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GBS (Guillain-Barre syndrom)


Guillain-Barré syndrome (GBS) is a disorder in which the body's immune system attacks part of the peripheral nervous system. The first symptoms of this disorder include varying degrees of weakness or tingling sensations in the legs. In many instances the symmetrical weakness and abnormal sensations spread to the arms and upper body. These symptoms can increase in intensity until certain muscles cannot be used at all and, when severe, the person is almost totally paralyzed. In these cases the disorder is life threatening - potentially interfering with breathing and, at times, with blood pressure or heart rate - and is considered a medical emergency. Such an individual is often put on a ventilator to assist with breathing and is watched closely for problems such as an abnormal heart beat, infections, blood clots, and high or low blood pressure. Most individuals, however, recover from even the most severe cases of Guillain-Barré syndrome, although some continue to have a certain degree of weakness.
Guillain-Barré syndrome can affect anybody. It can strike at any age and both sexes are equally prone to the disorder. The syndrome is rare, however, afflicting only about one person in 100,000. Usually Guillain-Barré occurs a few days or weeks after the patient has had symptoms of a respiratory or gastrointestinal viral infection. Occasionally surgery will trigger the syndrome. In rare instances vaccinations may increase the risk of GBS.
After the first clinical manifestations of the disease, the symptoms can progress over the course of hours, days, or weeks. Most people reach the stage of greatest weakness within the first 2 weeks after symptoms appear, and by the third week of the illness 90 percent of all patients are at their weakest.

What causes Guillain-Barré syndrome?


No one yet knows why Guillain-Barré — which is not contagious — strikes some people and not others. Nor does anyone know exactly what sets the disease in motion.
What scientists do know is that the body's immune system begins to attack the body itself, causing what is known as an autoimmune disease. Usually the cells of the immune system attack only foreign material and invading organisms. In Guillain-Barré syndrome, however, the immune system starts to destroy the myelin sheath that surrounds the axons of many peripheral nerves, or even the axons themselves (axons are long, thin extensions of the nerve cells; they carry nerve signals). The myelin sheath surrounding the axon speeds up the transmission of nerve signals and allows the transmission of signals over long distances.
In diseases in which the peripheral nerves' myelin sheaths are injured or degraded, the nerves cannot transmit signals efficiently. That is why the muscles begin to lose their ability to respond to the brain's commands, commands that must be carried through the nerve network. The brain also receives fewer sensory signals from the rest of the body, resulting in an inability to feel textures, heat, pain, and other sensations. Alternately, the brain may receive inappropriate signals that result in tingling, "crawling-skin," or painful sensations. Because the signals to and from the arms and legs must travel the longest distances they are most vulnerable to interruption. Therefore, muscle weakness and tingling sensations usually first appear in the hands and feet and progress upwards.
 
When Guillain-Barré is preceded by a viral or bacterial infection, it is possible that the virus has changed the nature of cells in the nervous system so that the immune system treats them as foreign cells. It is also possible that the virus makes the immune system itself less discriminating about what cells it recognizes as its own, allowing some of the immune cells, such as certain kinds of lymphocytes and macrophages, to attack the myelin. Sensitized T lymphocytes cooperate with B lymphocytes to produce antibodies against components of the myelin sheath and may contribute to destruction of the myelin. In two forms of GBS, axons are attacked by antibodies against the bacteria Campylobacter jejuni, which react with proteins of the peripheral nerves.  Acute motor axonal neuropathy is particularly common in Chinese children.  Scientists are investigating these and other possibilities to find why the immune system goes awry in Guillain-Barré syndrome and other autoimmune diseases. The cause and course of Guillain-Barré syndrome is an active area of neurological investigation, incorporating the cooperative efforts of neurological scientists, immunologists, and virologists.

How is Guillain-Barré syndrome diagnosed?

 


Guillain-Barré is called a syndrome rather than a disease because it is not clear that a specific disease-causing agent is involved. A syndrome is a medical condition characterized by a collection of symptoms (what the patient feels) and signs (what a doctor can observe or measure). The signs and symptoms of the syndrome can be quite varied, so doctors may, on rare occasions, find it difficult to diagnose Guillain-Barré in its earliest stages.
Several disorders have symptoms similar to those found in Guillain-Barré, so doctors examine and question patients carefully before making a diagnosis. Collectively, the signs and symptoms form a certain pattern that helps doctors differentiate Guillain-Barré from other disorders. For example, physicians will note whether the symptoms appear on both sides of the body (most common in Guillain-Barré) and the quickness with which the symptoms appear (in other disorders, muscle weakness may progress over months rather than days or weeks). In Guillain-Barré, reflexes such as knee jerks are usually lost. Because the signals traveling along the nerve are slower, a nerve conduction velocity (NCV) test can give a doctor clues to aid the diagnosis. In Guillain-Barré patients, the cerebrospinal fluid that bathes the spinal cord and brain contains more protein than usual. Therefore a physician may decide to perform a spinal tap, a procedure in which a needle is inserted into the patient's lower back and a small amount of cerebrospinal fluid from the spinal column is withdrawn for study..
 

How is Guillain-Barré treated?


