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Cancer of Pancreas

The document provides a comprehensive overview of pancreatic cancer, including the anatomy of the pancreas, epidemiology, types of pancreatic cancers, clinical features, diagnostic evaluations, and treatment options. It highlights that pancreatic cancer is the 13th most common cancer globally with a very low survival rate of 2-5% at five years post-diagnosis. Additionally, it outlines nursing management strategies and the importance of specialized surgical centers for effective treatment.

PANCREATIC CANCER Presented by: Ms. Priyanka Malhotra, M.Sc. Nursing 2nd year
LOCATION OF PANCREAS
Anatomy of Pancreas Derived from ‘Pan’ – all ‘Kreas’ – flesh 15-20cm long, 2.5 – 3.8cm broad, 1.2 – 1.8cm thick Weighs 80g Situated in retro-peritoneum region Head of pancreas (30%)- right side of the abdomen (behind where the stomach meets the duodenum). Body of pancreas (Body & Tail, 70%)- behind the stomach. Tail of the pancreas- left side of the abdomen next to the spleen.
Head, Neck ,Body & Tail of Pancreas
Histology 80-90% of pancreatic tissue – Exocrine Acinar Tissue organised as lobules Pancreatic duct Interlobular & Intralobular ducts Ductules Acini Main duct – Columnar cells, Ductules – Cuboidal cells Clusters of endocrine cells distributed throughout called Islets of Langerhans Islet: Hormone secretion 75% - B Cells- Insulin 20% - A Cells- Glucagon 5% - D Cells- Somatostatin
Posterior Relations Of Pancreas
Blood Supply, Lymphatics & Nerve Supply Arterial: Pancreatic Branches of splenic artery Superior pancreaticoduodenal artery Inferior pancreaticoduodenal artery Venous: Drains into splenic, superior mesenteric and portal veins Lymphatics: Head & Neck – Pancreaticoduodenal Body & Tail – Pancreaticosplenic Nerve Supply: Parasympathetic – Vagus Sympathetic – plexuses around its arteries
BLOOD SUPPLY OF PANCREAS
Physiology In response to food – secretes digestive enzymes in an alkaline (bicarbonate) rich fluid. Secretions enhanced by: Secretin, Cholecystokinin & Vagal Stimulation. Within cells enzymes are in inactive form. Composition of Pancreatic secretions: Electrolytes: Cations: Na+, K+, Ca2+, Mg2+, Zn2+ Anions: HCO3-, Cl- and traces of SO42-, HPO42 Enymes: Pancreatic alpha-amylase, Pancreatic lipase & Pancreatic esterase Proteolytic enymes: Trypsinogen, Chymotrypsin, Pro- carboxypeptidase, Ribonuclease & Deoxy-ribonuclease.
EPIDEMIOLOGY Estimated 278,684 cases of CA pancreas occur annually worldwide. 13th most common cancer globally. Up to 60% of cases are diagnosed in developed countries. Incidence is highest in the U.S., Western Europe and lowest in parts of Africa and South Central Asia. It is associated with poor survival and ranks as the 4th or 5th most common cause of cancer mortality. India-Incidence of CA pancreas is 0.5–2.4 per 100,000 men and 0.2–1.8 per 100,000 women. (Thapa,P. (2015). Epidemiology of Pancreatic and Periampullary Cancer.)
CANCER OF THE PANCREAS Cancer is caused by the abnormal and uncontrolled growth of cells in the pancreas. It may arise in any portion of the pancreas. It can also be the site of metastasis from other tumors. Clinical manifestations vary depending on the location of lesion. CA Pancreas has only a 2-5% survival rate at 5 years regardless of stage of disease at diagnosis. Infiltrating ductal adenocarcinomas, account for the vast majority of cases arising most frequently in the head of pancreas.
