To prevent complications from iron overload caused by frequent transfusions in beta-thalassaemia major, iron chelation therapy is crucial. Iron chelation agents such as Deferiprone, Deferoxamine, and Deferasirox are commonly used for this purpose. Trientine is a copper chelator used in Wilson’s disease, while Dimercaptosuccinic acid is used as a lead chelator. Penicillamine is primarily used to treat copper toxicity.

Understanding Beta-Thalassaemia Major

Beta-thalassaemia major is a genetic disorder that results from the absence of beta globulin chains on chromosome 11. This condition typically presents in the first year of life with symptoms such as failure to thrive and hepatosplenomegaly. Microcytic anaemia is also a common feature, with raised levels of HbA2 and HbF, but absent HbA.

Management of beta-thalassaemia major involves repeated transfusions, which can lead to iron overload and organ failure. Therefore, iron chelation therapy, such as desferrioxamine, is crucial to prevent complications. It is important to understand the features and management of this condition to provide appropriate care for affected individuals.

The presence of necrosis in a tumour may indicate that it has become too large for its blood supply, suggesting a high grade tumour. However, when grading breast cancer using the Bloom-Richardson model, nuclear features such as mitoses, coarse chromatin, and pleomorphism are given more weight. The formation of tubular structures is a key indicator of the level of differentiation, with well differentiated tumours showing the presence of tubules.

Tumour Grading and Differentiation

Tumours can be classified based on their degree of differentiation, mitotic activity, and other characteristics. The grading system ranges from grade 1, which is the most differentiated, to grade 3 or 4, which is the least. The evaluation is subjective, but generally, high-grade tumours indicate a poor prognosis or rapid growth.

Glandular epithelium tumours tend to form acinar structures with a central lumen. Well-differentiated tumours exhibit excellent acinar formation, while poorly differentiated tumours appear as clumps of cells around a desmoplastic stroma. Some tumours produce mucous without acinar formation, and these are referred to as mucinous adenocarcinomas. Squamous cell tumours produce structures resembling epithelial cell components, and well-differentiated tumours may also produce keratin, depending on the tissue of origin.

ESR and its association with diseases

Erythrocyte sedimentation rate (ESR) is a laboratory test that measures the rate at which red blood cells settle in a tube over a period of time. Elevated ESR levels are often associated with inflammatory diseases such as rheumatoid arthritis, systemic lupus erythematosus, and polymyalgia rheumatica. In these conditions, the body’s immune system is activated, leading to inflammation and tissue damage. Malignancies such as myeloma can also cause an increase in ESR levels, particularly in females and with increasing age.

On the other hand, low ESR levels are seen in conditions such as polycythaemia, where there is an excess of red blood cells in the body. It is important to note that ESR is not a specific diagnostic test and must be interpreted in conjunction with other clinical findings. Multiple myeloma, a type of plasma cell neoplasm, is the most common haematological malignancy and can lead to a range of symptoms such as hypercalcaemia, renal failure, anaemia, and bone pain. While it is not curable, advances in treatment have significantly improved the median survival of patients. the association between ESR and various diseases can aid in the diagnosis and management of these conditions.

If a patient has a history of gastrectomy and is experiencing macrocytic anaemia, it is likely that they are suffering from B12 deficiency.

Vitamin B12 is essential for the development of red blood cells and the maintenance of the nervous system. It is absorbed through the binding of intrinsic factor, which is secreted by parietal cells in the stomach, and actively absorbed in the terminal ileum. A deficiency in vitamin B12 can be caused by pernicious anaemia, post gastrectomy, a vegan or poor diet, disorders or surgery of the terminal ileum, Crohn’s disease, or metformin use.

Symptoms of vitamin B12 deficiency include macrocytic anaemia, a sore tongue and mouth, neurological symptoms, and neuropsychiatric symptoms such as mood disturbances. The dorsal column is usually affected first, leading to joint position and vibration issues before distal paraesthesia.

Management of vitamin B12 deficiency involves administering 1 mg of IM hydroxocobalamin three times a week for two weeks, followed by once every three months if there is no neurological involvement. If a patient is also deficient in folic acid, it is important to treat the B12 deficiency first to avoid subacute combined degeneration of the cord.

The spleen is responsible for breaking down most of the red blood cells. This is achieved through the action of macrophages that identify and eliminate old red blood cells. It is worth noting that in a healthy individual, the liver, kidneys, and blood vessels do not participate in the breakdown of red blood cells. Additionally, while the bone marrow plays a crucial role in producing blood cells, it is not involved in the destruction of red blood cells.

