WHAT IS A PAIN MANAGEMENT DOCTOR?

 

Question: What is Pain Management?

 

Pain management is a branch of medicine that applies science to the reduction of pain. It covers a wide spectrum of conditions including neuropathic pain, sciatica, postoperative pain and more.

 

Answer: Pain management is a rapidly growing medical specialty that takes a multi-disciplinary approach to treating all kinds of pain. Dr. Sameh Yonan, a pain management specialist at the Cleveland Clinic, says "we evaluate, rehabilitate and treat people in pain." Your doctor may refer you to pain management if she or he determines that your pain has become out of control.

Pain Management Specialists: What They Do, How to Find One

Doctors who specialize in pain management recognize the complex nature of pain, and a pain doctor "approaches the problem from all directions," Yonan said. Ideally, treatment at a pain clinic is patient-centric, but in reality this may depend on the available resources of the institution. Currently, there are no established standards for the types of disciplines that must be included, and this is another reason why treatment offerings will vary from clinic to clinic.

But at the very least, experts say that a facility should offer to patients three types of physicians: a coordinating physician, who provides consultation to specialists on your behalf, a physical rehabilitation specialist, and a psychiatrist, to help you deal with any accompanying depression or anxiety, especially if you have chronic pain.

Other medical specialties represented in pain management are anesthesiology, neurosurgery and internal medicine. Your coordinating physician may also refer you for services from occupational medicine specialists, social workers and/or alternative and complementary medicine practitioners.

To qualify as a pain management specialist in the eyes of the American Board of Medical Specialties, a health care provider should be an MD with board certification in at least one of the following specialties:

·         Anesthesiology

·         Physical rehabilitation

·         Psychiatry and neurology.

Dr. James Dillard, an assistant professor of medicine at Columbia University College of Physicians and Surgeons, says that the pain management physician should also have her or his practice limited to that specialty in which they hold the certification. You can check to see if the doctors at the pain management clinic you are considering are board certified by going to the American Board of Medical Specialties web site.

Goals of Pain Management

While some types of pain come from primary sources such as headaches, and others from secondary sources such as from surgery, the field of pain management treats all of it as a disease. This allows for the application of science, and the latest advances in medicine to relieve your pain. And while many patients, especially those in chronic pain, see a psychiatrist or therapist as part of the experience, learning to cope with pain is less and less the focus of treatment.

"We now have many modalities, including medication, interventional pain management techniques (nerve blocks, spinal cord stimulators and similar treatments), along with physical therapy and alternative medicine to help reduce the pain," says Yonan.

The goal of pain management is to minimize pain, rather than eliminate it. This is because quite often it is not possible to completely do away with it. Two other goals are to improve function and increase quality of life. These three goals go hand-in-hand.

As a first-time patient in a pain management clinic, you might experience the following:

·         Evaluation.

·         Diagnostic tests, if necessary, as determined in the evaluation.

·         Referral to surgeon, if indicated by the tests and evaluation.

·         Interventional treatment, such as injections or spinal cord stimulation.

·         Physical therapy to increase range-of-motion and strength, and to prepare you to go back to work.

·         Psychiatry to deal with depression, anxiety and/or other issues that may accompany your chronic pain.

·         Alternative medicine to provide a complement to your other treatments.

Back and neck pain sufferers who do best with a pain management program, says Yonan, are those who have had multiple back surgeries, including failed surgeries, and are still in pain, those with neuropathy, and those for whom it has been determined that surgery would not benefit their condition.

"People who have become addicted to pain medication actually need more sophisticated help than what a pain management program can offer them. A chronic pain rehab program is a better choice for these people," he says.

According to Pain Physician, results from research studies on pain management are not always applicable to the problems patients come in with to the clinics on a day-to-day basis. Unfortunately, this has a negative effect on insurance reimbursement and other payment arrangements, as well as standardization of this medical specialty.

"Better understanding of pain syndromes by communities and insurance companies and more studies on pain will help increase insurance coverage for pain management treatments. In the future, the use of technology will help improve the outcomes of interventional pain management techniques," Yonan says.