VARIOUS TYPES OF PANCREATIC CANCERS 1) Tumors of the Head of the Pancreas (75%) Tumors producing the obstruction may arise from: The pancreas, the common bile duct, or the Ampulla of Vater. 2) Exocrine pancreatic cancers (most common type) • Pancreatic adenocarcinoma (90%): Starts in ducts of pancreas. • Acinar cell carcinomas: From pancreatic enzyme making cells. • Less common types of exocrine cancer: Adenosquamous carcinomas, squamous cell carcinomas, signet ring cell carcinomas, undifferentiated carcinomas, and undifferentiated carcinomas with giant cells.
VARIOUS TYPES OF PANCREATIC CANCERS 3) Pancreatic endocrine tumors or Islet Tumors (neuroendocrine tumors-NETs) Two types of tumors of pancreatic islet cells are known: Insulinoma-Those that secrete insulin and “Nonfunctioning” islet cell cancer-Those in which insulin secretion is not increased. 4) Ampullary cancer (Carcinoma of the Ampulla of Vater) They often block the bile duct, which leads to jaundice. They are usually found earlier than most pancreatic cancers. Therefore, have a better prognosis.
P A T H O P H Y S I O L O G Y
CLINICAL FEATURES Physical Signs • Jaundice, cachexia, and scratch marks. • Courvoisier's sign: palpable gallbladder. Distant metastases Physical signs: • Hepatomegaly & Ascites • Virchow's node -left supraclavicular lymphadenopathy and • Sister Mary Joseph's nodes- periumbilical nodules. Abdominal discomfort, pruritus, lethargy, weight loss, nausea and vomiting . Less common presenting features: New-onset diabetes mellitus and acute pancreatitis.
DIAGNOSTIC EVALUATION Physical Examination & History Collection Diagnostic Imaging Provides resectability and prognostic information. Imaging modality of choice: • Dual-phase, contrast-enhanced spiral CT Accurate visualization of surrounding viscera, vessels and lymph nodes. • MRI (characterizes nature of small indeterminate liver lesions) • Endoscopic retrograde cholangiopancreatography (ERCP) It reveals small pancreatic lesions.
Coronal CT showing pancreatic cancer, dilated intrahepatic and pancreatic ducts (arrows)
DIAGNOSTIC EVALUATION • Magnetic resonance cholangiopancreatography (MRCP) • EUS (highly sensitive in detecting lesions <3 cm size) • Fluorodeoxyglucose positron emission tomography (FDG-PET)  Tissue Diagnosis and Cytology • EUS-guided fine-needle aspiration, Percutaneous biopsy • ERCP- useful method for obtaining ductal brushings  Serum Markers • Tumor markers- CA 19.9, CEA, DU-PAN-2 • Tumor-associated CA19.9 is elevated (in 70-80%) Preoperative CA19.9 1evels correlate with tumor stage and Post-resection CA19.9 level has prognostic value.
ERCP showing contrast in dilated pancreatic duct (arrows).
STAGING OF TUMOUR American Joint Committee on Cancer (AJCC): Tumor-node-metastasis (TNM) staging of pancreatic cancer. It takes into account- • The location and size of tumor, • The involvement of lymph nodes and • Distant metastasis. From a practical standpoint, grouping is done as: • Resectable, • Locally advanced (unresectable, but without distant spread), or • Metastatic (with distant spread).
TREATMENT OF PANCREATIC CANCER Resectable Disease Localized non-metastatic disease (10%) is best for surgical resection. • Rl resection (microscopic residual disease) • RO resection (no microscopic or macroscopic residual tumor) Tumors of pancreatic head or uncinate process- The standard surgical procedure is a pylorus-preserving pancreaticoduodenectomy (modified Whipple's procedure). • The common duct is sutured to end of jejunum, and • The remaining portion of the pancreas and the end of stomach are sutured to the side of jejunum.