There is no known cure for Guillain-Barré syndrome. However, there are therapies that lessen the severity of the illness and accelerate the recovery in most patients. There are also a number of ways to treat the complications of the disease.
Currently, plasma exchange (also called plasmapheresis) and high-dose immunoglobulin therapy are used. Both of them are equally effective, but immunoglobulin is easier to administer. Plasma exchange is a method by which whole blood is removed from the body and processed so that the red and white blood cells are separated from the plasma, or liquid portion of the blood. The blood cells are then returned to the patient without the plasma, which the body quickly replaces. Scientists still don't know exactly why plasma exchange works, but the technique seems to reduce the severity and duration of the Guillain-Barré episode. This may be because plasmapheresis can remove antibodies and other immune cell-derived factors that could contribute to nerve damage.
In high-dose immunoglobulin therapy, doctors give intravenous injections of the proteins that, in small quantities, the immune system uses naturally to attack invading organisms. Investigators have found that giving high doses of these immunoglobulins, derived from a pool of thousands of normal donors, to Guillain-Barré patients can lessen the immune attack on the nervous system. Investigators don't know why or how this works, although several hypotheses have been proposed.
The use of steroid hormones has also been tried as a way to reduce the severity of Guillain-Barré, but controlled clinical trials have demonstrated that this treatment not only is not effective but may even have a deleterious effect on the disease.
The most critical part of the treatment for this syndrome consists of keeping the patient's body functioning during recovery of the nervous system. This can sometimes require placing the patient on mechanical ventilatory assistance, a heart monitor, or other machines that assist body function. The need for this sophisticated machinery is one reason why Guillain-Barré syndrome patients are usually treated in hospitals, often in an intensive care ward. In the hospital, doctors can also look for and treat the many problems that can afflict any paralyzed patient - complications such as pneumonia or bed sores.
Often, even before recovery begins, caregivers may be instructed to manually move the patient's limbs to help keep the muscles flexible and strong and to prevent venous sludging (the buildup of red blood cells in veins, which could lead to reduced blood flow) in the limbs which could result in deep vein thrombosis.  Later, as the patient begins to recover limb control, physical therapy begins. Carefully planned clinical trials of new and experimental therapies are the key to improving the treatment of patients with Guillain-Barré syndrome. Such clinical trials begin with the research of basic and clinical scientists who, working with clinicians, identify new approaches to treating patients with the disease.

What is the long-term outlook for those with Guillain-Barré syndrome?


Guillain-Barré syndrome can be a devastating disorder because of its sudden and unexpected onset. In addition, recovery is not necessarily quick. As noted above, patients usually reach the point of greatest weakness or paralysis days or weeks after the first symptoms occur. Symptoms then stabilize at this level for a period of days, weeks, or, sometimes, months. The recovery period may be as little as a few weeks or as long as a few years. About 30 percent of those with Guillain-Barré still have a residual weakness after 3 years. About 3 percent may suffer a relapse of muscle weakness and tingling sensations many years after the initial attack.
Guillain-Barré syndrome patients face not only physical difficulties, but emotionally painful periods as well. It is often extremely difficult for patients to adjust to sudden paralysis and dependence on others for help with routine daily activities. Patients sometimes need psychological counseling to help them adapt.
 

What research is being done?


Scientists are concentrating on finding new treatments and refining existing ones. Scientists are also looking at the workings of the immune system to find which cells are responsible for beginning and carrying out the attack on the nervous system. The fact that so many cases of Guillain-Barré begin after a viral or bacterial infection suggests that certain characteristics of some viruses and bacteria may activate the immune system inappropriately. Investigators are searching for those characteristics. Certain proteins or peptides in viruses and bacteria may be the same as those found in myelin, and the generation of antibodies to neutralize the invading viruses or bacteria could trigger the attack on the myelin sheath. As noted previously, neurological scientists, immunologists, virologists, and pharmacologists are all working collaboratively to learn how to prevent this disorder and to make better therapies available when it strikes.


 

Tanda Awal Penyakit Buah Pinggang

RAMAI orang beranggapan mereka cukup sihat, walaupun bertahun-tahun tidak menjalani pemeriksaan kesihatan. Malah, tidak kurang juga beranggapan mereka tidak akan berdepan masalah kesihatan, sedangkan setiap orang sebenarnya mempunyai risiko sama untuk mengalaminya kerana kebanyakan penyakit kronik menyerang badan dalam diam. Sikap suka meletakkan diri dalam keadaan selesa menyebabkan ramai melepaskan peluang menjalani pemeriksaan kesihatan, walaupun ia diberikan secara percuma.
Sikap ini juga menyebabkan ada yang tidak boleh menerima hakikat apabila diberitahu mereka menghidap sesuatu penyakit serius kerana tidak mengalami sebarang gejala.
Namun, itulah sifat penyakit kronik. Kehadirannya tidak dirasai dan pesakit masih boleh menjalankan kegiatan harian tanpa masalah kerana kesan hanya timbul apabila penyakit sampai ke tahap serius.
Fenomena sama turut ditunjukkan dengan masalah kerosakan buah pinggang.Ia mengambil masa bertahun-tahun sebelum menunjukkan kesan kepada kesihatan.Bagaimanapun, anda perlu lebih berhati-hati dan segera mendapatkan pemeriksaan kesihatan jika anda mengalami tanda seperti:
-Ketidakselesaan atau rasa terbakar ketika membuang air kecil.
-Darah keluar bersama-sama air kencing.
-Perubahan pada kekerapan membuang air kecil.
-Sakit belakang.
-Kerap buang air kecil, terutama pada tengah malam.
-Bengkak pada pergelangan kaki.
-Sembap pada keliling mata yang berlarutan, terutama pada sebelah pagi.