_{Sources:
Manchikanti, L. MD, Mark V. Boswell, M. MD, PhD., James Giordano, J. PhD Evidenced Based Interventional Pain Management: Principles, Problems, Potential and Applications Pain Physician 2007; 10:329-356
Personal Interview. Dr. Sameh Yonan, MD, Pain Management Specialist at Hillcrest, Willoughby and South Pointe Pain Centers at Cleveland Clinic Health System
James N. Dillard, MD., DC. CAc. The Chronic Pain Solution: Your Personal Path to Pain Relief Bantam Dell a division of Random House New York 2003}

 

POSTED BY ATTORNEY RENE G. GARCIA:

For more information:- Some of our clients have suffered injuries that require a Pain Management Doctor due to a serious accident. The Garcia Law Firm, P.C. was able to successfully handle these types of cases. For a free consultation please call us at 1-866- SCAFFOLD or 212-725-1313.

http://backandneck.about.com/od/chronicpainconditions/f/painmanagement.htm

OVERVIEW OF HAND SURGERY

What is hand surgery?

Hand surgery is a broad term that incorporates a vast array of different types of surgery on the hand. Plastic surgeons who perform hand surgery attempt to restore not only the function of the hand, but try to maximize the cosmetic appearance of the hand, as well. Surgery on the hand may be done for many reasons, including, but not limited to, the following:

• Trauma to the hand
• Rheumatic changes to the structures in the hand
• Congenital (present at birth) deformities
• Infections

What are the different types of hand surgery?

Many different types of surgeries can be performed on the hand, depending on the underlying cause of the problem. The following is a brief overview of some of the types of surgery that may be performed:

• Skin grafts. Skin grafts involve replacing or attaching skin to a part of the hand that has missing skin. The most common type of injury requiring a skin graft is fingertip amputations or injuries. Skin grafts are performed by taking a piece of healthy skin from another area of the body (called the donor site) and attaching it to the needed area.
• Skin flaps. A skin flap is similar to a skin graft, in which a part of the skin is taken from another area. However, with a skin flap, the skin that is retrieved has its own blood supply. The section of skin used includes the underlying blood vessels, fat, and muscles. Flaps may be used when an area that is missing the skin does not have a good supply of blood because of the location, damage to the vessels, or extensive damage to the tissue.
• Closed reduction and fixation. This technique may be used when there is a fracture in part of the hand, including the fingers. This type of surgery attempts to realign the fractured bone and then immobilize the area during the healing phase. Immobilization can be done with internal fixtures, such as with wires, rods, splints, and casts.
• Tendon repair. Tendons are the fibers that attach muscle to bone. Repair of tendons remains a surgical challenge because of the structure of the tendon. Tendon injuries can occur due to infection, trauma, or spontaneous rupture. Repair of a tendon may be classified as primary, delayed primary, or secondary. Primary repair of an acute injury is usually completed within 24 hours of the injury. Delayed primary repair is usually performed a few days after the injury, but while there is still an opening in the skin from the wound. Secondary repairs may occur two to five weeks or longer after the injury. Primary repairs usually involve direct surgical correction of the injury, while secondary repairs may include tendon grafts (inserting tendons from other areas of the body in place of the damaged tendon) or other more complex procedures.
• Nerve repairs. There are three main nerves that innervate the hand, including the ulnar nerve, the median nerve, and the radial nerve. Damage to these nerves from injury may result in decreased ability to move the hand and experience feeling. Some nerve injuries may heal on their own, while others require surgery. Overall, about three to six weeks after the injury is the best time for nerve repairs that are associated with other, more complicated, injuries. Surgery to investigate a damaged nerve that is not complicated by other injuries is usually performed early after the trauma, to increase the likelihood of a full recovery. If severed, the nerve may be repaired by reattaching it directly to the other end of the nerve, or by using a nerve graft (inserting nerves from other areas of the body in place of the damaged nerve) to repair the damaged section.
• Fasciotomy. This procedure is performed to help treat compartment syndromes. A compartment is a three-dimensional anatomic space in the body that is surrounded by fascia or bone and contains arteries, nerves, and veins. A compartment syndrome is a condition that arises when there is an increase in intracompartmental tissue pressure within a space in the body, usually caused by trauma, which can interfere with the circulation to the body tissues and destroy function. In the hand, a compartment syndrome may lead to severe and increasing pain, muscle weakness, and, eventually, a change in color of the fingers or nailbeds.
  Fasciotomy is the treatment for the early stage of compartment syndromes. Surgical incisions are placed in the hand or arm to allow a release of the pressures that are increasing inside the body. Any tissue inside the body that is already damaged may be removed at this time. A fasciotomy will help prevent a further decrease in function and damage of the affected extremity.
• Surgical drainage and/or debridement. Our hands are constantly at risk for injury and infection. Infections of the hand are a common reason people seek treatment. The treatment for infections to the hand may include rest, use of heat, elevation, antibiotics, and surgery. Surgical drainage may be used if there is an abscess in the hand to help remove the collection of pus. Debridement, or cleansing of a wound to prevent further infection and to help promote healing, may be used if the infection or wound is severe.
• Joint replacement. This type of surgery, also called arthroplasty, may be used in people with severe arthritis of the hand. This involves replacing a joint that has been destroyed by the disease process with an artificial joint. This artificial joint may be made out of metal, plastic, silicone rubber, or the patient's own body tissue (such as a tendon).
• Replantation. This type of surgery replaces fingers or hands that have inadvertently been amputated, usually by some type of trauma. Replantation uses microsurgery, which is an intricate and precise surgery that is performed under magnification. Some severe injuries may require more than one surgery for optimal recovery.