Pancreatoduodenectomy (Whipple’s procedure or resection)
VIDEO ON WHIPPLE’S PROCEDURE
TREATMENT OF PANCREATIC CANCER For tumors of the pancreatic body and tail- Distal pancreatectomy (includes splenectomy). When tumor cannot be excised- To relieve jaundice anastomosis of jejunum to gallbladder, known as cholecystojejunostomy. Adjuvant chemotherapy (6 cycles of gemcitabine). Adjuvant radiotherapy (bulky tumors of pancreatic head). • Metastatic Disease (60%) 5-FU/FA, irinotecan and oxaliplatin (FOLFIRINOX) • Inoperable Locally Advanced Disease (30%) Chemotherapy + consolidation radiotherapy
Studies of Adjuvant Chemotherapy in Resected Pancreatic Cancer Study Comparator Arm No. of patients Survival PFS/DFS (Months) Median Survival (Months) ESPAC-1, Neoptolemos et al: N Engl J Med 350:1200,2004 Chemotherapy (folinic acid + bolus 5-FU) vs no chemotherapy 289 PFS 15.3 vs 9.4. (p=0.02) 20.1 vs 155 (HR 0.71,95%CI 055- 0.92; P=0.009) CONKO 001, Oettle et al: JAMA 297:267,2007 Gemcitabine vs observation 368 Median DFS 13.4 vs 6.9 (p<0.001) 22.1 vs 20.2 (p= 0.06) ESPAC-3, Neoptolemos et al: JAMA 304:1073, 2010 5-FU/LV vs gemcitabine 1088 23 vs 23.6 (HR 0.94; 95% CI 0.81- 1.08,p=39) Abbreviations: CI-Confidence Interval; CONKO- Charité Onkologie; DFS- Disease-free survival; ESPAC- European Study Group for Pancreatic Cancer; 5-FU- 5-fluorouracil; HR- Hazard ratio; LV- Leucovorin; PFS- Progression-free survival.
NURSING MANAGEMENT Nursing Diagnosis for Pancreatic Cancer Diagnosis 1: Chronic abdominal pain related to tumor growth secondary to progressive pancreatic cancer. Diagnosis 2: Imbalanced nutrition, less than body requirements, related to anorexia, cachexia, malabsorption or nausea and vomiting secondary to chemotherapy. Diagnosis 3: Impaired skin integrity related to erythematous and wet desquamation reactions to radiation therapy. Diagnosis 4: Impaired tissue integrity related to alopecia secondry to chemotherapy.
Nursing Diagnosis for Pancreatic Cancer Diagnosis 5: Activity intolerance related to fatigue or weakness secondary to chemotherapy or surgical intervention. Diagnosis 6: Potential complications (risk for GI bleeding) related to diseased condition. Diagnosis 7: Risk for infection related to altered immunologic response secondary to chemo-radiation therapy. Diagnosis 8: Disturbed body image and situational low self- esteem related to changes in appearance, function, and roles secondary to surgical interventions (Whipple’s procedure).
Guidelines for perioperative care for pancreaticoduodenectomy
Nursing Interventions Pain management- Use of opioids or patient controlled analgesia (PCA) for severe or escalating pain. Nutritional and fluid requirements- To overcome anorexia and profound weight loss. Skin care- Use of Specialty mattresses and skin hygiene. Teaching Patients Self-Care Chemotherapy- Teaching on prevention of side effects and complications of agents used. Surgery- Management of drainage system and monitoring for complications. Continuing Care- Arrange palliative care (hospice services).
SUMMARY The various topics discussed are as follows: Location of the pancreas Various types of pancreatic cancers Risk factors for the pancreatic cancer Clinical manifestations of pancreatic cancer Diagnostic evaluation for pancreatic cancer Treatment modalities for pancreatic cancer Nursing management for pancreatic cancer
CONCLUSION • Incidence of CA Pancreas has decreased slightly over past 25 years in non-Caucasian men. • Diabetes mellitus, chronic pancreatitis, and hereditary pancreatitis are associated with pancreatic cancer. • Pancreas can also be site of metastasis from other tumors. • In fact, pancreatic carcinoma has only a 2% to 5% survival rate at 5 years regardless of stage of disease at diagnosis or treatment. • Patients should have surgery in dedicated pancreatic centers that have lower postoperative morbidity and mortality rates.