 
Semua tanda di atas menunjukkan seseorang itu mengalami masalah kerosakan buah pinggang. Biasanya gejala ini dianggap perkara biasa dan sering diketepikan, sedangkan ia petanda penting kepada masalah buah pinggang.
Risiko kegagalan buah pinggang semakin tinggi dengan pertambahan umur.Setiap tahun dianggarkan 2,400 kes baru kegagalan buah pinggang dilaporkan dan kes baru di kalangan golongan berumur antara 60 hingga 65 tahun menunjukkan peningkatan 25 peratus.
Buah pinggang bertugas menapis darah dan membuang bahan toksik, sisa buangan dan air berlebihan dari badan.Kegagalan buah pinggang melakukan tugas penting ini boleh menyebabkan pesakit menemui maut jika rawatan penggantian buah pinggang tidak dilakukan. Namun, bukan mudah untuk mendapatkan buah pinggang baru dan kosnya pula sangat mahal; boleh mencecah RM300,000!
Justeru, perkara terbaik ialah menjalani pemeriksaan pengesanan. Ujiannya pula sangat mudah iaitu melalui ujian darah dan air kencing yang mengambil masa beberapa minit saja.
Selain dua ujian mudah ini, beberapa kaedah lain boleh digunakan, iaitu biopsi jarum halus dan ujian bagi tekanan darah tinggi dan kencing manis.
Kaedah terbaik untuk mengelak menanggung kos perubatan tinggi ialah kerap membuat pemeriksaan kesihatan untuk mengesan penyakit pada peringkat awal. Ujian saringan kesihatan ini sangat mudah dan keputusannya boleh diketahui segera.
Semua orang perlu menjalani pemeriksaan kesihatan ini, terutama mereka yang mempunyai sejarah atau ahli keluarga menghidap penyakit kencing manis dan tekanan darah tinggi, kerana mereka berisiko tinggi mendapat masalah kegagalan buah pinggang.
Kencing manis dan tekanan darah tinggi yang tidak terkawal juga antara punca utama kerosakan buah pinggang. Jika ini berlaku, bermakna pesakit terpaksa bergantung kepada mesin dialisis darah sepanjang hayat.
Saringan ini sangat mudah. Tiga parameter diukur iaitu tekanan darah, kandungan glukosa darah dan kandungan protein dalam air kencing. Jika air kencing menunjukkan ada protein, pesakit disaran menjalani ujian susulan untuk pengesahan kerana ia antara petanda awal kegagalan buah pinggang.
Masalah kegagalan buah pinggang yang semakin meningkat di kalangan masyarakat kita dipercayai akibat gaya hidup dan tabiat pemakanan tidak sihat yang boleh menjurus kepada penyakit kencing manis serta tekanan darah tinggi.
Kajian terbaru Universiti Sains Malaysia (USM) 2004 mendapati, rakyat Kelantan paling ramai menghidap kencing manis (78,000 orang) dan kebanyakannya adalah pesakit muda berumur 30 tahun.
Peningkatan sekali ganda sebanyak 13 peratus ini sangat merisaukan berbanding hanya 5.3 peratus 10 tahun lalu.
Kencing manis juga menyebabkan 95.3 peratus pesakit di negeri itu terpaksa kehilangan anggota badan yang kesemuanya berpunca daripada pengambilan gula berlebihan.
Jika anda turut mengamalkan gaya hidup tidak sihat, masih belum terlewat untuk mengubahnya.
Mulakan hidup baru dengan menjalani ujian saringan ini sebelum membuat pemeriksaan berkala sekurang-kurangnya setahun sekali.
Kegagalan buah pinggang juga boleh dicegah dengan mengamalkan:
-Pemakanan seimbang.
-Minum sekurang-kurangnya dua liter air sehari.
-Berhenti merokok.
-Makan ubat selepas mendapat nasihat doktor. Paling penting, elakkan ubat yang tidak perlu termasuk ubat untuk menguruskan badan.
-Kekalkan berat badan seimbang.
-Bersenam setiap hari sekurangnya-kurangnya 30 minit.




mecomin or mecobalamin for peripheral neurology(nerve)

 Mecomin is a type of oral preparation used for the treatment of diseases of the nervous system or peripheral neuropathies edge.

Mecomin contain mecobalamin, which is a vitamin B12-Coenzyme existing system highlighted in the blood and cerebrospinal fluid us, it will be actively absorbed by our nervous tissues as compared with normal vitamin B12.

In terms of biochemical angle, speed up metabolic Mecomin nucleic acid, protein, and fat body through particular reaction; with this response, it will improve the nervous tissues affected or injured.

Scientific studies show that mecobalamin is very effective in the treatment of symptoms of numbness, pain, and paralysis that comes from the edge of a nervous system disease. The cause of the edge of a nervous system disease is diabetes and neurological disease itself called polyneuritis (multiple nerve injury).

