Category Science

Why countries urged to cut down on plastic?

The Southeast Asian importers became swamped with waste posing significant threat to the environment. The sheer quantity of imported scrap not only overwhelmed ports, but also caused a sharp uptick in illegal recycling operations. Illegal recyclers dumped toxic wastewater into waterways and polluted the air with fumes from burning plastic.

These countries began to face backlash from the public and environmental groups, who used officials to permanently ban the import of plastic waste. This made countries send unwanted and contaminated waste back to the countries it came from and to impose new controls.

  • In 2018, Malaysia announced bans on imports of plastic scrap by 2021. Malaysia has revoked import permits and has been clamping down on illegal processing plants.
  • Thailand has temporarily prohibited plastic waste import.
  • Indonesia has restricted the import of non-recyclable waste and Vietnam will bar all imports of plastic scrap by 2025.
  • India announced that a ban on import of plastic waste would began in August, 2019.

 

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Why did China stop taking recycling?

China was the world’s biggest importer of scrap plastic, receiving close to half of the world’s global plastic waste for three decades. But serve pollution concerns prompted the country to impose a ban on plastic waste import abruptly in January 2018. This shook up the global garbage/scrap trade. With the primary importer of plastic waste out of the market, exporting countries began sending increasing volumes of scrap to Southeast Asia, with Malaysia emerging as the number one importer. Vietnam, Thailand and Indonesia also picked up a lot of the slack. Malaysia’s imports rose five-fold and the Philippines’, three-fold.

The recycling crisis triggered by China’s ban could have an upside, experts say, if it leads to better solutions for managing the world’s waste, such as expanding processing capacities in North America and Europe, and spurring manufacturers to make their products more easily recyclable. Above all, experts say it should be a wake-up call to the world on the need to sharply cut down on single-use plastics.

Over the coming decade, as many as 111 million tons of plastics will have to find a new place to be processed or otherwise disposed of as a result of China’s ban, according to Brooks and University of Georgia engineering professor Jenna Jambeck. However, the places trying to take up some of the slack in 2018 tended to be lower-income countries, primarily in Southeast Asia, many of which lack the infrastructure to properly handle recyclables. Many of those countries were quickly overwhelmed by the volume and have also now cut back on imports.

 

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Why some countries are shipping back plastic waste?

For many years now, wealthier nations have been shipping their waste including paper, plastic, metal and electronic items, to developing countries, which recycle them and use them as raw material in their manufacturing businesses. For the former, it’s a cheap way to dispose of their waste, and for the latter, waste is a valuable source of income. But in recent months, the global waste trade has been facing a crisis. A growing number of countries are demanding that nations take back their plastic waste. Malaysia, the Philippines and Indonesia have started to send contaminated waste back to where it came from. Returning 42 shipping containers of illegally imported plastic waste to the U.K., Malaysia’s Environment Minister Yeo Bee Yin announced last month that Malaysia would take steps to ensure it does not become the garbage dump of the world. In 2019, the Philippines shipped back 69 containers of plastic to Canada that it said was falsely labelled as recyclable in 2013 and 2014.

Global trade in plastic waste is a big business. According to an estimate, from 1988 to 2016, the top 10 plastic waste exporters shipped 168 million tonnes, most of it to China. Exporting is seen as a cheaper option than sorting, cleaning, recycling or reusing it locally.

In developing countries on the other hand, recyclers line up to buy this waste and turn it into new products.

In the recent past, countries found themselves dealing with huge volumes of waste they are ill-prepared to handle. Such waste also contains a variety of materials, chemical additives and dyes that make it next to impossible to recycle. Workers who process these shipments are often exposed to hazardous chemicals. Further, the plastic that cannot be recycled is disposed of in incinerators, landfills, thereby polluting the air, land and sea. Worries about receiving such waste have forced countries to act.

The Exporters

  • Garbage is exported from about a dozen developed countries, including the U.S., Canada, France, Belgium, Germany, Spain, the Netherlands and the U.K., according to Greenpeace.
  • The European Union is the largest exporter of plastic waste, with the U.S. leading as the top exporter for a single country.

The Importers

  • The list predominantly includes Asia countries such as China, Malaysia, India, Indonesia, Vietnam, Thailand, the Philippines, South Korea, Taiwan, and Hong Kong. They import some form of waste or the other.
  • About 1,21,000 metric tonnes of plastic waste is imported to India.
  • Interestingly, some developed countries too import plastic waste. They include Germany, the U.S., Italy, Canada, Sweden, France, the U.K., the Netherlands and Belgium.

 

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HOW DO VACCINATIONS WORK?

In 1796, an English doctor called Edward Jenner (1749-1823) gave the first vaccination. He realized that milkmaids who caught cowpox did not catch the very dangerous disease of smallpox. By injecting the cowpox virus into a child, he was able to vaccinate him against the more serious disease. As the body fights the virus, antibodies are formed in the blood that prevents further infections or infection by some similar viruses. Today, huge vaccination programmers ensure that most children are protected against a range of diseases.

A person may become immune to a specific disease in several ways. For some illnesses, such as measles and chickenpox, having the disease usually leads to lifelong immunity to it. Vaccination is another way to become immune to a disease. Both ways of gaining immunity, either from having an illness or from vaccination, are examples of active immunity. Active immunity results when a person’s immune system works to produce antibodies and activate other immune cells to certain pathogens. If the person encounters that pathogen again, long-lasting immune cells specific to it will already be primed to fight it.