Understanding Haemolytic Anaemias by Site

Haemolytic anaemias can be classified by the site of haemolysis, either intravascular or extravascular. In intravascular haemolysis, free haemoglobin is released and binds to haptoglobin. As haptoglobin becomes saturated, haemoglobin binds to albumin forming methaemalbumin, which can be detected by Schumm’s test. Free haemoglobin is then excreted in the urine as haemoglobinuria and haemosiderinuria. Causes of intravascular haemolysis include mismatched blood transfusion, red cell fragmentation due to heart valves, TTP, DIC, HUS, paroxysmal nocturnal haemoglobinuria, and cold autoimmune haemolytic anaemia.

On the other hand, extravascular haemolysis occurs when red blood cells are destroyed by macrophages in the spleen or liver. This type of haemolysis is commonly seen in haemoglobinopathies such as sickle cell anaemia and thalassaemia, hereditary spherocytosis, haemolytic disease of the newborn, and warm autoimmune haemolytic anaemia.

It is important to understand the site of haemolysis in order to properly diagnose and treat haemolytic anaemias. While both intravascular and extravascular haemolysis can lead to anaemia, the underlying causes and treatment approaches may differ.

Transfusion reactions can be classified as immunological or non-immunological. Immunological reactions are caused by anti-HLA or other antibodies in the donor blood, while non-immunological reactions are triggered by an inflammatory cascade with lipids found in blood products.

Symptoms of transfusion-related acute lung injury (TRALI) include dyspnea, cough, fever, and hypotension. Signs and investigations may reveal hypoxemia and pulmonary infiltrates visible on a chest x-ray.

Fluid overload, on the other hand, typically presents with dyspnea, orthopnea, and paroxysmal nocturnal dyspnea.

Severe allergic reactions are rare but may occur when the immune system attacks the donated blood, usually due to a mismatch in blood type. Symptoms may include urticaria, edema, dizziness, and headaches.

Blood product transfusion complications can be categorized into immunological, infective, and other complications. Immunological complications include acute haemolytic reactions, non-haemolytic febrile reactions, and allergic/anaphylaxis reactions. Infective complications may arise due to transmission of vCJD, although measures have been taken to minimize this risk. Other complications include transfusion-related acute lung injury (TRALI), transfusion-associated circulatory overload (TACO), hyperkalaemia, iron overload, and clotting.

Non-haemolytic febrile reactions are thought to be caused by antibodies reacting with white cell fragments in the blood product and cytokines that have leaked from the blood cell during storage. These reactions may occur in 1-2% of red cell transfusions and 10-30% of platelet transfusions. Minor allergic reactions may also occur due to foreign plasma proteins, while anaphylaxis may be caused by patients with IgA deficiency who have anti-IgA antibodies.

Acute haemolytic transfusion reaction is a serious complication that results from a mismatch of blood group (ABO) which causes massive intravascular haemolysis. Symptoms begin minutes after the transfusion is started and include a fever, abdominal and chest pain, agitation, and hypotension. Treatment should include immediate transfusion termination, generous fluid resuscitation with saline solution, and informing the lab. Complications include disseminated intravascular coagulation and renal failure.

TRALI is a rare but potentially fatal complication of blood transfusion that is characterized by the development of hypoxaemia/acute respiratory distress syndrome within 6 hours of transfusion. On the other hand, TACO is a relatively common reaction due to fluid overload resulting in pulmonary oedema. As well as features of pulmonary oedema, the patient may also be hypertensive, a key difference from patients with TRALI.

GVHD occurs when T cells from the donor tissue attack the recipient’s cells. This often manifests as skin and gastrointestinal symptoms in a host who lacks T cells, following a bone marrow or stem cell transplant. The immune response is initiated by donor CD4+ T cells recognizing the recipient’s MHC II as foreign, while donor CD8+ T cells cause tissue damage.

Understanding Graft Versus Host Disease

Graft versus host disease (GVHD) is a complication that can occur after bone marrow or solid organ transplantation. It happens when the T cells in the donor tissue attack the recipient’s cells. This is different from transplant rejection, where the recipient’s immune cells attack the donor tissue. GVHD is diagnosed using the Billingham criteria, which require that the transplanted tissue contains functioning immune cells, the donor and recipient are immunologically different, and the recipient is immunocompromised.

The incidence of GVHD varies, but it can occur in up to 50% of patients who receive allogeneic bone marrow transplants. Risk factors include poorly matched donor and recipient, the type of conditioning used before transplantation, gender disparity between donor and recipient, and the source of the graft.

Acute and chronic GVHD are considered separate syndromes. Acute GVHD typically occurs within 100 days of transplantation and affects the skin, liver, and gastrointestinal tract. Chronic GVHD may occur after acute disease or arise de novo and has a more varied clinical picture.

Diagnosis of GVHD is largely clinical and based on the exclusion of other pathology. Signs and symptoms of acute GVHD include a painful rash, jaundice, diarrhea, nausea, vomiting, and fever. Chronic GVHD can affect the skin, eyes, gastrointestinal tract, and lungs.

