Durante la oculogénesis y después se establecen importantes zonas o puntos de fijación entre el

vítreo y las estructuras circundantes.

La base del humor vítreo mantiene una fijación firme durante toda la vida al epitelio de la pars
plana y a la retina que se sitúa justo por detrás de la ora serrata. La fijación a la cápsula del
cristalino y a la papila es firme en etapas tempranas de la vida pero pronto desaparece y su
viscosidad varía con la edad.

En otros puntos el gel cortical que constituye la membrana hialoidea posterior se adhiere a la
retina a través de la "lámina limitante interna", siendo esta inserción más fuerte en la ora serrata,
en la papila y en la zona foveal.

Uniones vítreas:

The peripheral or outer layer of vitreous is known as the vitreous cortex. The posterior vitreous cortex,
which lies along the inner retina, is approximately 100 μm thick, but is thinner over the macula and absent
over the optic disc.

In the vitreous cortex, there is less hyaluronic acid, the collagen fibrils are more densely packed, and the
vitreous gel is correspondingly denser compared with the central vitreous cavity. 5,17 Following vitreous
separation from the retina, the collagen fibrils composing the outer surface of the vitreous cortex become
further condensed and realigned to form a distinct membrane known as the posterior hyaloid membrane.

The vitreous is most firmly attached to the retina at those sites where the ILM is thinnest, including the
vitreous base, along major retinal vessels, the optic disc margin, and the 500-μm-diameter foveola

The condensed collagen fibrils that form the vitreous cortex insert superficially into the ILM of the retina (or
basal lamina of Müller cells).20,21 The precise nature of the adhesion between the posterior vitreous cortex
and the ILM is not known but is thought to result in part from physicochemical properties of extracellular
matrix molecules.12,2

The vitreous is most firmly attached to the retina at those sites where the ILM is thinnest, including the
vitreous base, along major retinal vessels, the optic disc margin, and the 500-μm-diameter foveola

The attachment between the vitreous gel and its surrounding tissues is greatest in the vitreous base, where
the concentration of vitreous collagen fibrils is especially high. 12,20 Following the vitreous base, the
peripheral margin of the optic nerve head (and immediate peripapillary retina) is the zone of firmest
adhesion between the cortical vitreous and retinal surface. 12 Here, vitreous fibrils are intermeshed with
microscopic gaps in the basal lamina and often with astroglial epipapillary membranes. 25 Clinical evidence of
this firm attachment zone is the ring of thickened tissue (Weiss ring) visible on the posterior hyaloid
membrane overlying the optic nerve following vitreopapillary separation during PVD
The ILM is thicker posteriorly than anteriorly, reaching its maximal thickness of approximately 25,000 Å in
the posterior retina.20,21 However, at the crest of the foveal clivus, it begins to rapidly thin, becoming
extremely thin (200 Å or less) at the foveola. 20 In a scanning electron microscopic study of autopsy eyes with
spontaneous PVD, Kishi and coworkers 23 found remnants of vitreous cortex in the foveal area in 26 (44%) of
59 eyes. Most remnants had the configuration of a 500-μm-diameter plaque or ring of vitreous adherent to the
foveola. In some eyes, a 1,500-μm-diameter ring of vitreous remnants was found adherent to the foveal
margin. These observations strongly suggest that the central 500-μm foveolar area and the margin of the
1,500-μm fovea are sites of firm vitreoretinal adhesion. These observations are consistent with the thinness of
the ILM in the foveal area and possibly with the distribution of ILM attachment plaques (hemidesmosomes)
in the posterior retina.12,20
In addition to these zones of firm vitreoretinal adhesion in the posterior pole, there are several types of
lesions in the peripheral fundus associated with abnormally strong vitreoretinal attachments. These include
lattice degeneration, meridional complexes, cystic retinal tufts, firm paravascular attachments, and some
chorioretinal scars.7 Such lesions play an important role in the complications of complete PVD.

Área menor a 500um: Agujero macular.

Área Mayor a 1500um: Tracción macular -> Edema cistoideo por tracción.

Etapas de desprendimiento vítreo posterior:

1.- Adherencia vitreofoveal residual.

2.- DVP macular sin adherencia vitreofoveal.

3.- DVP completo con adhesión vitreopapilar.

4.- DVP completo.

Complicaciones:

Leves (Precoces): MER, Agujero macular, Punto Foveal Rojo (clínica), AM idiopático, Tracción EMD.
EMC y maculopatía miope, síndrome de tracción vitreopapilar.

Tardías (Final, DVP completo): Hemorragia retinal, papilar y vítreo. Desprendimiento de retina.

Fenómenos de degeneración del vítreo

LIQUEFACTION AND SYNERESIS

Orden:

1.- Anatomía y composición vítreo

Generalidades (Morfología)

Vítreo Primario y Vítreo Secundario (Embriología básica)

Base, Corteza vítrea y Hialoides (Composición)

2.- Adherencias vítreas

Ubicación

Mecanismo

Importancia

Interfase Vítreoretinal: Hialoides y MLI

3.- Fisiología: Funciones:

-Estabilidad morfológica (Soporte)

-Barrera de difusión

-Taponamiento metabólico

-Estructura Óptica

4.- Envejecimiento Vítreo: Licuefacción y sinquisis

“Factores de riesgo”

Teorías

Complicaciones.

Duda: Si el vítreo actúa como reservorio de elementos (glucosa, VEGF H, Vitamina C,

etc), entonces, al inyectar Avastín o algún fármaco, ¿Éste no debería ver afectada su
farmacocinética? ¿Debería tenerse en cuenta la licuefacción del vítreo al momento de plantear
esta terapia? ¿Sería pertinente en algunos casos la terapia con anti-VEGF + Vitrectomía?(Riesgo
de GNV por pérdida de barrera de difusión)