cochlear anatomy, function and pathology iii

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Cochlear anatomy, function and pathology III Professor Dave Furness Keele University d.n.furness @keele.ac.uk

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Page 1: Cochlear anatomy, function and pathology III

Cochlear anatomy, function and pathology III

Professor Dave FurnessKeele University

[email protected]

Page 2: Cochlear anatomy, function and pathology III

Aims and objectives of this lecture

• Focus (3) on the cochlear lateral wall and Reissner’s membrane:

– The spiral ligament

– The stria vascularis

– The endolymphatic potential and potassium recycling

– Reissner’s membrane

Page 3: Cochlear anatomy, function and pathology III

Homeostatic mechanisms generate a battery called the endocochlear(endolymphatic) potential which drives the sensitive transduction process

80 mV

0 mV

Page 4: Cochlear anatomy, function and pathology III

Fluid segregation

• The three chambers contain different fluids

• Endolymph, high in potassium, in scala media

• Perilymph, high in sodium, in scala vestibuliand scala tympani

Page 5: Cochlear anatomy, function and pathology III

Transduction by inner hair cells• The driving voltage of endocochlear potential and cell

membrane potential rapidly depolarises the cell which produces neurotransmitter from the base

stimulus

response

+80 mV

-70 mV

0 mV

Page 6: Cochlear anatomy, function and pathology III

Transduction to motion - the endocochlear potential powers the outer hair cell movement

stimulus

response

+80 mV

-70 mV

0 mV

Page 7: Cochlear anatomy, function and pathology III

Vulnerability of BM tuning to furosemide which inhibits generation of the EP

From: Robles and Ruggero, Physiological Reviews 81, No. 3, 2001

Page 8: Cochlear anatomy, function and pathology III

Structure of the lateral wall

Stria vascularis

Spiral ligament

Spiral prominence

Basilar crest

Page 9: Cochlear anatomy, function and pathology III

The stria vascularis

• Consists of three layers of cells: basal, intermediate and marginal

• Contains numerous blood vessels and melanocytes in pigmented animals

• Expresses proteins involved in potassium recycling such as potassium channels and sodium/potassium ATPases

• Basal and intermediate cells are connected together by gap junctions, and basal cells to adjacent cells of the spiral ligament (fibrocytes) also by gap junctions

Page 10: Cochlear anatomy, function and pathology III

Structure of the stria vascularis

Basal cell

Intermediate cells

Marginalcells

Page 11: Cochlear anatomy, function and pathology III

Structure of the stria vascularis

Basal cell

Intermediate cells

Marginalcells

Page 12: Cochlear anatomy, function and pathology III

The spiral ligament

• The ligament is a much neglected, yet important part of the cochlea

• It consists of extracellular matrix with several cell types in it and has a complex cytoarchitecture.

– The majority of cell types are called fibrocytes, of which there are five types

– There are also endothelial cells surrounding blood vessels/capillaries

– There are also root cells

Page 13: Cochlear anatomy, function and pathology III

Fibrocyte types

Type I

Page 14: Cochlear anatomy, function and pathology III

types

Type II

Page 15: Cochlear anatomy, function and pathology III

Fibrocytes – five types

Type III

Type III

Page 16: Cochlear anatomy, function and pathology III

Fibrocytes – five types

Type IV

Page 17: Cochlear anatomy, function and pathology III

Fibrocytes – five types

Type V

Page 18: Cochlear anatomy, function and pathology III

Sodium/potassium ATPase is localised to membrane processes

• Type II and type V cells possess many processes

• These strongly express the sodium/potassium ATPase and increase the surface area to increase the ability to exchange sodium and potassium

Page 19: Cochlear anatomy, function and pathology III

Fibrocytes express a range of proteins -some associated with homeostasis

• Sodium/potassium ATPase

• Aquaporin

• Glutamate transporter

• Potassium channels

• Gap junctions

• Calcium binding proteins

• Connective tissue growth factors

Page 20: Cochlear anatomy, function and pathology III

Fibrocyte protein expression is complex

• Each of these proteins has a different distribution

Page 21: Cochlear anatomy, function and pathology III

Fibrocyte structural features

• Membranes of all types are thrown into folds, but especially type II and type V which also express the most sodium/potassium ATPase

• Type III fibrocytes have a honeycomb membrane surface and are the only types to express aquaporin

• However, they also possess thick actin cables and are considered ‘tension’ fibrocytes, maintaining BM tension

• Type IV fibrocytes are similar in appearance to type III but lack the ATPase, aquaporin and actin cables