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Cancer of Pancreas

  • 1.
    PANCREATIC CANCER Presented by:Ms. Priyanka Malhotra, M.Sc. Nursing 2nd year
  • 2.
  • 3.
    Anatomy of Pancreas Derivedfrom ‘Pan’ – all ‘Kreas’ – flesh 15-20cm long, 2.5 – 3.8cm broad, 1.2 – 1.8cm thick Weighs 80g Situated in retro-peritoneum region Head of pancreas (30%)- right side of the abdomen (behind where the stomach meets the duodenum). Body of pancreas (Body & Tail, 70%)- behind the stomach. Tail of the pancreas- left side of the abdomen next to the spleen.
  • 4.
    Head, Neck ,Body& Tail of Pancreas
  • 5.
    Histology 80-90% of pancreatictissue – Exocrine Acinar Tissue organised as lobules Pancreatic duct Interlobular & Intralobular ducts Ductules Acini Main duct – Columnar cells, Ductules – Cuboidal cells Clusters of endocrine cells distributed throughout called Islets of Langerhans Islet: Hormone secretion 75% - B Cells- Insulin 20% - A Cells- Glucagon 5% - D Cells- Somatostatin
  • 6.
  • 7.
    Blood Supply, Lymphatics& Nerve Supply Arterial: Pancreatic Branches of splenic artery Superior pancreaticoduodenal artery Inferior pancreaticoduodenal artery Venous: Drains into splenic, superior mesenteric and portal veins Lymphatics: Head & Neck – Pancreaticoduodenal Body & Tail – Pancreaticosplenic Nerve Supply: Parasympathetic – Vagus Sympathetic – plexuses around its arteries
  • 8.
  • 9.
    Physiology In response tofood – secretes digestive enzymes in an alkaline (bicarbonate) rich fluid. Secretions enhanced by: Secretin, Cholecystokinin & Vagal Stimulation. Within cells enzymes are in inactive form. Composition of Pancreatic secretions: Electrolytes: Cations: Na+, K+, Ca2+, Mg2+, Zn2+ Anions: HCO3-, Cl- and traces of SO42-, HPO42 Enymes: Pancreatic alpha-amylase, Pancreatic lipase & Pancreatic esterase Proteolytic enymes: Trypsinogen, Chymotrypsin, Pro- carboxypeptidase, Ribonuclease & Deoxy-ribonuclease.
  • 11.
    EPIDEMIOLOGY Estimated 278,684 casesof CA pancreas occur annually worldwide. 13th most common cancer globally. Up to 60% of cases are diagnosed in developed countries. Incidence is highest in the U.S., Western Europe and lowest in parts of Africa and South Central Asia. It is associated with poor survival and ranks as the 4th or 5th most common cause of cancer mortality. India-Incidence of CA pancreas is 0.5–2.4 per 100,000 men and 0.2–1.8 per 100,000 women. (Thapa,P. (2015). Epidemiology of Pancreatic and Periampullary Cancer.)
  • 12.
    CANCER OF THEPANCREAS Cancer is caused by the abnormal and uncontrolled growth of cells in the pancreas. It may arise in any portion of the pancreas. It can also be the site of metastasis from other tumors. Clinical manifestations vary depending on the location of lesion. CA Pancreas has only a 2-5% survival rate at 5 years regardless of stage of disease at diagnosis. Infiltrating ductal adenocarcinomas, account for the vast majority of cases arising most frequently in the head of pancreas.
  • 13.
    VARIOUS TYPES OFPANCREATIC CANCERS 1) Tumors of the Head of the Pancreas (75%) Tumors producing the obstruction may arise from: The pancreas, the common bile duct, or the Ampulla of Vater. 2) Exocrine pancreatic cancers (most common type) • Pancreatic adenocarcinoma (90%): Starts in ducts of pancreas. • Acinar cell carcinomas: From pancreatic enzyme making cells. • Less common types of exocrine cancer: Adenosquamous carcinomas, squamous cell carcinomas, signet ring cell carcinomas, undifferentiated carcinomas, and undifferentiated carcinomas with giant cells.
