TEXT E As people age, their cells
become less efficient and less able replace damaged components. At the same time
their tissues stiffen, For example the lungs and the heart muscle expand less
successfully, the blood vessels become increasingly rigid, and the ligaments and
tendons tighten. Few investigators would attribute such diverse
effects to a single cause. Nevertheless, researchers have discovered that a
process long known to discolor and toughen foods may also contribute to
age-related impairment of both cells and tissues. That process is nonenzymatic
glycosylation, whereby glucose becomes attached to proteins without the aid of
enzymes. When enzymes attach glucose to proteins (enzymatic glycosylation), they
do so at a specific site on a specific protein molecule for a specific purpose.
In contrast, the nonenzymatic process adds glucose haphazardly to any of several
sites along any available peptide chain within a protein molecule.
This nonenzymatic glycosylation of certain proteins has been understood by
food chemists for decades, although few biologists recognized until recently
that the same steps could take place in the body. Nonenzymatic glycosylation
begins when an aldehyde group (CHO) of glucose and an amino group (HN2) of a
protein are attracted to each other. The molecules combine, forming what is
called a Schiff base within the protein. This combination is unstable and
quickly rearranges itself into a stabler, but still reversible, substance known
as an Amadori product. If a given protein persists in the body
for months or years, some of its Amadori products slowly dehydrate and rearrange
themselves yet again, into new glucose-derived structures. These can combine
with various kinds of molecules to form irreversible structures named advanced
glycosylation end products (AGE’s). Most AGE’s are yellowish brown and
fluorescent and have specific spectrographic properties. More important for the
body, many are also able to cross-link adjacent proteins, particularly ones that
give structure to tissues and organs. Although no one has yet satisfactorily
described the origin of all such bridges between proteins, many investigators
agree that extensive cross-linking of proteins probably contributes to the
stiffening and loss of elasticity characteristic of aging tissues.
In an attempt to link this process with the development of cataracts (the
browning and clouding of the lens of the eye as people age), researchers studied
the effect of glucose on solutions of purified crystallin, the major protein in
the lens of the eye. Glucose-free solutions remained clear but solutions with
glucose caused the proteins to form clusters, suggesting that the molecules had
become cross-linked. The clusters diffracted light, making the solution opaque.
The researchers also discovered that the pigmented cross-links in human
cataracts have the brownish color and fluorescence characteristic of AGE’s.
These data suggest that nonenzymatic glycosylation of lens crystallins may
contribute to cataract formation. With which of the following statements concerning the stiffening of aging tissues would the author most likely agree
A.It paradoxically both helps and hinders the longevity of proteins in the human body. B.It can be counteracted in part by increased ingestion of glucose-free foods. C.It is exacerbated by increased enzymatic glycosylation. D.It probably involves the nonenzymatic glycosylation of proteins.