The recommended dose is 3 tablets a day, 1 capsule 3 times daily, dose may be reduced if the symptoms have subsided. The duration of treatment is usually 2 to 3 months. If the symptoms do not disappear after this period, please consult your doctor for further examination.


 The most common form of vitamin B12 is called cyanocobalamin. However, over the last ten years, a number of central and peripheral neurological (nerve) diseases have been linked to a deficiency of a very specific cobalamin, the methylcobalamin form - that is required to protect against neurological diseases. The liver converts a small amount of cyanocobalamin into methylcobalamin within the body, but larger amounts of methylcobalamin are necessary to correct neurological defects. 

Live-Well Mecomin

Note: Methylcobalamin is most bioavailable form as well as the best utilized form of vitamin B12 in the body. It is the only form of vitamin B12 which does not need to be converted by the liver before the body can use it.



  • Pre-Diabetics
  • Diabetics
  • Those suffering from Pernicious Aneamia
  • Vegetarians


  • Helps regenerate damaged nerves
  • Reduces nerve pain from diabetes

Ubat intravenous immunoglobulin (IVIg) untuk neurology



The clinical use of intravenous immunoglobulin (IVIg) has expanded beyond its traditional place in the treatment of patients with primary immunodeficiencies. Due to its multiple anti-inflammatory and immunomodulatory properties, IVIg is used successfully in a wide range of autoimmune and inflammatory conditions. Recognized autoimmune indications include idiopathic thrombocytopenic purpura (ITP), Kawasaki disease, Guillain–Barré syndrome and other autoimmune neuropathies, myasthenia gravis, dermatomyositis and several rare diseases. Several other indications are currently under investigation and require additional studies to establish firmly the benefit of IVIg treatment. Increasing attention is being turned to the use of IVIg in combination with other agents, such as immunosuppressive agents or monoclonal antibodies. For example, recent studies suggest that combination therapy with IVIg and rituximab (an anti-CD20 monoclonal antibody) may be effective for treatment of autoimmune mucocutaneous blistering diseases (AMBDs), with sustained clinical remission. The combination of IVIg and rituximab has also been used in the setting of organ transplantation. Firstly, IVIg ± rituximab has been administered to highly human leucocyte antigen (HLA)-sensitized patients to reduce anti-HLA antibody levels, thereby allowing transplantation in these patients. Secondly, IVIg in combination with rituximab is effective in the treatment of antibody-mediated rejection following transplantation. Treatment with polyclonal IVIg is a promising adjunctive therapy for severe sepsis and septic shock, but its use remains controversial and further study is needed before it can be recommended routinely. This review covers new developments in these fields and highlights the broad range of potential therapeutic areas in which IVIg may have a clinical impact.
Keywords: autoimmunity, immunoglobulin, vasculitis, sepsis, transplantation

Introduction

Intravenous immunoglobulins (IVIgs) are therapeutic preparations of pooled polyspecific IgG obtained from the plasma of a large number of healthy individuals. These preparations were commercialized in the early 1980s to replace intramuscular preparations of polyspecific IgG, which were the only available substitutive therapy at that time for patients with primary or secondary immunodeficiencies. For patients with primary immunodeficiencies, IVIg (or subcutaneous immunoglobulin – SCIg) remains the treatment option of choice.
In 1981, Imbach and colleagues reported that, in patients with Wiskott–Aldrich syndrome who presented with thrombocytopenia and hypogammaglobulinaemia, high-dose IVIg infusion was followed by an increase in the platelet count [
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Since then, IVIg has been demonstrated to be effective in idiopathic thrombocytopenic purpura (ITP) and a large number of autoimmune and/or systemic inflammatory diseases, notably Kawasaki disease, and in immune-mediated neurological disorders such as Guillain–Barré syndrome (GBS), chronic idiopathic demyelinating polyneuropathy (CIDP), multi-focal neuropathy with conduction block (MNCB) and acute myasthenia gravis [
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For other diseases, IVIg is not always used as a first-line therapy. It may be administered as a steroid-sparing agent and in certain conditions may represent an alternative to other available therapeutic approaches, such as immunosuppressants, plasma exchange or monoclonal antibodies. IVIg is also often employed to treat diseases that are refractory to other treatments or where conventional therapies result in unacceptable side effects. Combination therapy of IVIg with immunosuppressants has been applied successfully in several conditions, including autoimmune vasculitis, dermato- and polymyositis, transplantation and sepsis [
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When considering the emerging uses of IVIg, it is important to consider the evidence base. In some patient populations the therapeutic value of IVIg has been proven in large controlled trials, while in other patient populations only small, uncontrolled studies or case reports are available, often due to the small numbers of patients with these rare diseases.