  • 16.
    VARIOUS TYPES OFPANCREATIC CANCERS 3) Pancreatic endocrine tumors or Islet Tumors (neuroendocrine tumors-NETs) Two types of tumors of pancreatic islet cells are known: Insulinoma-Those that secrete insulin and “Nonfunctioning” islet cell cancer-Those in which insulin secretion is not increased. 4) Ampullary cancer (Carcinoma of the Ampulla of Vater) They often block the bile duct, which leads to jaundice. They are usually found earlier than most pancreatic cancers. Therefore, have a better prognosis.
  • 18.
  • 20.
    CLINICAL FEATURES Physical Signs •Jaundice, cachexia, and scratch marks. • Courvoisier's sign: palpable gallbladder. Distant metastases Physical signs: • Hepatomegaly & Ascites • Virchow's node -left supraclavicular lymphadenopathy and • Sister Mary Joseph's nodes- periumbilical nodules. Abdominal discomfort, pruritus, lethargy, weight loss, nausea and vomiting . Less common presenting features: New-onset diabetes mellitus and acute pancreatitis.
  • 22.
    DIAGNOSTIC EVALUATION Physical Examination& History Collection Diagnostic Imaging Provides resectability and prognostic information. Imaging modality of choice: • Dual-phase, contrast-enhanced spiral CT Accurate visualization of surrounding viscera, vessels and lymph nodes. • MRI (characterizes nature of small indeterminate liver lesions) • Endoscopic retrograde cholangiopancreatography (ERCP) It reveals small pancreatic lesions.
  • 23.
    Coronal CT showingpancreatic cancer, dilated intrahepatic and pancreatic ducts (arrows)
  • 24.
    DIAGNOSTIC EVALUATION • Magneticresonance cholangiopancreatography (MRCP) • EUS (highly sensitive in detecting lesions <3 cm size) • Fluorodeoxyglucose positron emission tomography (FDG-PET)  Tissue Diagnosis and Cytology • EUS-guided fine-needle aspiration, Percutaneous biopsy • ERCP- useful method for obtaining ductal brushings  Serum Markers • Tumor markers- CA 19.9, CEA, DU-PAN-2 • Tumor-associated CA19.9 is elevated (in 70-80%) Preoperative CA19.9 1evels correlate with tumor stage and Post-resection CA19.9 level has prognostic value.
  • 26.
    ERCP showing contrastin dilated pancreatic duct (arrows).
  • 29.
    STAGING OF TUMOUR AmericanJoint Committee on Cancer (AJCC): Tumor-node-metastasis (TNM) staging of pancreatic cancer. It takes into account- • The location and size of tumor, • The involvement of lymph nodes and • Distant metastasis. From a practical standpoint, grouping is done as: • Resectable, • Locally advanced (unresectable, but without distant spread), or • Metastatic (with distant spread).
  • 35.
    TREATMENT OF PANCREATICCANCER Resectable Disease Localized non-metastatic disease (10%) is best for surgical resection. • Rl resection (microscopic residual disease) • RO resection (no microscopic or macroscopic residual tumor) Tumors of pancreatic head or uncinate process- The standard surgical procedure is a pylorus-preserving pancreaticoduodenectomy (modified Whipple's procedure). • The common duct is sutured to end of jejunum, and • The remaining portion of the pancreas and the end of stomach are sutured to the side of jejunum.
  • 37.
  • 38.
  • 39.
    TREATMENT OF PANCREATICCANCER For tumors of the pancreatic body and tail- Distal pancreatectomy (includes splenectomy). When tumor cannot be excised- To relieve jaundice anastomosis of jejunum to gallbladder, known as cholecystojejunostomy. Adjuvant chemotherapy (6 cycles of gemcitabine). Adjuvant radiotherapy (bulky tumors of pancreatic head). • Metastatic Disease (60%) 5-FU/FA, irinotecan and oxaliplatin (FOLFIRINOX) • Inoperable Locally Advanced Disease (30%) Chemotherapy + consolidation radiotherapy
  • 43.
