Appendix Flashcards
Discuss the embryology and anatomy of the appendix
- midgut organ, first identified at 8wks gestation as a small outpouching of the caecum
- as gestation proceeds, appendix becomes more elongated & tubular as the caecum rotates medially & becomes fixed in the RLQ
- agenesis of appendix + duplication & even triplication reported
- variable size (5-35cm) but averages 9cm length in adults
- base lies at convergence of taenia
- unequal growth of saculated caecum during childhood (R side enlarges more rapidly) –> appendix lies medially & posteriorly
- variable position of tip:
- retrocaecal (but intraperitoneal) 60%
- pelvic 30%
- retroperitoneal 7-10%
- appendiceal artery (end artery) = usu off inf division of ileocolic –> mesoappendix
- mesoappendix also contains lymphatics of appendix which drain to ileocaecal nodes, along blood supply from SMA
- bloodless fold of Treves - rins between ileum & mesoappendix (sapce under it is inferior ileocaecal recess
What is the management of incidental appendiceal NETs?
- tumours ≤1cm with clear resection margins, mesoappendiceal invasion <3mm, absence of angio or neuroinvasion and Ki67 <3% = appendiectomy only
- tumours 1-2cm, positive/unclear margins, mesoappendiceal invasion >3cmm, LVI, G2 proliferation rate (Ki67 3-20%) = consider right hemi
- tumours >2cm or G3 proliferation rate (Ki67>20%) = right hemi
What are goblet cell carcinomas of the appendix and how are they classified?
Type of adenocarcinoma showing combined mucinous & neuroendocrine differentiation.
Tang classification (A, B, C)
Considered more aggressive than other NETs, could behave more like appendiceal adenocarcinomas in terms of LN involvement, chance of peritoneal spread & prognosis - treat as adenocarcinomas; most guidelines say right hemi for all. If perforated w/o evidence of peritoneal spread CONSIDER adjuvant CRS and HIPEC. IF evidence of peritoneal spread deeemed resectable, adjuvant CRS & HIPEC should ALWAYS BE DONE.
How are incidental appendiceal LAMNs (found on histo) managed?
- no need for right hemi - appendicectomy sufficient
- if cellular or acellular mucin, regardless of whether perforated or not, with no postop rad/biochemical signs of residual disease, can consider adjuvant CRS and HIPEC
ANZJS Soucisse et al:
- type I LAMNs, completely resected: low risk for recurrence, f/u
- if positive margins or type 2 LAMNs (characterised by leakage of mucus thorugh appendix wall) - consider abdominal exploration with prophylactic HIPEC
How are incidental HAMNs of the appendix (found on histo) managed?
- if nonperforated pT<4,Nx,M0,R0 and no postop rad/biochem signs of residual disease, CAN CONSIDER adjuvant right sided hemi & CRS & HIPEC
- if perforated or M1b, DO R HEMI & CRS & HPEC
What is the management of an incidental appendiceal mucinous adenocarcinoma (found on histo)?
And a nonmucinous adenocarcinoma?
Mucinous adenocarcinoma:
- adjuvant right hemi always done +/- consider adding CRS and HIPEC especially if T4, perforated or if resection margins positive
- ?systemic chemo for stage III and high risk stage II as for nonmucinous adenocarcinoma
Nonmucinous adenocarcinoma:
- right hemi + systemic chemo if stage III or stage II w high risk features
What are the contraindications to CRS and HIPEC in appendiceal PMP?
- Absolute
- extensive SB serosal involvement, where not possible to leave ≥1.5-2m of SB
- mesenteric involvement causing retraction
- Relative
- age >75yrs
- aggressive histo w PCI >20
- involvement of liver hilum
- infiltration of anterior pancreatic surface
- ureteric obstruction
- need for complete gastric resection
- in pts w appendiceal PMP who aren’t fit for a major procedure and/or have unresectable disease, or if they have resectable disease but negative prognostic factors (high grade, signet ring cell histo), maximal tumour debulking (greater omentectomy, lower abdominal peritonectomies & an extended right hemicolectomy +/- bilateral oophorectomy) +/- HIPEC can be considered
What does CRS and HIPEC involve?
Cytoreductive surgery
- evaluate for any contraindications eg extensive SB serosal involvement, mesenteric disease compromising SB viability, heavy porta hepatis involvement, extensive retroperitoneal nodal disease or extensive liver mets
- excise peritoneum - sometimes all
- omentectomy routinely done & heavily involved organs excised - common resections include right hemi, anterior resection, splenectomy and segmental SB resections
HIPEC
- when complete or near complete cytoreduction obtained (ie all tumour nodules >0.25cm removed), HIPEC added to treat microscopic residual tumour cells
- depending on chemo agent & histo, tissue penetration into tumour nodules is 2-3mm
- heating the chemo enhances effect while having a direct cytotoxic effect on neoplastic cells
- different protocols; range from 30-90mins, most use Mitomycin C or oxaliplatin
Classification for appendiceal neoplasms
- epithelial neoplasms
- nonneoplastic mucinous (mucocele)
- mucinous epithelial neoplasms
- serrated polyp of appendix, w or w/o dysplasia
- LAMN
- HAMN
- mucinous adenocarcinoma, w or w/o signet ring cells
- nonmucinous epithelial neoplasms
- adenoma
- adenocarcinoma, w or w/o signet ring cells
- epithelial neoplasms with neuroendocrine features
- neuroendcrine tumour
- goblet cell carcinoma
- other neoplasms
- metastases
- mesenchymal eg GIST, lymphoma, granular cell tumour
How is PMP classified?