IVIg for the treatment of autoimmune and inflammatory disorders

Despite the large number of autoimmune diseases being treated with IVIg, guidance on the clinical usage is limited to only three conditions: ITP, GBS and Kawasaki disease. Because of the costs, finite supply and time for the patient receiving IVIg therapy, there is a need to rationalize and prioritize the disorders for which, based on currently available evidence, IVIg is adopted. In France, the Comité d'Evaluation et de Diffusion des Innovations Technologiques (CEDIT) IVIg expert group, chaired by Professor Loïc Guillevin, aims to identify scientifically validated uses and issue recommendations regarding the usage of IVIg [
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 Guidelines for the use of immunoglobulin have also been developed in the United Kingdom [
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 Canada [
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Australia [
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and elsewhere.
Indications have been divided into those patients for whom the benefit of IVIg treatment is recognized, those under evaluation and those where benefit is not documented. Recognized indications include ITP, Kawasaki disease, myasthenia gravis, dermatomyositis (DM), as well as autoimmune neuropathies such as GBS, chronic inflammatory demyelinating polyradiculoneuropathy, multi-focal motor neuropathy (MMN) and stiff person syndrome. IVIg efficacy is also recognized in rare diseases, such as parvovirus B19 infection, autoimmune erythroblastopenia and neutropenia, acquired hypocoagulability and birdshot retinochoroidopathy; however, no prospective randomized studies in these indications exist, due mainly to the rarity of these conditions.
Indications that are currently under evaluation by CEDIT include inclusion body myositis (IBM), demyelinating central nervous system diseases (but not multiple sclerosis or Devic syndrome), corticoresistant polymyositis, autoimmune encephalitis and refractory epilepsy. The efficacy of IVIg in the treatment of select populations of transplant patients, haemolytic anaemia, adult-onset Still's disease, anti-phospholipid syndrome, anti-neutrophil cytoplasmic autoantibodies (ANCA)-associated vasculitides and pemphigus vulgaris is also under evaluation.

IVIg for the treatment of autoimmune vasculitides

Systemic vasculitides are classified based on the diameter of the vessels involved. Large vessel involvement is found in giant cell arteritis and Takayasu's arteritis, while medium vessels are affected in diseases such as polyarteritis nodosa and Kawasaki disease. Small vessels are involved in necrotizing glomerulonephritis and ANCA-associated systemic vasculitides.
Kawasaki disease is characterized by a systemic inflammation of the blood vessels and affects predominantly children under the age of 5 years [
The following popper user interface control may not be accessible. Tab to the next button to revert the control to an accessible version. It is one of the first vasculitides reported to be treated with IVIg, with or without acetyl salicylic acid (aspirin) [
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 Since then, IVIg in combination with aspirin has become the standard of care for patients with Kawasaki disease [
The following popper user interface control may not be accessible. Tab to the next button to revert the control to an accessible version. A meta-analysis of 16 prospective randomized trials was conducted in 2003, showing that there is a significant decrease in new coronary abnormalities at day 30 in patients treated with IVIg compared with placebo and demonstrated that infusion of a single dose of 2 g/kg body weight induces a significant reduction in coronary aneurysms at day 30
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. The analysis concluded that children fulfilling the diagnostic criteria for Kawasaki disease should be treated with 2 g/kg of IVIg within 10 days of the first symptoms in order to gain the maximum benefit [
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Wegener's granulomatosis (WG), microscopic polyangiitis (MPA) and Churg–Strauss syndrome (CSS) are small-sized vessel vasculitides that are associated frequently with anti-neutrophil cytoplasmic autoantibodies [
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ANCA-associated vasculitides are characterized by vascular necrosis either in the glomerular visceral epithelial cells or in other visceral tissues. Renal and lung involvement is often observed. The major target of anti-neutrophil antibodies in WG is proteinase 3, whereas in MPA and CSS the antibodies target myeloperoxidase (MPO). Treatment of ANCA-associated vasculitides is initiated commonly with induction therapy of corticosteroids, cyclophosphamide and sometimes plasma exchanges. Maintenance therapy usually involves azathioprine, methotrexate or mycophenolate mofetil (MMF). Relapses of ANCA-associated vasculitides are often treated with immunosuppressants, such as cyclophosphamide or methotrexate or with biologicals such as IVIg, anti-TNF or anti-CD20 therapy. Plasma exchanges can also be used in this setting.
Several small prospective clinical studies of IVIg treatment of ANCA-associated vasculitides have been conducted The first open prospective study of seven patients with WG, MPA or rheumatoid vasculitis was performed in 1991 and showed promising results, with six patients in complete remission and one with transient response to IVIg therapy (total dose 2 g/kg) [
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This study was followed by an extensive report on 26 patients, showing that 8 weeks after IVIg treatment 13 patients were in full and 13 in partial remission [
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. The clinical benefit was maintained in 18 patients for up to 1 year after IVIg therapy. Conflicting results were obtained in another study of 15 patients with ANCA-associated vasculitis who responded poorly to conventional therapy. These patients were treated with single or multiple courses of IVIg, to a total dose of 30 g/day over 5 days [
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 Six of 15 patients experienced significant clinical benefit; however, no patient experienced complete remission. Another study with patients resistant to conventional treatment similarly showed that IVIg treatment was effective in six of 10 patients [
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Only one randomized, placebo-controlled trial of IVIg in ANCA-associated vasculitis has been conducted to date. The study investigated the efficacy of a single course of IVIg (total dose 2 g/kg) in previously treated patients with persistent disease. At the 3-month time-point (primary end-point), 14 of 17 patients showed improvement in response to IVIg treatment, compared with six of 17 in the placebo group (P = 0·035). However, this was a short trial of only 3 months, so there is still need for additional data in this setting [
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Table 1
Clinical studies of the use of intravenous immunoglobulin (IVIg) for the treatment of anti-neutrophil cytoplasmic autoantibody (ANCA)-associated vasculitis.
A recent open, prospective non-randomized study evaluated the efficacy and safety of IVIg administered for 6 months for the treatment of relapses of WG, MPA or CSS that occurred during or within 1 year following the withdrawal of corticosteroids and/or immunosuppressants [
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. The study evaluated 22 patients (21 with ANCA-specific antibodies). Twenty-one patients experienced partial initial responses and, at 9 months, 13 patients experienced complete remission. At 24 months, eight patients were in complete remission in the absence of any other treatment, while another 10 were in remission with the help of treatment modification.
Although studies in a number of ANCA-associated vasculitides have shown some benefit of IVIg treatment, proven efficacy is observed in only a handful of conditions. For example, the benefits of IVIg in the treatment of Kawasaki disease are well documented, and the data suggest that children meeting the diagnostic criteria for this disease must be treated within 10 days of the onset of symptoms. IVIg may also represent an option in patients with relapsing ANCA-associated vasculitides, but additional randomized controlled trials are needed in this field.