A different type of immunity, called passive immunity, results when a person is given someone else’s antibodies. When these antibodies are introduced into the person’s body, the “loaned” antibodies help prevent or fight certain infectious diseases. The protection offered by passive immunization is short-lived, usually lasting only a few weeks or months. But it helps protect right away.

Infants benefit from passive immunity acquired when their mothers’ antibodies and pathogen-fighting white cells cross the placenta to reach the developing children, especially in the third trimester. A substance called colostrum, which an infant receives during nursing sessions in the first days after birth and before the mother begins producing “true” breast milk, is rich in antibodies and provides protection for the infant. Breast milk, though not as rich in protective components as colostrum, also contains antibodies that pass to the nursing infant. This protection provided by the mother, however, is short-lived. During the first few months of life, maternal antibody levels in the infant fall, and protection fades by about six months of age.

Passive immunity can be induced artificially when antibodies are given as a medication to a nonimmune individual. These antibodies may come from the pooled and purified blood products of immune people or from non-human immune animals, such as horses. In fact, the earliest antibody-containing preparations used against infectious diseases came from horses, sheep, and rabbits.

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HOW ARE NEW DRUGS DEVELOPED?

Research chemists examine different chemicals to find out how they react with other chemicals and with living cells. When a mixture of chemicals is thought to have potential in the treatment of certain conditions, various combinations of the chemicals will be tested to see whether they might be dangerous to living things. Tests on individual cells and on animals are made before human beings are given the new drug. Many people think that drug-testing on animals is wrong, but others feel that this is the best way to make sure that drugs are safe. Trials of the drug, in which some patients are given a placebo (a drug with no active ingredients), carried out to assess the drug’s effectiveness. It is usually only after many years of testing and monitoring that the drug is released for use by doctors.

The journey will have begun in a university laboratory where researchers, with grants from the research bodies or the pharmaceutical industry, have undertaken basic research to understand the processes behind a disease, often at a cellular or molecular level. It is through better understanding of disease processes and pathways that targets for new treatments are identified. This might be a gene or protein instrumental to the disease process that a new treatment could interfere with, for example, by blocking an essential receptor.

Once a potential target has been identified, researchers will then search for a molecule or compound that acts on this target. Historically, researchers have looked to natural compounds from plants, fungi or marine animals to provide the basis for these candidate drugs but, increasingly, scientists are using knowledge gained from the study of genetics and proteins to create new molecules using computers. As many as 10,000 compounds may be considered and whittled down to just 10 to 20 that could theoretically interfere with the disease process.

The next stage is to confirm that these molecules have an effect and that they are safe. Before any molecules are given to humans, safety and efficacy tests are conducted using computerised models, cells and animals. Around half of candidates make it through this pre-clinical testing stage and these five to 10 remaining compounds are now ready to be tested in humans for the first time. In the UK, approval by the Medicines and Healthcare products Regulatory Agency (MHRA) is required before any testing in humans can occur. The company will put in a clinical trial application (CTA), which will be reviewed by medical and scientific experts, who will decide whether or not sufficient preliminary research has been conducted to allow testing in humans to go ahead.

Each year sees a couple of dozen new drugs licensed for use, but in their wake there will be tens of thousands of candidate drugs that fell by the wayside. The research and development journey of those new drugs that make it to market will have taken around 12 years and cost around £1.15bn.

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WHAT CAUSES ILLNESS?

Understanding the cause of an illness can often help a doctor to bring a patient back to good health or to suggest ways to prevent the illness from recurring or affecting other people. Illness may he caused by an accident, which physically affects part of the body, or it may be brought about by tiny organisms such as bacteria and viruses. Antibiotics are used to treat bacterial infections, while antiviral drugs attack viruses. In both cases, some disease-causing organisms are resistant to drug therapy. Occasionally, the cells of the body seem to act in destructive ways for no obvious reason. This is what happens in some forms of cancer. However, researchers are finding new ways to combat disease all the time.

A complex illness contains two or more elements of illness, causal illness, injury illness and blockage illness, with a single cause. A complex illness requires a cure for each illness element.

For complex illnesses, the first cure is to address the cause.  The second cure is to heal the damage, the third to transform the negative attributes that resulted from illness and from healing. It is possible, sometimes necessary to work on elemental cures out of sequence, or at the same time. However, cures can seldom be completed out of sequence, because the prior illness is a cause, and the illness will recur.

The hierarchy is also a hierarchy of life and of health. It is also useful to view the hierarchy of illness. An illness can exist in a single cell, the simplest life form. A single cell might have an illness with a single cause that causes an injury that is healed, but leaves a blockage resulting in congestion.

An illness might exist in a bodily tissue, independent of the cells comprising the tissue.  A tissue is a layer of life above individual cells.  A tissue might have an illness because that is not a cause of cellular illnesses that leads to tissue injury, which heals and leaves a tissue blockage, resulting in congestion in the tissue.  In the same manner, a limb, or an organ, or an organ system might have a simple or compound illness.

An illness can be based in an organ, an organ system, or in the body.  This is the common view of much of today’s medical practice. It is sometimes a useful view, sometimes not so useful. The illness of the body, like that of a cell, or that of a tissue might begin with a cause, or as an injury or a blockage, caused by an internal or external factor.

An illness might also arise in the mind, or the spirit, or even the community aspects of a life entity, from internal or external causes. An illness might result in damage to the mind, or to the spirit, or to the community aspects of the patient, which when healing is not perfect, results in a negative attribute – leading to congestion, and possibly even a new illness.

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