Rapidly growing dizzy, Hofmann asked his assistant to accompany him as he rode his bicycle home through the streets of Basel. For the next few hours he went through the full range of experiences that later users came to know as a bad trip. As well as having visual hallucinations, he became paranoid, alternated between feelings of intense restlessness and paralysis, babbled incoherently, feared choking, felt he had left his body, and perceived sounds visually. At some point Hofmann even considered the possibility that he might have suffered permanent brain damage. His symptoms gradually subsided, though his visual disturbances persisted for some time. Hofmann awoke the morning after this experience feeling totally normal, with a complete memory of what had happened but seemingly with no side effects.
In 1947 the Sandoz company began to market LSD as a tool in psychotherapy and in particular for the treatment of alcoholic schizophrenia. In the 1960s LSD became a popular drug for young people around the world. It was promoted by Timothy Leary, a psychologist and one-time member of the Harvard University Center for Research in Personality, as the religion of the twenty-first century and the way to spiritual and creative fulfillment. Thousands followed his advice to “turn on, tune in, drop out.” Was this alkaloid-induced escape from everyday life in the twentieth century so different from that experienced by women accused of witchcraft a few hundred years before? Though centuries apart, the psychedelic experiences were not always positive. For the flower children of the 1960s, taking the alkaloid-derivative LSD could lead to flashbacks, permanent psychoses, and in extreme cases suicide; for the witches of Europe, absorbing the alkaloids atropine and scopolamine from their flying salves could lead to the stake.
The atropine and ergot alkaloids did not cause witchcraft. Their effects, however, were interpreted as evidence against large numbers of innocent women, usually the poorest and most vulnerable in society. Accusers would make a chemical case against the witch: “She must be a witch, she says she can fly” or “she must be guilty, the whole village is bewitched.” The attitudes that had allowed four centuries of persecution of women as witches did not change immediately once the burnings were stopped. Did these alkaloid molecules contribute to a perceived heritage of prejudice against women—a view that may still linger in our society?
In medieval Europe the very same women who were persecuted kept alive the important knowledge of medicinal plants, as did native people in other parts of the world. Without these herbal traditions we might never have produced our present-day range of pharmaceuticals. But today, while we no longer execute those who value potent remedies from the plant world, we are eliminating the plants instead. The continuing loss of the world’s tropical rain forests, now estimated at almost two million hectares each year, may deprive us of the discovery of other alkaloids that would be even more effective in treating a variety of conditions and diseases.
We may never know that there are molecules with antitumor properties, that are active against HIV, or that could be wonder drugs for schizophrenia, for Alzheimer’s or Parkinson’s disease in the tropical plants that are daily becoming closer to extinction. From a molecular point of view, the folklore of the past may be a key to our survival in the future.
13. MORPHINE, NICOTINE, AND CAFFEINE
GIVEN THE HUMAN tendency to desire those things that make us feel good, it is not surprising that three different alkaloid molecules—morphine from the opium poppy, nicotine in tobacco, and caffeine in tea, coffee, and cocoa—have been sought out and prized for millennia. But for every benefit these molecules have brought to mankind, they have also offered danger. Despite, or maybe because of, their addictive nature, they have affected many different societies in many ways. And all three came together unexpectedly at one intersection in history.
THE OPIUM WARS
Although it is nowadays mainly associated with the Golden Triangle—the border region of the countries of Burma, Laos, and Thailand—the opium poppy, Papaver somniferum, is native to the eastern Mediterranean region. The products of the opium poppy may have been gathered and appreciated since prehistoric times. Evidence suggests that more than five thousand years ago the properties of opium were known in the Euphrates River delta, generally credited as the site of the first recognizable human civilization. Archaeological indications of the use of opium at least three thousand years ago have been unearthed in Cyprus. Opium was included in the herbal lists and healing remedies of the Greeks, Phoenicians, Minoans, Egyptians, Babylonians, and other civilizations of antiquity. Supposedly around 330 B.C., Alexander the Great took opium to Persia and India, from where cultivation slowly spread eastward and reached China in about the seventh century.
For hundreds of years opium remained a medical herb, either drunk as a bitter infusion or swallowed as a rolled pellet. By the eighteenth and particularly the nineteenth centuries artists, writers, and poets in Europe and the United States used opium to achieve a dreamlike state of mind that was thought to enhance creativity. Being less expensive than alcohol, opium also found a use by the poor as a cheap intoxicant. During these years its habit-forming qualities, if recognized, were seldom a concern. So pervasive was its use that even small babies and teething infants were dosed with opium preparations that were advertised as soothing syrups and cordials and that contained as much as 10 percent morphine. Laudanum, a solution of opium in alcohol often recommended for women, was widely consumed and available at any pharmacy without a prescription. It was a socially acceptable form of opium until it was prohibited in the early twentieth century.
