Press Release: The 1999 Nobel Prize in Physiology or
Medicine
NOBELFÖRSAMLINGEN KAROLINSKA INSTITUTET
THE NOBEL ASSEMBLY AT
THE KAROLINSKA INSTITUTE
11 October 1999
The Nobel Assembly at Karolinska
Institutet has today decided to award the Nobel Prize in
Physiology or Medicine for 1999 to
Günter Blobel
for the discovery that
"proteins have intrinsic
signals that govern their transport and localization in the
cell"
Summary
A large number of proteins carrying out
essential functions are constantly being made within our cells.
These proteins have to be transported either out of the cell, or to
the different compartments - the organelles - within the cell. How
are newly made proteins transported across the membrane surrounding
the organelles, and how are they directed to their correct
location?
These questions have been answered through the
work of this year’s Nobel Laureate in Physiology or Medicine, Dr
Günter Blobel, a cell and molecular biologist at the Rockefeller
University in New York. Already at the beginning of the 1970s he
discovered that newly synthesized proteins have an intrinsic signal
that is essential for governing them to and across the membrane of
the endoplasmic reticulum, one of the cell’s organelles. During the
next twenty years Blobel characterized in detail the molecular
mechanisms underlying these processes. He also showed that similar
"address tags", or "zip codes", direct proteins to other
intracellular organelles.
The principles discovered and described by
Günter Blobel turned out to be universal, operating similarly in
yeast, plant, and animal cells. A number of human hereditary
diseases are caused by errors in these signals and transport
mechanisms. Blobel’s research has also contributed to the
development of a more effective use of cells as "protein factories"
for the production of important drugs.
Several important functions
An adult
human being is made up of approximately 100,000 billion cells. A
cell contains many different compartments, organelles, each
surrounded by a membrane. The organelles are specialized to carry
out different tasks. The cell nucleus, for instance, contains the
genetic material (DNA) and thus governs all functions of the cell.
The mitochondria are the "power plants" producing energy needed by
the cell, and the endoplasmic reticulum is, together with the
ribosomes, responsible for synthesizing proteins.
Every cell contains approximately one billion
protein molecules. The different proteins have a large number of
important functions. Some constitute the building blocks for
constructing the cell while others function as enzymes catalyzing
thousands of specific chemical reactions. The proteins within a cell
are constantly degraded and resynthesized. The number of amino acids
- the building blocks making up all proteins - may in a single
protein range from about 50 to several thousands, forming long,
folded chains.
How do proteins cross the barriers?
Thus, it was for a long time a puzzle how large proteins could
traverse the tightly sealed, lipid-containing, membranes surrounding
the organelles. Some decades ago, it was also unknown how newly made
proteins were directed to their correct locations in the cell.
Günter Blobel was going to solve both of these
puzzles. At the end of the 1960s he joined the famous cell biology
laboratory of George Palade at the Rockefeller Institute in New
York. Here, during two decades, scientists had studied the structure
of the cell and the principles for the transport of newly
synthesized proteins out of the cell. This work earned George Palade
the Nobel Prize in Physiology or Medicine in 1974 (which he shared
with the Belgian scientists Albert Claude and Christian de
Duve).
"The signal hypothesis"
Günter
Blobel’s research was built on the traditions of Palade´s
laboratory. In particular, Blobel studied how a newly made protein,
destined to become transported out of the cell, is targeted to a
specialized intracellular membrane system, the endoplasmic
reticulum. In 1971 he formulated a first version of the "signal
hypothesis". He postulated that proteins secreted out of the cell
contain an intrinsic signal that governs them to and across
membranes.
Based on elegant biochemical experiments, Blobel
described in 1975 the various steps in these processes. The signal
consists of a peptide, i.e. a sequence of amino acids in a
particular order that form an integral part of the protein. He also
suggested that the protein traverses the membrane of the endoplasmic
reticulum through a channel (Fig. 1). During the next twenty years,
Blobel and coworkers step by step characterized the molecular
details of these processes. Eventually it was shown that the signal
hypothesis was both correct and universal, since the processes
operate in the same way in yeast, plant, and animal cells.