What are the risks of hand surgery?

Most surgery carries the risks of anesthesia and bleeding. Additional risks associated with surgery depend greatly on the type of surgery being performed and may include, but are not limited to, the following:

• Infection
• Incomplete healing
• Loss of feeling or movement of the hand or fingers
• Blood clots may form

 

POSTED BY ATTORNEY RENE G. GARCIA:

 

For more information:- Some of our clients have suffered this kind of injuries due to a serious accident. The Garcia Law Firm, P.C. was able to successfully handle these types of cases. For a free consultation please call us at 1-866- SCAFFOLD or 212-725-1313.

http://www.hopkinsmedicine.org/healthlibrary/conditions/plastic_surgery/overview_of_hand_surgery_85,P01130/

 

OCCUPATIONAL ASTHMA

A. Introduction
Occupational Asthma (OA) is a form of asthmaassociated with work or a hobby involving inhalation of a chemical, allergen, or irritant which is aerosolized as dust or fumes. Occupational asthma symptoms have been observed among workers (e.g., bakers, grain workers), even dating back to ancient times. OA may only affect a small percentage of the population; however, it is a serious problem which can lead to permanent lung damage.

Occupational asthma affects the bronchial tree, resulting in symptoms that mimic those of bronchial asthma (e.g., coughing, wheezing, dyspnea, and chest congestion) and is associated with airway obstruction and/or airway hyper-responsiveness. These symptoms may also be accompanied by typical allergy symptoms such as itchy eyes, itchy nose and sneezing when OA is IgE-mediated.

There are many types of OA, and it is now understood that there is more than one possible mechanism involved in its development.

Unlike most cases of bronchial asthma (which usually respond to treatment and may be reversible), OA with long-term exposure to workplace allergens and irritants can lead to a chronic, irreversible form of asthma that is unresponsive to medication, even when the patient is no longer exposed to the original offending agent.

The common form of allergic bronchial asthma is often provoked by common aeroallergens found at home and outdoors during the pollen season. In contrast, OA is associated with the inhalation of specific and potent airborne agents unique to the workplace.

