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Juvenile Nasopharyngeal
Angiofibroma
DEPCIT
approach
Angus Shao
Definition
• Rare, benign
• Locally destructive fibrovascular tumour
JNA Otolaryngol Clin N Am 44 (2011)
989–1004
Epidemiology
• Males
• Teenage, young adult - range from 9 to 29
years (mean age, 15 years)
• 0.05% ? of H&N tumours
• Extremely rare in female/ patient older than
25
JNA Otolaryngol Clin N Am 44 (2011)
989–1004
Aetiology
• Unknown
• Theories:
–Nonchromaffin paraganglionic cells
–Vascular hamartoma (Girgis 1973)
–JNA stroma cells (Coutinho-Camillo 2008)
• Vascular endothelial growth factor receptor-2
• Transforming growth factor beta 1
• Insulin-like growth factor 2
• Deletion of chr 17 (p53)
Aetiology
• Hormonal Receptors (Montag 2006)
– Androgen
– Estrogen
• Embryologic chondrocartilage of skull bones (Schiff 1959)
– Superior margin of sphenopalatine foramen
– Trifurcation
• Palatine bone
• Horizontal ala of vomer
• Root of pterygoid process
Origin
(Operative Techniques in Otolaryngology 1999; 10(2): 101-106.)
Controversial
• Posterolateral nasal wall at
sphenopalatine foramen
• Vidian canal
Pathology
• Macro
– well defined, mucosalised, red/purple lobulated
mass arising in the nasopharynx from the lateral
wall, posterior to MT
Pathology
• Micro
– non-encapsulated, fibrous pseudocapsule
– spindle/stellate cells in a rich collagen matrix
– with vascular spaces devoid of elastic fibers (elastic
lamina)
• Lack muscularis layer
– Partially androgen dependent
• Receptors for testosterone, DHT, Androgen
– not useful in Tx
– B-catenin mutation
• APC/B-catenin mutation in FAP
• JNA 25 times more likely in FAP - controversial
(Hauptman 2007)
Clinical
• Adolescent male
• Unilateral nasal
obstruction most common
• Recurrent epistaxis
• Nasal mass
– Smooth, lobulated
– Compressible
– Purplish or reddish hue
(Operative Techniques in Otolaryngology 2011; 22(4):281-284.)
Staging
• No universal staging system
• Most commonly accepted:
– Radkowski
(Radkowski 1996)
Investigation
• Bloods
• Biopsy??!!!!
• Imaging
Timing of surgery related to
embolisation
• Within 24 hr  negate the benefits of
embolization, insufficient devascularization and
tumor necrosis  greater operative blood loss
• thrombus formation and multinucleated giant cell
reaction within 7 days of embolization
• recanalization and partial revascularization can be
observed in 30% of embolized vessels after 7 days
• Maximal tumour softening observed at 8 days
J NeuroIntervent Surg doi:10.1136/neurintsurg-2012-010350
Treatment
• Surgical disease
• Open vs Endoscopic
• Rtx (unresectable) / Chemotherapy(rarely)
• Hormonal therapy
• Observation? !
Open Approach
• Transpalatal
• Lateral Rhinotomy
• Mandibular swing
• Midfacial degloving
Endoscopic
• Shift towards endoscopic approach in last 10
years
• Mostly for early disease
• Endoscopic appropriate up to stage IIIA
tumors (Wormald 2003)
Endoscopic Coblation Technique
Annals of Otology, Rhinology & Laryngology
122(6):353-357.
Summary
• Benign rare but locally destructive disease in
adolescent male
• Fibrovascular tumour originated at SPF/Vidian
canal
• Surgery is the treatment of choice (most)
• Shift to endoscopic approach with similar rate
of recurrence compared to open technique