"Address tags" for organelle
localization
In collaboration with other research groups,
Günter Blobel was soon able to show that similar intrinsic signals
target the transport of proteins also to other intracellular
organelles. On the basis of his results, Günter Blobel formulated in
1980 general principles for the sorting and targeting of proteins to
particular cell compartments. Each protein carries in its structure
the information needed to specify its proper location in the cell.
Specific amino acid sequences (topogenic signals) determine whether
a protein will pass through a membrane into a particular organelle,
become integrated into the membrane, or be exported out of the cell.
A range of signals that govern proteins to the
different parts of the cell have now been identified (Fig. 2),
showing that the principles formulated by Blobel are correct. These
signals can be compared to address tags or zip codes which ensure
that a traveler's luggage arrives at the correct destination, or a
letter reaches its correct addressee. These signal sequences are in
fact a chain of different amino acids present either as a short
"tail" at one end of the protein, or sometimes located within the
protein.
Significance of Blobel's discovery
Günter Blobel's discovery has had an immense impact on modern
cell biological research. When a cell divides, large amounts of
proteins are being made and new organelles are formed. If the cell
is to function correctly, the proteins have to be targeted to their
proper locations. Blobel´s research has substantially increased our
understanding of the molecular mechanisms governing these processes.
Furthermore, knowledge about the topogenic signals has increased our
understanding of many medically important mechanisms. For example,
our immune system uses topogenic signals, e.g. in the production of
antibodies.
Blobel's research has helped explain the
molecular mechanisms behind several genetic diseases. If a sorting
signal in a protein is changed, the protein could end up in a wrong
location in the cell. One example is the hereditary disease primary
hyperoxaluria, which causes kidney stones already at an early age.
In some forms of familial hypercholesterolemia, a very high level of
cholesterol in the blood is due to deficient transport signals.
Other hereditary diseases, e.g. cystic fibrosis, are caused by the
fact that proteins do not reach their proper destination.
Future applications
In the near
future the entire human genome will be mapped. As a result one can
also deduce the structure and topogenic signals of the proteins.
This knowledge will increase our understanding of processes leading
to disease and can be used to develop new therapeutic strategies.
Already today drugs are produced in the form of proteins, e.g.
insulin, growth hormone, erythropoetin and interferon. Usually
bacteria are used for the production of the drug, but in order to be
functional certain human proteins need to be synthesized in more
complex cells, such as yeast cells. With the help of gene technology
the genes of the desired proteins are provided with sequences coding
for transport signals. The cells with the modified genes can then be
efficiently used as protein factories.
Increased knowledge about the process by which
proteins are being directed to different parts of the cell also
makes it possible to construct new drugs that are targeted to a
particular organelle to correct a specific defect. The ability to
reprogram cells in a specific way will also be important for future
cell and gene therapy.
 |
|
Fig. 1. "The signal hypothesis".
Proteins which are to be exported out of the cell are
synthesized by ribosomes, associated with the endoplasmic
reticulum. The genetic information from DNA is transferred via
messenger RNA (mRNA). This information determines how the
amino acids build up the proteins. First, a signal peptide is
formed as a part of the protein. With the help of binding
proteins, the signal peptide directs the ribosome to a channel
in the endoplasmic reticulum. The growing protein chain
penetrates the channel, the signal peptide is cleaved, and the
completed protein is released into the lumen of the
endoplasmic reticulum. The protein is subsequently transported
out of the cell. |
 |
|
Fig. 2. Examples of directed transport
mediated by topogenic signals. The figure shows a schematic
cell with some of its compartments, the organelles. (A
chloroplast is an organelle that is present in plant cells but
not in animal cells). The organelles have special functions
and they are surrounded by membranes. Newly synthesized
proteins are provided with special "address tags", signal
sequences or topogenic signals, which direct the proteins to a
correct place within the cell and allow them to cross the
membranes of the organelles. The signal itself consists of a
chain of amino acids. It is an integral part of the protein,
and it is often located at one end of the
protein. |
| 