Symptoms of OA can include:

• coughing
• wheezing
• itchy eyes
• chest tightness
• shortness of breath
• itchy nose
• sneezing
• congestion

In addition to a new onset of asthma symptoms at work in a previous non-asthmatic individual, some patients with pre-existing asthma may notice that their symptoms are triggered or worsened while at work. This may be due to exposure to non-specific airborne irritants or inhaled allergens to which the patient is already sensitive.

In addition, asthmatic patients may also develop new sensitivities or lung damage due to inhaled environmental agents unique to the workplace.

The following section details the known mechanisms at work in the development of OA.

B. Causes of OA

There are at least two major mechanisms involved in the development of OA:

1. The most common type of OA occurs after prolonged exposure to workplace allergens. During this time, the patient becomes sensitized to the inhaled workplace agent. The initial period in which the patient is symptom-free is called the latency phase, which can sometimes last years. During this period, the patient has no asthma symptoms as the immunologic hypersensitivity to the workplace allergen is developing. The mechanism is mostly IgE-mediated, and the patient may also develop typical allergy-like symptoms that include itchy eyes, itchy nose and sneezing prior to or during the presentation of asthma symptoms. Early in the course of OA, asthma symptoms usually lessen or resolve when the patient is not at work, especially during evenings, weekends, and vacations.

Immunologic sensitization to a workplace agent in this form of OA is mostly due either to high molecular weight (HMW) agents (e.g., flour, animal protein), or less often, to low molecular weight (LMW) agents (e.g., chemicals such as isocyanates). The mechanism for HMW sensitization is usually IgE-mediated, while the mechanism for LMW sensitization is often a result of T-cell mediation (cellular hypersensitivity).

2. The less common type of OA results from exposure to high levels of airborne irritants in the workplace. Symptoms begin soon after entering the new work environment, with little to no latency period. Since there is no underlying immunologic mechanism or sensitization (latency) period, symptoms result from direct irritation or damage to the airway. This presentation is often referred to as reactive airway dysfunction syndrome (RADS), or irritant-induced asthma (IrIA), which is mentioned in the next section.

C. Mechanisms of OA
Immunologic: IgE-mediated sensitization

HMW agents (e.g., animal proteins) have the size and molecular weight to act as complete allergens; therefore, they can elicit a specific IgE response to a workplace allergen (for example, baker’s asthma is a specific IgE response to airborne flour). In this example, sensitization is not immediate, but it follows a latency period that can last years. Although IgE sensitization is usually the result of HMW allergen exposure, a few LMW agents, classified as haptens or incomplete allergens (e.g., platinum salts), can also cause a similar reaction. LMW haptens can act as sensitizers when they combine with body proteins to form complete allergens. Such allergens then behave as HMW allergens, thus eliciting the production of specific IgE against the offending workplace allergen.

Immunologic: Non-IgE mediated sensitization

LMW chemicals (e.g., isocyanates, plicatic acid/western cedar) that induce OA are not usually associated with specific IgE production. Although IgE and IgG antibodies have been detected against some LMW agents, a cellular immunologic reaction involving T-cell activation appears to be more commonly associated with LMW sensitization to workplace agents.

Non-immunologic

Irritant-induced asthma (IrIA) or reactive airway dysfunction syndrome (RADS) can occur after a single dose or multiple exposures to high concentrations of non-specific irritants (e.g., acids). While the exact mechanism is unknown, epithelial damage to the bronchi is common early in the disease process, leading to airway narrowing and typical symptoms of asthma. In other words, a previously non-asthmatic individual can develop OA following a single exposure to a strong irritant or chemical. An example of this would be the first responders present at the collapse of the World Trade Center on 9/11. This often occurs following an intense irritant or chemical exposure, as with a chemical spill.

Combined immunologic and non-immunologic

Some agents (e.g., toluene diisocyanate/TDI) can cause OA through both immunologic and non-immunologic mechanisms, causing epithelial damage in addition to sensitization.

D. The OA history
The possibility of OA should always be considered with a new onset of asthma symptoms or a recent worsening of asthma symptoms or recent worsening of asthma. Beyond current employment and hobbies, the physician should consider the patient’s past work history and exposure experiences to assess prior risk of OA.