PSOGI/Sugarbaker
-
PMP
- acellular mucin
- low-grade mucinous carcinoma peritonei (M1b G1 / DPAM)
-
high-grade mucinous carcinoma peritonei
- well, moderately, poorly differentiated
- (M1b G2 or G3 / PMCA-I / moderately or poorly differentated PMCA)
-
high-grade mucinous carcinoma peritonei with signet ring cells
- poorly differentiated
- (M1b G3 / PMCA-S)
- Peritoneal carcinomatosis
Ronnett
- Disseminated peritoneal adenomucinosis (DPAM)
- PMCA-I (well differentiated peritoneal mucinous carcinomatosis)
- PMCA (moderately or poorly differentiated)
- PMCA-S (poorly differentiated with signet ring cells)
What is pseudomyxoma peritonei?
What is the pathophysiology of PMP?
PMP is a clinical condition characterized by diffuse collections of gelatinous material in the abdomen and pelvis, and mucinous implants on the peritoneal surfaces. It is not a histologically based term and is not used in the staging or histological classification of appendiceal neoplasms.
Mucinous appendiceal neoplasms are the leading cause of PMP and it can also be caused by mucinous adenocarcinomas and goblet cell tumours. Peritoneal seeding of all other appendiceal lesions = peritoneal metastases. PMP can also be caused by mucin-producing invasive adenocarcinomas of the large/small bowel, lung, breast, pancreas, stomach, bile ducts, GB & fallopian tubes/ovary.
Appendiceal PMP = a clinical entity that incorporates 2 malignant components; the appendix primary and secondary peritoneal disease - both have individual histo subclassification, sometimes with discordance.
In MANs, as the tumor grows and occludes the lumen, mucus accumulates, and the appendix ruptures. The peritoneum is then seeded with mucus-producing cells, which continue to proliferate and produce mucus. The progressive accumulation of copious amounts of mucinous fluid gradually fills the peritoneal cavity, resulting in the characteristic “jelly belly”.
What are the two eponymous signs associated with appendicitis in pregnancy?
- Adler’s sign - shifting tenderness suggests tubo-ovarian pathology rather than appendicits
- Bryan’s sign - pain when uterus is shifted to the right.
Classify appendiceal neoplasms
-
Neuroendocrine tumours (“Carcinoid”)
- 50%
-
Epithelial tumours
-
Mucinous
- Mucinous adenoma
- Low grade appendiceal mucinous neoplasm
- Mucinous adenocarcinoma
-
Non-mucinous
- Goblet cell carcinoma (“adenocarcinoid”)
- Intestinal type adenocarcinoma
- Signet ring cell adenomcarcinoma
-
Mucinous
What is the argument for early use of MRI in pregnant patients where concerns of appendicitis exist?
- Foetal loss in complicated appendicitis is ~6% (2% in early)
- Foetal loss in negative appendicectomy is ~4%
- Pre-term labour in complicated appendicitis is ~11% (6% in early)
- Pre-term labour in negative appendicectomy is ~10%
- Atypical presentations of appendicitis are present ~50% of the time in pregnant patients.
- Ultrasound accuracy is reduced in pregnancy - 78% sens, 83% spec
- MRI has halved the negative appendicectomy rate w/o a significant increase in perforation rate, and has been shown to be cost effective
- if MRI not available, surgery
- Some recommend CT - associated with 8% negative appendicectomy rate cf 32% by clinical assessment & USS combined
- these authors argued the amount of radiation delivered during a limited CT is below threshold required to induce fetal malformations & that most cases of appendicitis in pregnancy occur in 2nd or 3rd trimester, when organogenesis is already complete
Discuss imaging in appendicitis.
When do you do a CT to diagnose appendicitis?
- USS: sens 80%, spec 88% - high spec when positive but can’t exclude appendicitis
- >7mm = abnormal, bullseye appearance, on-compressible tender structure in RIF
- most useful in children or pregnancy
- CT: sens 95%, spec 99%
- thick-walled, >7mm diameter, mural enhancement, target sign/bullseye appearance, periappendiceal fat stranding +/- fluid/air if perf
- MRI: sens 100%, spec 98%
- reserved for pregnancy mainly, done w/o contrast
- >7mm, thickening >2mm, presence of inflammation
- a recent meta-analysis concluded CT is increasing in use and has reduced negative appendiectomy rates; proposed routine use of CT in adult pts
- I would request a CT if:
- there are other causes for RIF pain felt to be genuinely competitive w appendicitis as the diagnosis, eg sigmoid diverticulitis
- there is a history and exam consistent w appendix abscess or phlegmon, which may dictate non-op mx w PCI and delayed appendicectomy
- there is a mass
- typically used in older patients (>50) to confirm the diagnosis prior to surgery