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Jna reg presentation

  • 2. Definition • Rare, benign • Locally destructive fibrovascular tumour JNA Otolaryngol Clin N Am 44 (2011) 989–1004
  • 3. Epidemiology • Males • Teenage, young adult - range from 9 to 29 years (mean age, 15 years) • 0.05% ? of H&N tumours • Extremely rare in female/ patient older than 25 JNA Otolaryngol Clin N Am 44 (2011) 989–1004
  • 4. Aetiology • Unknown • Theories: –Nonchromaffin paraganglionic cells –Vascular hamartoma (Girgis 1973) –JNA stroma cells (Coutinho-Camillo 2008) • Vascular endothelial growth factor receptor-2 • Transforming growth factor beta 1 • Insulin-like growth factor 2 • Deletion of chr 17 (p53)
  • 5. Aetiology • Hormonal Receptors (Montag 2006) – Androgen – Estrogen • Embryologic chondrocartilage of skull bones (Schiff 1959) – Superior margin of sphenopalatine foramen – Trifurcation • Palatine bone • Horizontal ala of vomer • Root of pterygoid process
  • 6. Origin (Operative Techniques in Otolaryngology 1999; 10(2): 101-106.) Controversial • Posterolateral nasal wall at sphenopalatine foramen • Vidian canal
  • 7. Pathology • Macro – well defined, mucosalised, red/purple lobulated mass arising in the nasopharynx from the lateral wall, posterior to MT
  • 8. Pathology • Micro – non-encapsulated, fibrous pseudocapsule – spindle/stellate cells in a rich collagen matrix – with vascular spaces devoid of elastic fibers (elastic lamina) • Lack muscularis layer – Partially androgen dependent • Receptors for testosterone, DHT, Androgen – not useful in Tx – B-catenin mutation • APC/B-catenin mutation in FAP • JNA 25 times more likely in FAP - controversial (Hauptman 2007)
  • 9. Clinical • Adolescent male • Unilateral nasal obstruction most common • Recurrent epistaxis • Nasal mass – Smooth, lobulated – Compressible – Purplish or reddish hue (Operative Techniques in Otolaryngology 2011; 22(4):281-284.)
  • 10. Staging • No universal staging system • Most commonly accepted: – Radkowski (Radkowski 1996)
  • 12. Timing of surgery related to embolisation • Within 24 hr  negate the benefits of embolization, insufficient devascularization and tumor necrosis  greater operative blood loss • thrombus formation and multinucleated giant cell reaction within 7 days of embolization • recanalization and partial revascularization can be observed in 30% of embolized vessels after 7 days • Maximal tumour softening observed at 8 days J NeuroIntervent Surg doi:10.1136/neurintsurg-2012-010350
  • 13. Treatment • Surgical disease • Open vs Endoscopic • Rtx (unresectable) / Chemotherapy(rarely) • Hormonal therapy • Observation? !
  • 14. Open Approach • Transpalatal • Lateral Rhinotomy • Mandibular swing • Midfacial degloving
  • 15. Endoscopic • Shift towards endoscopic approach in last 10 years • Mostly for early disease • Endoscopic appropriate up to stage IIIA tumors (Wormald 2003)
  • 17. Annals of Otology, Rhinology & Laryngology 122(6):353-357.
  • 18. Summary • Benign rare but locally destructive disease in adolescent male • Fibrovascular tumour originated at SPF/Vidian canal • Surgery is the treatment of choice (most) • Shift to endoscopic approach with similar rate of recurrence compared to open technique

Editor's Notes

  1. Advanced Facial swelling/mass Proptosis Cranial neuropathy Headaches Massive hemorrhage
  2. CT MRI Angio
  3. Review article in 2012 Head, neck and brain tumor embolization guidelines Duffis et al
  4. Yi et al (2013) described a simplified classification system and management option for juvenile nasopharyngeal angiofibroma, as follows[10] : Type I includes tumor localized in the nasal cavity, paranasal sinus, nasopharynx, or pterygopalatine fossa. The transnasal cavity approach with endoscopic guidance is suitable for this type. Type II is if the lesion extends into the infratemporal fossa, cheek region, or orbital cavity, with anterior and/or minimal middle cranial fossa extension but intact dura mater. The transantral-infratemporal fossa-nasal cavity combined approach is reliable for type II. Type III is a calabashlike, massive tumor lobe in the middle cranial fossa. For type III tumors, the complete removal is challenging. A combined extracranial and intracranial approach is often needed. Radiotherapy is useful for treating the residual intracranial part.
  5. KTP-laser embolization (Hazarika 2002) Gamma knife (Dare 2003, Park 2006) Coblation (Ruiz 2012) Stage I-IIIa disease