Diagnostic clues

• Type of symptoms (wheezing, etc. prominent in the workplace)
• Relationship of symptoms to workplace
• Risk factors at workplace due to known sensitizers
• Past medical and occupational history
• History of lung disease
• Chemicals, processes, and exposure incidence, as well as potential agent exposure risks within the profession or industry
• Location of patient within the work environment

Material safety data (MSD) sheets obtained from the patient’s employer can help identify the offending agent. However, the MSD is not required by law in work environments where the offending chemical is present in concentrations of less than 1%. Therefore, information on a suspected agent must be obtained directly from its manufacturer.

Identifying high-risk agents in the work environment may require detective work by the patient with the guidance of an allergist or other specialist. He/she will need to gather information regarding the duration and frequency of agent exposure, concentration of exposure, preventive measures used in the workplace (e.g., masks, ventilation methods, air cleaners, etc.), and location of the worker in relation to agent exposure. These bits of information may offer clues in detecting the presence of OA.

In the development of OA, the occurrence of symptoms of allergic rhinitis and conjunctivitis in the workplace often precede chest symptoms, especially when HMW agents are involved (e.g., animal protein, grains). Workers with OA frequently notice that chest symptoms begin early in their shift, progress in severity during the shift, and later extend into the hours after the shift has ended. Improvement in asthma symptoms when not at work is suggestive of OA, but not conclusive.

In the early stages of OA, symptoms usually resolve during weekends and holidays. However, with continued exposure to the offending agent, the disease process and symptoms become chronic, often persisting outside of the workplace.

For many patients with longstanding OA, symptoms may not resolve even when the patient discontinues work completely and is no longer exposed to the allergen. Therefore, early detection of OA and removal of the individual from the workplace before permanent changes occur may prevent chronic lung symptoms. It has been reported that early intervention may result in resolution of asthma symptoms in one third or more of OA patients.

Agent exposure history may not always be obvious. For example, a bookkeeper in an office connected to a warehouse or factory may be exposed to high levels of an allergen or irritant via a common ventilation system. Therefore, such a clerical worker may develop OA symptoms without awareness of his or her exposure to a high-risk agent.

In contrast, awareness of high-risk occupational exposure to agents with the potential to cause OA (see Tables 1 and 2) will help the physician reach an early diagnosis in the development of OA symptoms. This is no simple matter since there are more than 400 known sensitizers or irritants which can cause asthma in the workplace. One compilation of these triggers can be found at the following web address: www.remcomp.fr/asmanet/asmapro/agents.htm#start.

About 10% of adult workers with a prior diagnosis of asthma will experience a worsening of their asthma symptoms in the workplace. Such asthma symptoms may be due to either non-specific air pollution irritating a hyperreactive airway or result from allergic sensitivity to the presence of a specific airborne allergen or agent.

E. Typical onset of OA
For those exposed to HMW allergens, allergy symptoms such as conjunctivitis and rhinitis often precede or accompany the development of coughing, wheezing or dyspnea in cases of OA. The diagnosis may be complicated when exposure to a workplace allergen is intermittent or the patient has a history of asthma and airway hyperreactivity prior to beginning employment. In this latter instance, workplace exposure to non-specific pollution can trigger underlying asthma. On the other hand, the patient can have symptoms resulting from a workplace inhaled allergen, either as a result of a newly acquired sensitization or from prior sensitization.

The latency period for sensitization to a workplace allergen varies with the type of allergen inhaled. For example, the latency period is generally shorter with exposure to LMW substances (e.g., isocyanates) and longer with HMW substances (e.g., flour, animal protein). As discussed earlier, the latency period may persist for years with HMW sensitization.

F. Diagnosis of OA

Occupational asthma diagnosis is based on: 1) History of asthma-related symptoms in the workplace

2) Pulmonary function tests

A pulmonary function test performed during or after work that demonstrates an obstructive pattern with or without significant reversibility supports the diagnosis of OA.