Combination therapy with IVIg in autoimmune mucocutaneous blistering diseases

Autoimmune mucocutaneous blistering diseases (AMBDs) are rare but potentially fatal diseases. Since the introduction of corticosteroids, the annual mortality rate due to blistering diseases has fallen; nonetheless patients suffering from these conditions continue to experience high morbidity and mortality.
There are currently two approaches to the pharmacological management of AMBDs. One approach targets the production of the autoantibody in the bone marrow, spleen and lymph nodes, and involves the use of immunosuppressive drugs such as azathioprine, MMF, cyclophosphamide and methotrexate. The other approach targets the sites at which the autoantibodies exert their effects, namely in the skin or mucosal surfaces. This approach uses anti-inflammatory drugs, such as prednisone and dapsone, to ameliorate the effects of the autoantibodies [
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].
Conventional immunosuppressive therapy for the treatment of AMBDs involves high-dose corticosteroids (80–240 mg/day) for prolonged periods of time. However, this therapy is not always effective and usually results in a poor quality of life. Conventional immunosuppression has a variety of reversible and non-reversible side effects, including prolonged vulnerability to infection and increased risk of cancer. Indeed, the side effects of such therapies are often the ultimate cause of death in these patients.
IVIg is usually employed when conventional therapy fails, causes side effects or is contraindicated. Beneficial clinical effects of IVIg have been demonstrated in the treatment of a number of AMBDs, including pemphigus vulgaris, pemphigus foliaceus, bullous pemphigoid, mucous membrane pemphigoid and epidermolysis bullosa aquisita (EBA). A ‘Consensus Statement’ on the use of IVIg in these diseases recommends a dose of 2 g/kg/cycle, given monthly until clinical control, with a progressive increase of the intervals between the cycles thereafter to 6, 8, 10, 12 and 14 weeks [
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. The last cycle is given after a 16-week interval, and is considered as the end of therapy.
In a recent study, 156 patients with AMBD treated with IVIg using this protocol demonstrated successful clinical outcomes [
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. In these patients IVIg could be used as monotherapy, once concomitant prednisone and immunosuppressive agents were gradually discontinued. These included 42 patients with pemphigus vulgaris, 26 with pemphigus foliaceus, 32 with bullous pemphigoid, 68 with mucous membrane (cicatricial) pemphigoid and nine with epidermolysis bullosa acquisita. IVIg produced long-term, sustained remission for at least 2 years of follow-up, after discontinuing IVIg therapy. The patients were in serological remission and enjoyed a high quality of life. It could be speculated that, compared to previous therapies, IVIg changed the clinical course of these diseases [
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Destroy user interface control21].
As a therapeutic option, the costs associated with IVIg use are often perceived to be high. However, when the true costs of conventional therapy are calculated, including the costs of the treatment of side effects and hospitalizations, they are approximately two- to threefold higher than the costs of IVIg therapy. According to one US analysis, the true cost of conventional therapy for pemphigus vulgaris was $US 123 133 per patient per year, while the mean annual cost of IVIg was $US 76 249 [
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Destroy user interface control22].
A large study analysed 275 patients who had been treated according to the Consensus Statement protocol and who remained in clinical remission for a minimum of 2 years after discontinuing IVIg (unpublished data). About 70% of the patients responded to IVIg monotherapy and were considered high responders. The remaining 30% were partial responders or non-responders. Partial responders, in whom the dose of prednisone and immunosuppressive agent was reduced by 50% or less, were subclassified as mild (clinical response of 50% or less) or moderate (clinical response between 50% and 100%) responders. Moderate responders were treated subsequently with 50–150 mg dapsone daily. Clinical improvement was achieved in less than 4 months (mean 3·8, range 2·1–7·5). Mild responders were treated with oral methotrexate (5–20 mg/weekly) and dapsone (50–150 mg daily). These patients responded to therapy within 6 months (mean 5·7, range 4–8·6). Thereafter, the clinical response of each group of patients was the same as that observed in the high responder group. Non-responders were patients whose disease, in spite of adjunctive therapy, flared if the interval between cycles was increased by more than 4 weeks, or who continued to have active disease after 1 year of IVIg therapy. These patients were treated with rituximab and IVIg, and all showed clinical improvement.
It has been demonstrated previously that the combination of IVIg and rituximab is effective in patients with refractory pemphigus vulgaris who had inadequate responses to conventional therapy and IVIg. Patients were treated with two cycles of rituximab (375 mg/m2 of body-surface area) once weekly for 3 weeks and IVIg (2 g/kg) in the fourth week, followed by a monthly infusion of rituximab and IVIg for 4 months [
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In this study, nine of 11 patients showed rapid resolution of lesions and a clinical remission lasting 22–37 months (mean 31·1 months). All immunosuppressive therapy, including prednisone, could be discontinued. Two patients were treated with rituximab only during recurrences and had sustained remission. None of the patients in this study had serious side effects, although the long-term consequences of rituximab and IVIg combination therapy in such patients with autoimmune diseases are unknown and need to be investigated.