In China opium had been a respected medicinal herb for hundreds of years. But the introduction of a new alkaloid-bearing plant, tobacco, changed the role of opium in Chinese society. Smoking was unknown in Europe until Christopher Columbus, at the end of his second voyage in 1496, brought tobacco back from the New World, where he had seen it in use. Tobacco use spread rapidly, despite severe penalties for its possession or importation in many Asian and Middle Eastern countries. In China in the middle of the seventeenth century the last emperor of the Ming dynasty prohibited the smoking of tobacco. Possibly the Chinese started to smoke opium as a substitute for the banned tobacco, as some reports suggest. Other historians credit the Portuguese from small trading posts on Formosa (now Taiwan) and Amoy in the East China Sea with introducing Chinese merchants to the idea of mixing opium with tobacco.
The effect of alkaloids such as morphine and nicotine, absorbed directly into the bloodstream through smoke inhaled into the lungs, is extraordinarily rapid and intense. When taken in this manner, opium quickly becomes addictive. By the beginning of the eighteenth century the smoking of opium was widespread throughout China. In 1729 an imperial edict banned the importation and sale of opium in China, but it was probably too late. An opium-smoking culture and a vast opium-related network of distribution and marketing already existed.
This is where our third alkaloid, caffeine, enters the story. Traders from Europe had previously found little satisfaction in trading with China. There were few commodities that China was willing to buy from the West, least of all the manufactured goods that the Dutch, British, French, and other European trading nations wanted to sell. But Chinese exports were in demand in Europe, particularly tea. Probably caffeine, the mildly addictive alkaloid molecule in tea, fueled the insatiable appetite of the West for the dried leaves of a shrub that had been grown since antiquity in China.
The Chinese were quite prepared to sell their tea, but they wanted to be paid in silver coin or bullion. For the British, buying tea with valuable silver was not their definition of trade. It soon became apparent that there was one commodity, though illegal, that the Chinese wanted and did not have. Thus Britain entered the opium business. Opium, cultivated in Bengal and other parts of British India by agents of the British East India Company, was sold to independent traders. It was then resold to Chinese importers, often under the protection of bribed Chinese officials. In 1839 the Chinese government attempted to halt this outlawed but flourishing trade. It confis
cated and destroyed a year’s supply of opium located in warehouses in Canton (present-day Guangzhou) and in British ships awaiting unloading in Canton’s harbor. Only days later a group of drunken British sailors was accused of killing a local farmer, giving the British an excuse to declare war on China. British victory in what is now called the First Opium War (1839-1842) changed the balance of trade between the nations. China was required to pay a very large amount in reparations, to open five Chinese ports to British trade, and to cede Hong Kong as a British crown colony.
Nearly twenty years later another Chinese defeat in the Second Opium War, involving the French as well as the British, wrung further concessions from China. More ports were opened to foreign trade, Europeans were allowed the right of residence and travel, freedom of movement was given to Christian missionaries, and ultimately the opium trade was legalized. Opium, tobacco, and tea became responsible for breaking down centuries of Chinese isolation. China entered a period of upheaval and change that culminated in the Revolution of 1911.
IN THE ARMS OF MORPHEUS
Opium contains twenty-four different alkaloids. The most abundant one, morphine, makes up about 10 percent of crude opium extract, a sticky, dried secretion from the poppy flowerpod. Pure morphine was first isolated from this poppy latex in 1803 by a German apothecary, Friedrich Serturner. He named the compound that he obtained morphine, after Morpheus, the Roman god of dreams. Morphine is a narcotic, a molecule that numbs the senses (thus removing pain) and induces sleep.
Intense chemical investigation followed Serturner’s discovery, but the chemical structure of morphine was not finally determined until 1925. This 122-year delay should not be seen as unproductive. On the contrary, organic chemists often view the actual deciphering of the structure of morphine as equally beneficial to mankind as the well-known pain-relieving effects of this molecule. Classical methods of structure determination, new laboratory procedures, an understanding of the three-dimensional nature of carbon compounds, and new synthetic techniques were just some of the results of the unraveling of this marathon chemical puzzle. Structures of other important compounds have been deduced because of the work done on the composition of morphine.
The structure of morphine. The darker lines of the wedge-shaped bonds point out of (above) the plane of the paper.
Today morphine and its related compounds are still the most effective painkillers known. Unfortunately, the painkilling or analgesic effect seems to be correlated with addiction. Codeine, a similar compound found in much smaller quantities (about 0.3 to 2 percent) in opium, is less addictive but is also a less powerful analgesic. The difference in structure is very small; codeine has a CH3O that replaces the HO at the position shown by the arrow on the structure below.
The structure of codeine. The arrow points to the only difference between codeine and morphine.
Well before the complete structure of morphine was known, attempts were made to modify it chemically in the hope of producing a compound that was a better pain reliever without addictive properties. In 1898, at the laboratory of Bayer and Company, the German dye manufacturer where, five years before, Felix Hofmann had treated his father with acetyl salicylic acid, chemists subjected morphine to the same acylation reaction that had converted salicylic acid to aspirin. Their reasoning was logical. Aspirin had turned out to be an excellent analgesic and a lot less toxic than salicylic acid.
The diacetyl derivative of morphine. The arrows indicate where CH3CO has replaced the Hs in the two HOs of morphine, producing heroin.