If spirometric pulmonary functions do not clearly support the diagnosis of OA, then a methacholine challenge may be necessary. A positive methacholine challenge will demonstrate the presence of airway hyperreactivity supporting the diagnosis of OA. In contrast, a negative methacholine challenge rules out the diagnosis of OA. These objective clinical studies may aid in creating solid documentation supporting the diagnosis of OA and the need for modification of the workplace environment with regard to agent exposure. These studies may also be necessary for disability claims.



An agent-specific bronchoprovocation challenge with a suspected workplace agent is usually not necessary and should only be carried out in specialized laboratories with experienced personnel. Such centers may be found at Johns Hopkins University Hospital in Maryland, The National Institutes of Health in Maryland, and National Jewish Health Center in Denver, Colorado, and the College of Medicine at the University of Cincinnati, among others.

Inhalational challenges to specific agents should be performed in a laboratory equipped to deliver precisely measured doses of the suspected agent in order to create a dose response curve. The challenge begins with a very tiny dose in order to avoid producing an irritant reaction or a serious flare of asthma symptoms. Specialized equipment—including a dosimeter (which precisely measures the dose of allergen to be inhaled) and an occupational challenge chamber—are used to quantify individual doses and provide a safe challenge area for both the patient and the testing personnel. Bronchoprovocation tests with allergens or workplace chemicals can result in significant broncho-pulmonary reactions leading to hospitalization and serious complications. Since most presentations of OA can be diagnosed accurately by combining history, serial pulmonary functions, allergy tests and/or evidence of sputum eosinophilia, the risks and additional benefits of bronchial provocation testing need to be carefully weighed. Finally, allergy skin testing can also be particularly valuable in detecting sensitivity to a HMW allergen in the workplace.

G. Objective studies

• Peak flow expiratory rate—Serial measurements of peak flow rates can be performed on a regular basis before, during and after work, 4-6x per day over a few weeks. This should be done similarly for a period when not at work. In OA, peak flows will trend downward during the workday, often improving by the following morning, on weekends, and on vacation. This is not a specific test identifying the cause, but it may help support the diagnosis by demonstrating airway obstruction related to workplace exposure. However, a malingering patient can manipulate these studies.

• Spirometry—Recording the FEV on workdays and non-workdays is a standard objective study that can confirm the presence of asthma in the workplace. This test will not identify the specific agent, but it can support that asthma symptoms are occurring in the workplace. Although the FEV is the most commonly used spirometric measurement, the FEF25-75 is actually a more sensitive measurement and less susceptible to patient manipulation. Another important advantage of measurement by spirometry versus peak flow measurement is that it is difficult, if not impossible, for the patient to manipulate the results without a skilled physician detecting such an attempt.

• Testing for airway hyperreactivity—Another objective method for identifying changes in the airway induced by workplace exposure to an allergen or chemical is demonstrating the presence or increase in bronchial hyperresponsiveness with a methacholine challenge. This study can be performed at the end of the work period and at the end of a period away from work. A decrease by 50% or more in the amount of methacholine required to induce a 20% drop in FEV following work would support the diagnosis of OA by revealing an increase in airway hyperreactivity.

In contrast, a lack of bronchial hyper-responsiveness when the subject is at work with asthma-like symptoms virtually excludes the diagnosis of OA. However, a negative methacholine challenge when the patient is not at work and asymptomatic does not rule out OA.

• Allergy skin testing—Allergy skin test antigens are not available for documenting hypersensitivity to many occupational agents, since many are of low molecular weight and therefore unsuitable for skin testing. Allergy extracts suitable for skin testing can be developed for some HMW antigens, such as animal dander, insect parts, and plant proteins. While a positive skin test would support the presence of IgE-mediated sensitization, in order to confirm an OA diagnosis, there must also be a concomitant history of asthma symptoms and pulmonary functions demonstrating obstruction and airway hypersensitivity. However, a negative allergy skin test with suspected HMW allergens (egg, flour or enzymes) probably rules out that those specific antigens are a cause of OA symptoms.