Cara Untuk Kempiskan Perut

 

Ingin mengatasi masalah perut buncit? Berikut adalah beberapa tips ringkas untuk membantu anda kempiskan perut. Untuk panduan lebih lanjut, sila rujuk kepada eBook Panduan Kurangkan 5kg 5 Minggu yang sekaligus membincangkan tentang cara-cara untuk membuang lemak.
  1. Penting kualiti daripada kuantiti! Tidak perlu melaku beratus-ratus sit ups setiap hari! 1 ataupun 2 sessi seminggu dengan latihan berkualiti adalah lebih baik. Don’t overtrain.
  2. Untuk merangsangkan otot abs anda setiap sessi, pelbagaikan latihan abs ! Gunakan latihan yang berbeza untuk latih abs daripada sudut yang berbeza. Bahagian abs termasuk, upper, mid, lower dan obliques.
  3. Fokus kepada contraction otot abs semasa latihan! Make sure its your abs that is doing the work dan bukan bahagian otot yang lain (back, leher dll).
  4. Fokus kepada pernafasan. Hembus nafas ketika “exertion” (ataupun ketika melakukan “crunch”). Ini akan membolehkan anda contract otot abs dengan sebaik mungkin
  5. Untuk sessi workout abs, lakukan 2-3 latihan yang berbeza. Sebagai panduan, stick to 3 set bagi setiap exercise dan 15-20 ulangan (reps) bagi setiap set!
  6. Latihan abs yang terbaik tidak akan menolong anda untuk kempiskan perut selagi adanya lapisan lemak antara otot dan kulit!
  7. Penjagaan makanan adalah mustahak untuk memeliki bahagian perut yang cantik! Elakkan makanan berminyak, garam. Minum banyak air dan pastikan anda mengamalkan diet yang seimbang.
  8. Look after your calories. Seperti mana yang saya katakana dahulu, anda harus create calorie deficit untuk membakar lemak berlebihan!
  9. Latihan cardio ataupun bersukan adalah cara yang sesuai untuk membakar calorie berlebihan! It also makes dieting easier as kita tidak perlu jaga pemakanan dengan terlalu rapat!
  10. Jika anda telahpun kurangkan lemak badan tetapi tidak lagi nampak abs yang cantik, kurangkan pengambilan sodium (yang takung air badan) dan make sure semasa latihan, abs are fatigued. Tingkatkan ulangan ataupun beban jika perlu!

hypertension @ Darah Tinggi

 


Kehidupan kita dipenuhi dengan angka dan nombor. Nombor kad pengenalan, nombor pin, tarikh lahir, tarikh tutup, masa, nombor telefon (nasib baiklah ada telefon pintar untuk membantu mengingatnya!). Begitu juga dari segi kesihatan dan tubuh badan kita, angka-angka seperti berat badan, ketinggian, tekanan darah, saiz pinggang – memainkan peranan sebagai indikator mengenai keadaan kesihatan dan kecergasan seseorang.
Berikut merupakan info angka bagi setiapa yang mempunyai tekanan darah tinggi, yang perlu diketahui oleh setiap orang.

Tekanan Darah (Hypertension)

Tekanan darah tinggi atau hypertension juga dikenali sebagai “silent killer” atau pembunuh senyap kerana ia tidak memberikan tanda-tanda symptom atau amaran seperti sakit gigi ataupun sakit belakang. Sekiranya tidak dirawat, ia boleh membawa risiko serangan jantung, strok, penyakit buah pinggang dan demensia.
Faktor-faktor yang mempengaruhinya termasuklah faktor seperti sejarah keluarga, umur, etnik dan gaya hidup seseorang tersebut.
  • Tekanan darah yang sihat adalah pada paras 120/80 mm Hg atau lebih rendah.
  • 140/90 mm Hg digunakan sebagai indikator untuk tekanan darah tinggi, tidak mengira usia seseorang itu. Angka pertama adalah tekanan sistolik iaitu tekanan apabila jantung mengalirkan darah ke seluruh tubuh anda.Angka kedua ialah tekanan diastolik iaitu tekanan ketika dalam keadaan rehat.