    Studies of AdjuvantChemotherapy in Resected Pancreatic Cancer Study Comparator Arm No. of patients Survival PFS/DFS (Months) Median Survival (Months) ESPAC-1, Neoptolemos et al: N Engl J Med 350:1200,2004 Chemotherapy (folinic acid + bolus 5-FU) vs no chemotherapy 289 PFS 15.3 vs 9.4. (p=0.02) 20.1 vs 155 (HR 0.71,95%CI 055- 0.92; P=0.009) CONKO 001, Oettle et al: JAMA 297:267,2007 Gemcitabine vs observation 368 Median DFS 13.4 vs 6.9 (p<0.001) 22.1 vs 20.2 (p= 0.06) ESPAC-3, Neoptolemos et al: JAMA 304:1073, 2010 5-FU/LV vs gemcitabine 1088 23 vs 23.6 (HR 0.94; 95% CI 0.81- 1.08,p=39) Abbreviations: CI-Confidence Interval; CONKO- Charité Onkologie; DFS- Disease-free survival; ESPAC- European Study Group for Pancreatic Cancer; 5-FU- 5-fluorouracil; HR- Hazard ratio; LV- Leucovorin; PFS- Progression-free survival.
  • 44.
    NURSING MANAGEMENT Nursing Diagnosisfor Pancreatic Cancer Diagnosis 1: Chronic abdominal pain related to tumor growth secondary to progressive pancreatic cancer. Diagnosis 2: Imbalanced nutrition, less than body requirements, related to anorexia, cachexia, malabsorption or nausea and vomiting secondary to chemotherapy. Diagnosis 3: Impaired skin integrity related to erythematous and wet desquamation reactions to radiation therapy. Diagnosis 4: Impaired tissue integrity related to alopecia secondry to chemotherapy.
  • 45.
    Nursing Diagnosis forPancreatic Cancer Diagnosis 5: Activity intolerance related to fatigue or weakness secondary to chemotherapy or surgical intervention. Diagnosis 6: Potential complications (risk for GI bleeding) related to diseased condition. Diagnosis 7: Risk for infection related to altered immunologic response secondary to chemo-radiation therapy. Diagnosis 8: Disturbed body image and situational low self- esteem related to changes in appearance, function, and roles secondary to surgical interventions (Whipple’s procedure).
  • 46.
    Guidelines for perioperativecare for pancreaticoduodenectomy
  • 49.
    Nursing Interventions Pain management-Use of opioids or patient controlled analgesia (PCA) for severe or escalating pain. Nutritional and fluid requirements- To overcome anorexia and profound weight loss. Skin care- Use of Specialty mattresses and skin hygiene. Teaching Patients Self-Care Chemotherapy- Teaching on prevention of side effects and complications of agents used. Surgery- Management of drainage system and monitoring for complications. Continuing Care- Arrange palliative care (hospice services).
  • 51.
    SUMMARY The various topicsdiscussed are as follows: Location of the pancreas Various types of pancreatic cancers Risk factors for the pancreatic cancer Clinical manifestations of pancreatic cancer Diagnostic evaluation for pancreatic cancer Treatment modalities for pancreatic cancer Nursing management for pancreatic cancer
  • 52.
    CONCLUSION • Incidence ofCA Pancreas has decreased slightly over past 25 years in non-Caucasian men. • Diabetes mellitus, chronic pancreatitis, and hereditary pancreatitis are associated with pancreatic cancer. • Pancreas can also be site of metastasis from other tumors. • In fact, pancreatic carcinoma has only a 2% to 5% survival rate at 5 years regardless of stage of disease at diagnosis or treatment. • Patients should have surgery in dedicated pancreatic centers that have lower postoperative morbidity and mortality rates.