• Type I fibrocytes have few membrane folds and possess some ATPase

Page 22: Cochlear anatomy, function and pathology III

Fibrocyte membrane morphology is designed to increase surface area – type II

Page 23: Cochlear anatomy, function and pathology III

Type III fibrocytes also have increased surface area and contain actin cables attaching to ecm

and the bony wall

Page 24: Cochlear anatomy, function and pathology III

Root cells also contribute to homeostasis

• Root cells connect the outer sulcal cells to the ligament cells

• They possess potassium recycling proteins and are thought to assist in the recycling of potassium via the epithelial cell gap junction network

From: Jagger DJ et al. The Membrane Properties of Cochlear Root Cells are Consistent with Roles in Potassium Recirculation and Spatial Buffering. J Assoc Res Otolaryngol. 2010 Sep;11(3):435-48.

Page 25: Cochlear anatomy, function and pathology III

The extracellular matrix of the ligament• Dominated by type II and type IX collagen but

also contains type IV and type V

Page 26: Cochlear anatomy, function and pathology III

Ultrastructure of ligament ecm

Organised into thick and thin fibres and plaques of type II collagen connected by type IX collage fibrils

Page 27: Cochlear anatomy, function and pathology III

Ligament and stria work together to generate EP and recycle potassium

• Potassium recycling is necessary for maintenance of:– The endocochlear potential

– Transduction by the hair cells

– Amplification by the OHCs

• Potassium ions follow at least two routes, both ending up passing through fibrocytes and then into the stria vascularis

• This is a highly energy-dependent, metabolic process

Page 28: Cochlear anatomy, function and pathology III

Connexins

• Connexins play a vital role in the function of the lateral wall

• Connexin 26 and 30 are the dominant types and are localised to both stria vascularis and spiral ligament

Page 29: Cochlear anatomy, function and pathology III

Distribution of connexins 26 and 31

From: Jagger and Forge, 2015, Cell and Tissue Research 360, 633-644

Page 30: Cochlear anatomy, function and pathology III

Two potassium recycling routes

Page 31: Cochlear anatomy, function and pathology III

Possible mechanism of potassium recycling and generation of the endocochlear potential

Hibino,and Kurachi. 2006. Molecular and Physiological Bases of the K+ Circulation in the Mammalian Inner Ear. Physiology Vol. 21 no. 5, 336-345

Page 32: Cochlear anatomy, function and pathology III

Fibrocyte culture – one of the few cochlear cell types that can be grown long term in

vitro

• Fibrocytes are mesenchymal in origin

• This means they retain a capacity to divide, unlike hair cells and spiral ganglion neurones

• A bank of fibrocyte cultures has several uses:– Study the electrophysiology and their role in

generating the EP

– Develop stem cell/replacement cell therapy

– Investigate growth promoting factors to stimulate cell survival and proliferation in vivo

Page 33: Cochlear anatomy, function and pathology III

Fibrocytes grown on well plates in 2D look very flat

They resemble fibroblasts

They do not have an endogenous fibrocytephenotype

Page 34: Cochlear anatomy, function and pathology III

Fibrocyte cultures grown on hydrogels

Have a more fibrocytic appearance than when grown flat

Express characteristic proteins

Appear to form networks, perhaps with gap junctions between them

Page 35: Cochlear anatomy, function and pathology III

Reissner’s membrane – the third border of the scala media

Left: Mahendrasingam et al., 2011, JARO; Right Hackney and Furness, Noise and its Pathophysiology (eds Luxon and Prasher, 2007, Wiley)

3 week old mouse8 week old guinea pig

Page 36: Cochlear anatomy, function and pathology III

Reissner’s membrane

• Reissner’s membrane is required to separate endolymph from perilymph and so maintain the endocochlear potential

• Other functional roles are uncertain, but it appears to express epithelial sodium channels and chloride channels

• It is likely to be involved in homeostasis of sodium chloride between the scala media and the scala vestibuli/tympani

Page 37: Cochlear anatomy, function and pathology III

Structure of Reissner’s membrane

Scala vestibuli surface, mesothelial

Scala media surface, endothelial

Tight junctions

Page 38: Cochlear anatomy, function and pathology III

Summary

• The cochlear lateral wall plays a major role in cochlear function

• The cells present in the outer sulcus, spiral ligament and stria vascularis work together to recycle potassium and regenerate the endocochlear potential on a continuous basis

• The EP powers both transduction and amplification to maintain the sensitivity and frequency selectivity of the cochlea