Diffuse Gastric ca.
It infiltrates deeply in the stomach without
forming obvious mass lesions but spreads widely
in the gastric wall Linitis Plastica
it has much more worse prognosis
3. Mixed Morphology.

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Morphology

Polypoid
Ulcerative
Superficial spreading
Linitis plastica

Gastric cancer can be divided into
Early
Limited to mucosa submucosa with or without
LN (T1, any N)
gtgt curable with 5 years survival rate in 90.
Advanced
It involves the Muscularis.
It has 4 types( Bormanns classification).
Type III IV are incurable.

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Staging of gastric cancer
Spread of Gastric Cancer
Direct Spread
Lymphatic spread
T1 lamina propria submucosa
T2 muscularis subserosa
T3 serosa
T4 Adjacent organs
N0 no lymph node
N1 Epigastric node
N2 main arterial trunk
M0 No distal metastasis
M1 distal metastasis
Tumor penetrates the muscularis, serosa
Adjacent organs (Pancreas,colon liver)
What is important here is Virchows node
(Trosiers sign)
Blood-borne metastasis
Transperitoneal spread
This is common Anywhere in peritoneal
cavity (Ascitis) Krukenberg tumor
(ovaries) Sister Joseph nodule (umbilicus)
Usually with extensive Disease where liver
1st Involved then lung Bone
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Complications

Peritoneal and pleural effusion
Obstruction of gastric outlet or small bowel
Bleeding
Intrahepatic jaundice by hepatomegaly

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Differential Diagnosis

1.Gastric ulcer
2.Other gastric neoplasms
3.Gastritis
4.Gastric Polyp
5.Crohns disease.

From history, Cancer is not relieved by
antacids Not periodic Not relieved by eating or
vomiting.
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INVESTIGATIONS

Full blood count IDA-
LFT,RFT
Amylase lipase.
Serum tumor markers (CA 72-4,CEA,CA19-9) not
specific
Stool examination for occult blood
CXR ,Bone scan.

Specific
UGI endoscopy with biopsy
Double contrast study
CT, MRI US
Laparoscopry

EGD esophagogastroduodenoscopy
Diagnostic accuracy is 98
if up to 7 biopsies is taken.
Double Contrast barium upper GI x-ray
Diagnostic accuracy 90
WHY?

Diagnostic study of Choice
1.Early superficial gastric mucosal lesion can
be missed. 2. cant differentiate b/w benign
ulcer Ulcerating adenocarcinoma.
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X-ray showing Extensive carcinoma involving
the cardia Fundus
X-ray showing Gastric ulcer With symmetrical
radiating Mucosal folds. By histology, no
evidence of Malignancies was observed.
Pyloric stenosis
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CT,MRI US
Laparoscopy

Help in assessment of wall thickness, metastases
(peritoneum ,liver LN)
Detection of peritoneal metastases
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UGI ENDOSCOPY

THE GOLD STANDARD
It allows taking biopsies
Safe (in experienced hands)

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UGI ENDOSCOPY,contd.

You may see an ulcer (25), polypoid mass (25),
superficial spreading (10),or infiltrative
(Linitis plastica)-difficult to be detected-
Accuracy 50-95 it depends on gross appearance,
size, location no. of biopsies

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IF YOU SEE ULCER ASK UR SELFBENIGN OR MALIGNANT?
MALIGNANT BENIGN
Irregular outline with necrotic or hemorrhagic base Round to oval punched out lesion with straight walls flat smooth base
Irregular raised margins Smooth margins with normal surrounding mucosa
Anywhere Mostly on lesser curvature
Any size Majoritylt2cm
Prominent edematous rugal folds that usually do not extend to the margins Normal adjoining rugal folds that extend to the margins of the base
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Management

Surgery
Chemotherapy
NO PROVEN
BENEFIT
Radiotherapy

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Treatment

Initial treatment
1.Improve nutrition if needed by parenteral or
enteral feeding.
2.Correct fluid electrolyte
anemia if they are present.

Preoperative Care
Preoperative Staging is important because we
dont want to subject the patient to radical
surgery that cant help him.

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PRE-OPERATIVE CARE

Careful preoperative staging
Screen for any nutritional deficiencies
consider nutritional support
Symptomatic control
Blood transfusion in symptomatic anemia
Hydration
Prophylactic antibiotics
ABO cross match
Ask about current medications allergies
Cessation of smoking

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BASIC SURGICAL PRINCIPLES

3 TYPES TOTAL,SUBTOTAL,PALLIATIVE
ANTRAL DISEASE?SUBTOTAL GASTRECTOMY
MIDBODY PROXIMAL? TOTAL GASTRECTOMY

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TOTAL (RADICAL) GASTRECTOMY

Remove the stomach distal part of esophagus
proximal part of duodenum greater lesser
omentum LN
Oesophagojejunostomy with roux-en-y .

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SUBTOTAL GASTRECTOMY

Similar to total one except that the PROXIMAL
PART of the stomach is preserved
Followed by reconstruction creating anastomosis
( by gastrojejunostomy, Billroth II )

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PALLIATIVE SURGERY

For pts with advanced (inoperable) disease
suffering significant symptoms e.g. obstruction,
bleeding.
Palliative gastrectomy not necessarily to be
radical, remove resectable masses reconstruct
(anastomosis/intubation/stenting/
recanalisation)

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POSTOPERATIVE ORDERS