• Specific agent bronchoprovocation challenge—Patients who have asthma symptoms in the workplace along with normal pulmonary functions in the workplace, negative methacholine challenges, and eosinophil-free sputum are unlikely to have occupational asthma as a cause of their symptoms. However, one can finalize a questionable diagnosis with a specific agent bronchoprovocation challenge. A negative challenge clearly rules out the presence of OA under these circumstances.

When the diagnosis of OA is suspected and yet not clearly defined, specific bronchoprovocation inhalation testing may be required to objectively finalize the diagnosis. The use of HMW agents in a bronchial challenge can be carried out in a single day because the reaction is immediate (IgE mediated). In contrast, LMW agents can induce a non-immediate or late response and daily challenges of increasing doses on subsequent days is often required to elicit a response.



In addition to spirometry, demonstration of bronchial hyperresponsiveness at the end of each day of the challenge and/or demonstration of eosinophils in sputum, or an increase in exhaled nitric oxide following the challenge adds support for the diagnosis of OA caused by the specific agent used in the challenge.

In asymptomatic workers, a positive methacholine challenge or presence of eosinophils in sputum after antigen exposure may predict the onset of occupational asthma and allow for an early and sensitive marker for the potential development of occupational asthma.

• Chest x-ray—Will either be normal or reveal signs of asthma such as air trapping in patients with OA. The x-ray or CT scan of the chest in OA will not reveal signs of fibrosis, while the presence of fibrosis is more typical of hypersensitivity pneumonitis and other chronic occupational lung diseases associated with interstitial pulmonary damage.

• Laboratory studies—In allergy-induced occupational asthma, the eosinophil count can be elevated in the blood and/or sputum. A RAST assay/Immunocap may be positive for one sensitized to a HMW allergen.

H. Common workplace allergens

Examples of HMW agents causing OA:

• Animal protein (animal lab researchers, veterinarians)

•Flour and grains - Cereals (e.g., wheat flour, soya dust used in baking), enzymes (amylase, cellulose), yeast, and storage mites.

• Latex (healthcare workers, lab workers)

Airborne latex allergens are often associated with the use of latex gloves. Sensitization to any of several different latex allergens may be involved. Aerosolization of latex often results from latex adhering to glove powder. Frequent changes of gloves will increase aerosolization and exposure to latex.

Examples of LMW agents causing OA:

• Diisocyanates (automobile painters, plastics manufacturers)

Among the diisocyanates, toluenediisocyanate (TDI) is the most commercially used of these sensitizers. It is often used in the manufacture of automobiles, foam rubber, and molds for insulation. Hexamethylene diisocyanate (HDI) is used in spray paints. This agent can cause OA, RADS, and even hypersensitivity pneumonitis. These chemicals are strong sensitizers and can cause OA in up to 10% of exposed workers.

• Wood dust (loggers, sawmill workers, carpenters)

Exposure to wood dust can cause OA as well as hypersensitivity pneumonitis. A common cause of OA in the Pacific northwestern United States is exposure to western red cedar dust, due to its content of plicatic acid. Plicatic acid as a hapten (LMW agent) can conjugate with body proteins to induce the production of specific IgE which is found in only 20% of exposed patients who developed OA. It appears that cellular hypersensitivity plays a more prominent role in sensitization than does IgE. Sensitization to western red cedar workers occurs in 5 -10% of this population of workers.

Occupational asthma must be differentiated from other occupational lung diseaseswhich can also be immunologically mediated, but by a different mechanism than that seen in OA. Further, unlike OA in which the bronchi are primarily affected, other occupational lung diseases usually involve the parenchyma of the lung.

I. Three different types of occupational lung disease

Occupational lung disease includes:

- Occupational asthma

- Hypersensitivity pneumonitis

- Pneumoconiosis

Each of these three occupational lung diseases differs either in the site of lung damage or the nature of reaction causing the damage. Yet, they share a common element in that they all result from inhaling allergens, chemicals, or mineral dust in the workplace.