The product of replacing the Hs of the two OH groups of morphine with CH3CO groups was, however, a different matter. At first the results seemed promising. Diacetylmorphine was an even more powerful narcotic than morphine, so effective that extremely low doses could be given. But its effectiveness masked a major problem, obvious when the commonly accepted name for diacetylmorphine is known. Originally marketed as Heroin—the name refers to a “hero” drug—it is one of the most powerfully addictive substances known. The physiological effects of morphine and heroin are the same; inside the brain the diacetyl groups of heroin are converted back to the original OH groups of morphine. But the heroin molecule is more easily transported across the blood-brain barrier than is morphine, producing the rapid and intense euphoria craved by those who become addicted.
Bayer’s Heroin, initially thought to be free of the common side effects of morphine like nausea and constipation and therefore assumed also to be free of addiction, was marketed as a cough suppressant and a remedy for headaches, asthma, emphysema, and even tuberculosis. But as the side effects of their “super aspirin” became obvious, Bayer and Company quietly stopped advertising it. When the original patents for acetyl salicylic acid expired in 1917 and other companies began producing aspirin, Bayer sued for breach of copyright over the name. Not surprisingly, Bayer has never sued for copyright violation of the Heroin trade name for diacetylmorphine.
Most countries now ban the importation, manufacture, or possession of heroin. But this has done little to stop the illegal trade in this molecule. Laboratories that are set up to manufacture heroin from morphine often have a major problem disposing of acetic acid, one of the side products of the acylation reaction. Acetic acid has a very distinctive smell, that of vinegar, which is a 4 percent solution of this acid. This smell often alerts authorities to the existence of an illicit heroin manufacturer. Specially trained police dogs can detect faint traces of vinegar odor below the level of human sensitivity.
Investigation into why morphine and similar alkaloids are such effective pain relievers suggests that morphine does not interfere with nerve signals to the brain. Instead it selectively changes how the brain receives these messages—that is, how the brain perceives the pain being signaled. The morphine molecule seems able to occupy and block a pain receptor in the brain, a theory that correlates with the idea that a certain shape of chemical structure is needed to fit into a pain receptor.
Morphine mimics the action of endorphins, compounds found in very low concentrations in the brain that serve as natural pain relievers and that increase in concentration in times of stress. Endorphins are polypeptides, compounds made from joining amino acids together, end to end. This is the same peptide formation that is responsible for the structure of proteins such as silk (see Chapter 6). But whereas a silk molecule has hundreds or even thousands of amino acids, endorphins consist of only a few. Two endorphins that have been isolated are pentapeptides, meaning that they contain five amino acids. Both of these endorphin pentapeptides and morphine have a structural feature in common: they all contain a β-phenylethylamine unit, the same chemical construction that is thought responsible for affecting the brain in LSD, in mescaline, and in some other hallucinogenic molecules.
The β-phenylethylamine unit
Though the pentapeptide endorphin molecules are otherwise quite unlike the morphine molecule, this structural similarity is thought to account for the common binding site in the brain.
Structure of the morphine molecule, showing the β-phenylethylamine unit
But morphine and its analogs differ in biological activity from other hallucinogens in that they also have narcotic effects—pain-relief, sleep-inducing, and addictive components. These are thought to be due to another combination found in the chemical structure of, taken in order: (1) a phenyl or aromatic ring, (2) a quaternary carbon atom; that is, a carbon atom directly attached to four other carbon atoms, (3) a CH2-CH2 group attached to (4) a tertiary N atom (a nitrogen atom directly attached to three other carbon atoms).
(1) The benzene ring, (2) quaternary carbon atom (bolded), (3) the two CH2 groups with the carbons bolded, and (4) the tertiary nitrogen atom (bolded)
Combined, this set of requirements—known as the morphine rule—looks like:
Essential components for the morphine rule
You can see in the diagrams of morphine that all four requirements are present, as they also are in codeine and heroin.
Morphine stru
cture, showing how it fits the morphine rule for biological activit.
The discovery that this part of the molecule might account for narcotic activity is another example of serendipity in chemistry. Investigators injecting a man-made compound, meperidine, into rats noted that it caused them to hold their tails in a certain way, an effect previously seen with morphine.
Meperidine
The meperidine molecule was not particularly similar to the morphine molecule. What meperidine and morphine did have in common were (1) an aromatic or phenyl ring attached to (2) a quaternary carbon, followed by (3) the CH2-CH2 group and then a tertiary nitrogen; in other words, the same arrangement that was to become known as the morphine rule.
Highlighting the morphine rule for the meperidine or Demerol structure
Testing of meperidine revealed that it had analgesic properties. Usually known by the trade name Demerol, it is often used instead of morphine as, although it is less effective, it is unlikely to cause nausea. But it is still addictive. Another synthetic and very potent analgesic, methadone, like heroin and morphine, depresses the nervous system but does not produce the drowsiness or the euphoria associated with opiates. The structure of methadone is not a complete match to the requirements for the morphine rule. There is a CH3 group attached to the second carbon atom of the -CH2-CH2-. This very small change in structure is presumed responsible for the difference in biological activity.
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