7 Langkah Kurangkan Tekanan Darah Tinggi

Masalah tekanan darah tinggi? Sebagai langkah permulaan untuk menangani kemungkinan anda mempunyai tekanan darah tinggi, iktuilah tip-tip berikut:

  1. Kurangkan berat badan. Ambil inisiatif untuk mengurangkan atau mengawal berat badan. Kurangkan berat 5kg pun sudah memberikan impak yang ketara dan mudahkan lagi kesan ubat pemberian doktor.
  2. Bersenamlah dengan kerap. Cuba untuk bersam dalam 30-45 minit pada hari minggu. Paling kurang pun 3-4x seminggu. Pada masa yang sama ini juga bantu kurangkan berat badan.
  3. Kurangkan pengambilan garam kepada kurang daripada 2.3g sehari. Garam umpama pasir yang serap air and tingkatkan tekanan darah. Kurangkan kicap, telur/ikan masin dan jangan tambah garam pada makanan yang sudah dihidang. Ingat: 1 teaspoon sudahpun mengandungi 2.3g!
  4. Jangan merokok: Kesan nikotin rokok dapat tingkatan tekanan darah sehingga 10 mm Hg sehingga sejam. Jadi sekiranya anda merokok sepanjang hari, tekanan darah pun lebih tinggi sepanjang masa.
  5. Kurangkan Stres. Stres kerja, duit, kesesakan jalan dan macam-macam lagi tingkatkan tekanan darah buat sementara waktu. Kalau anda mempunyai kronik stres, sudah tentu ia memudaratkan kesihatan anda dan boleh akibat serangan jantung, strok dan macam-macam lagi. Seimbangkan kehidupan anda dan cuba elak dari stres yang berpanjangan.
  6. Amalkan diet yang lebih baik. Sudah tentu diet seharian amatlah penting untuk mengawal dan kurangkan tekanan darah. Berikut adalah beberapa tip yang anda boleh amalkan:
    • Ketahuilah keperluan kalori seharian anda. Ini boleh mengawal jumlah makanan dan pasa masa yang masa bantu anda kawal atau kurangkan berat badan.
    • Makan 5-7 hidangan sehari tapi dalam sukatan yang kecil.
    • Lebihkan serat (fiber) seperi grains, nasi perang, buah-buahan dan sayur-sayuran segar.
    • Kawal kolesterol. Biasanya masalah tekanan darah tinggi, berat badan dismapingi dengan masalah kolesterol tinggi. Pastikan anda kawal tahap kolesterol anda dan elak makanan berkolesterol tinggi seperti makanan laut, organ-organ seperti paru-paru, kurangkan lemak-lemak haiwan dan tingkatkan pengambilan serat.
    • Pastikan ada sumber potassium dalam diet anda. Ia dapatkan kurangkan kesan garam pada tekanan darah. Pisang adalah pilihan potassium yang baik dan mudah didapati.
    • Kurangkan pengambilan alkohol dan kafein.
  7. Jangan leka: Pastikan anda melakukan pemeriksaan tekanan darah dengan kerap untuk memantau keadaan kesihatan anda. Walaupun anda tidak mempunyai masalah hypertension, pastikan anda melakukan pemeriksaan tekanan darah setiap 12 bulan sekali.

Pokok pegaga

PEGAGA
 
 
 
 
 
 
 Scientific name
:
Centella asiatica
(
L.)
Urban.
Common
name
:
Asiatic Pennywort, Gotu
Kola
Local name
:
Pegaga
Family
:
Umbelliferae
Introduction
This plant and its preparation have been in use
since ancient times especially in the Ayurv
edic
medical system of India and in the folk medicine of China
and Madagascar
.
It is recommended by the
World Health
Organization (WHO) as one of the most important medicinal
plant species to be conserved and cultivated. In Malaysia,
although it has been
used by our traditional healers in their
herbal
remedies, but its popularity is confined more as a
traditional vegetable or an ‘ulam’ especially among the
Malay communities rather than a medicinal plant.
Plant Description
Pegaga is a small, annual, slen
d
e
r, creeping her
b. It has
long
-
stalked, green
leaves with rounded apices which have
smooth textur
e with palmately netted veins. A
t the moment
there are three distinguishable pegaga subspecies namely
Pegaga salad, Pegaga kerinting or nyonya and Pegag
a
bi
asa
or pegaga ubi. The recommended race for commer
cial
production at this stage i
s pegaga ubi.
Plant habit
Pegaga grows wildly under a wide
range of conditions, some races prefer light shade, while
others do well in open sunny areas. Some even grow under
more harsh conditions like on stone
walls. In the wild, most of these plant are found in wet or moist surrounding like swamps, along
the margins of lakes, ponds and have also been seen growing in paddy fields
.
Plants parts
used
:
Whole plant, aerial pa
rts, roots
 
 
Uses in traditional medicine
Pegaga has been used for treating bronchitis, asthma, excessive secretion of gastric
juices,
dysentery,
kidn
ey trouble
and dropsy in many communities
.
This herb is said to have a direct
action on lowering the
blood pressure and is often referred to as rejuvenating medicament. In
Malaysia, it is commonly consumed
as
vegetable (ulam) among Malays, as a cooling drink by
the Chinese and as a brain tonic by the Indians. The Malays use the decoction of leaves to trea
t
leprosy and rheumatism. Infusion of the toased leaves or
juice extracted from the leaves
, together
with food
, is used to relieve minor dysentery in children. Some peoples also use
a
poultice of
leaves to treat sores, or pound leaves into a paste to apply
it to the body for fever. Juice from the
root is used to clean ulcerous wounds. The leaves are also believed to be good for mothers who
have just given birth and for preserving youthfulness