Occupational asthma is a disease of the bronchial tree resulting in an obstructive pattern on pulmonary function tests. OA is usually associated with symptoms of wheezing, coughing and shortness of breath. Early in the development of OA, symptoms may respond to bronchodilators and the pulmonary function test may reveal partial or total reversibility. In contrast, the two other occupational lung diseases involve damage to the parenchyma of the lung (interstitial tissue) resulting in shortness of breath without wheezing and eventually develop a restrictive pattern on pulmonary function tests.

　

Table 3:
Causes of hypersensitivity related to specific occupations

J. Treatment

The management of OA consists of limiting the worker’s exposure to the offending agent to amounts that will not induce disease. A number of approaches can be taken. For example, the worker can be moved to another location within the workplace where little or no offending agent is present. Other techniques include using effective equipment to remove dust and vapor exposure and improving workplace ventilation so that frequent air exchange limits agent accumulation. Evaluation of the workplace should be conducted by a trained industrial hygienist who can measure the degree of agent exposure. It is important to remember that levels of exposure below the legal limits are based on toxicity studies and, therefore, the presence of even tiny amounts of sensitizing agents may still cause immunologic reactions. Face masks of the filtering type are not especially efficient or well-tolerated. In contrast, a compressor with a HEPA filter creating a positive air flow through a mask or head piece can markedly diminish inhalation of airborne dust and therefore may be helpful when working with HMW agents.
Ideally, the work environment should be designed to limit the concentration of potential sensitizers to safe levels. Since this may be impractical in many manufacturing processes, even in a carefully monitored facility, recommended thresholds may be exceeded. Therefore, total avoidance of the workplace may be the only alternative for some sufferers of OA and may entail retraining and reassigning the employee(s) to another job free of potential exposure to the suspected agent.
Pharmacologic management of OA is rarely helpful in the presence of continued exposure on a chronic basis. Asthma resulting from contact with occupational exposures responds to therapeutic agents such as β-adrenergic agonists, cromolyn sodium, and steroids. As exposure continues, sensitivity may increase, rendering medication less effective.
Immunotherapy has been used with various occupational allergens causing asthma, including treatment of laboratory animal workers, bakers, and oyster gatherers, with reported success.

K. Prevention

The most important principle of OA management is prevention, rather than treatment. Educating exposed workers and managers in high-risk industries is crucial so that affected workers can be recognized early. Right-to-know legislation should increase awareness of occupational asthma.
At this time, there are no pre-employment screening criteria that have been shown to be accurate in predicting the eventual appearance of OA. There is conflicting evidence as to whether HLA studies are useful in predicting isocyanate asthma or anhydride asthma. It has been reported that atopy is a predisposing factor for a worker to develop IgE-mediated disease. Further, as many as 25-50% of the work force may have allergy, but it is impractical to avoid hiring such a large portion of the potential work force when only a small number of these individuals may develop OA.

L. Prognosis

Many workers with occupational asthma do not completely recover, even though they have been removed from exposure to a sensitizing agent for years. An unfavorable prognosis has been reported to be associated with a persistent, high level of specific IgE to the suspected agent, long duration of symptoms (>1 to 2 years), abnormal pulmonary function test results, and a high degree of airway hyperreactivity. The obvious conclusion based on these observations is that early diagnosis and removal from exposure are requisites for the goal of complete recovery. In workers who remain exposed to offending agents after being diagnosed with OA, further deterioration of lung function and increased airway hyperreactivity are likely. It should be understood that life-threatening attacks and even deaths have been reported with continued exposure after diagnosis of OA.

POSTED BY ATTORNEY RENE G. GARCIA:

For more information:- Some of our clients have suffered this kind of injuries due to a serious accident. The Garcia Law Firm, P.C. was able to successfully handle these types of cases. For a free consultation please call us at 1-866- SCAFFOLD or 212-725-1313.

http://www.asthmacenter.com/index.php/News/details/occupational_asthma/