Awardee OrganizationUNIVERSITY OF CALIFORNIA AT DAVIS
Description
Abstract Text
Cancer Associated Retinopathies (CAR) occur most commonly in patients
with small cell carcinoma of the lung (SCCL), although this phenomenon
has also been encountered in patients with retinopathies associated with
breast, colon, prostate and cervical carcinomas. CAR degenerations
progress rapidly and are reported to manifest prior to the recognition of
the causal cancer. Serum samples obtained from CAR patients have
consistently demonstrated a specific antibody reaction with a 23 kDa
retina protein which is now referred to as the retinal CAR antigen. The
cloning of the cDNA corresponding to this antigen and its recognition as
the photoreceptor molecule 'Recoverin' has identified an important link
in the biological processes involved in these retinopathies. The
molecular cloning of a cDNA of the same nucleic acid sequence from a cDNA
library prepared from mRNA derived from a culture of SCCL identifies an
immunological 'Cancer Connection' which could be responsible for
initiating an autoimmune retinopathy. These finding introduce the
hypothesis that, in some cancer associated retinopathies, 'Molecular
Mimicry' is the cause of the collective indications of retinal
hypersensitivity.
The long term goals of this proposal are to investigate the pathogenesis
of CAR. To ascertain the significance of the 23 kDa retinal CAR
antigen/antibody reaction to vision loss in CAR patients and determine if
this immunological response is directly involved in the retinopathic
events that occur in CAR or is it simply a marker which identifies the
presence of a SCCL aberrantly expressing a distinctive retinal protein.
The specific aims are to (a) evaluate the incidence of expression of the
retinal CAR antigen in cultures of SCCL deposited in the ATCC as well as
in primary cultures of SCCL originated from CAR patients, (b) investigate
the immunological response of experimental animals to sensitization to
the potentially uveitogenic retinal CAR antigen and specific peptide
components of the molecule and (c) characterize the nature of the genes
expressing the retinal CAR antigen and the corresponding antigenic
component identified in the culture of small cell carcinoma of the lung.
The study will use a combination of immunological and molecular biology
techniques to determine if the indications of retinal hypersensitivity
associated with CAR represent an example of immune-mediated vision loss
resulting from antigenic cross-reactions.
No Sub Projects information available for 5R01EY009063-02
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