Treatment of GVHD involves immunosuppression and supportive measures. Intravenous steroids are the mainstay of treatment for severe cases of acute GVHD, while extended courses of steroid therapy are often needed in chronic GVHD. Second-line therapies include anti-TNF, mTOR inhibitors, and extracorporeal photopheresis. Topical steroid therapy may be sufficient in mild disease with limited cutaneous involvement. However, excessive immunosuppression may increase the risk of infection and limit the beneficial graft-versus-tumor effect of the transplant.

If DNA cannot be repaired, it triggers cellular apoptosis instead of necrosis.

Genetic Conditions and Their Association with Surgical Diseases

Li-Fraumeni Syndrome is an autosomal dominant genetic condition caused by mutations in the p53 tumour suppressor gene. Individuals with this syndrome have a high incidence of malignancies, particularly sarcomas and leukaemias. The diagnosis is made when an individual develops sarcoma under the age of 45 or when a first-degree relative is diagnosed with any cancer below the age of 45 and another family member develops malignancy under the age of 45 or sarcoma at any age.

BRCA 1 and 2 are genetic conditions carried on chromosome 17 and chromosome 13, respectively. These conditions are linked to developing breast cancer with a 60% risk and an associated risk of developing ovarian cancer with a 55% risk for BRCA 1 and 25% risk for BRCA 2. BRCA2 mutation is also associated with prostate cancer in men.

Lynch Syndrome is another autosomal dominant genetic condition that causes individuals to develop colonic cancer and endometrial cancer at a young age. 80% of affected individuals will get colonic and/or endometrial cancer. High-risk individuals may be identified using the Amsterdam criteria, which include three or more family members with a confirmed diagnosis of colorectal cancer, two successive affected generations, and one or more colon cancers diagnosed under the age of 50 years.

Gardners syndrome is an autosomal dominant familial colorectal polyposis that causes multiple colonic polyps. Extra colonic diseases include skull osteoma, thyroid cancer, and epidermoid cysts. Desmoid tumours are seen in 15% of individuals with this syndrome. Due to colonic polyps, most patients will undergo colectomy to reduce the risk of colorectal cancer. It is now considered a variant of familial adenomatous polyposis coli.

Overall, these genetic conditions have a significant association with surgical diseases, and early identification and management can help reduce the risk of malignancies and other associated conditions.

The Thymus Gland: Development, Structure, and Function

The thymus gland is an encapsulated organ that develops from the third and fourth pharyngeal pouches. It descends to the anterior superior mediastinum and is subdivided into lobules, each consisting of a cortex and a medulla. The cortex is made up of tightly packed lymphocytes, while the medulla is mostly composed of epithelial cells. Hassall’s corpuscles, which are concentrically arranged medullary epithelial cells that may surround a keratinized center, are also present.

The inferior parathyroid glands, which also develop from the third pharyngeal pouch, may be located with the thymus gland. The thymus gland’s arterial supply comes from the internal mammary artery or pericardiophrenic arteries, while its venous drainage is to the left brachiocephalic vein. The thymus gland plays a crucial role in the development and maturation of T-cells, which are essential for the immune system’s proper functioning.

The correct diagnosis for the patient is sideroblastic anaemia, which is characterized by hypochromic microcytic anaemia, high levels of ferritin iron and transferrin saturation, and basophilic stippling of red blood cells. This condition is caused by vitamin B6 deficiency due to frequent alcohol consumption, leading to abnormal heme production. The peripheral smear shows basophilic stippling of red blood cells, and there is iron overload causing iron deposition in the bone marrow, observed as increased staining with Prussian blue.

Anaemia of chronic disease, iron deficiency anaemia, and aplastic anaemia are incorrect diagnoses. Anaemia of chronic disease is usually normocytic normochromic and has significantly low levels of folate, B12, and iron while ferritin is high. Iron deficiency anaemia may be microcytic hypochromic, but serum iron, ferritin, and transferrin levels would be reduced. Aplastic anaemia presents with pancytopenia and is rarely found in the given age group.

Understanding Sideroblastic Anaemia

Sideroblastic anaemia is a medical condition that occurs when red blood cells fail to produce enough haem, which is partly synthesized in the mitochondria. This results in the accumulation of iron in the mitochondria, forming a ring around the nucleus known as a ring sideroblast. The condition can be either congenital or acquired.

The congenital cause of sideroblastic anaemia is delta-aminolevulinate synthase-2 deficiency. On the other hand, acquired causes include myelodysplasia, alcohol, lead, and anti-TB medications.

To diagnose sideroblastic anaemia, doctors may conduct a full blood count, iron studies, and a blood film. The results may show hypochromic microcytic anaemia, high ferritin, high iron, high transferrin saturation, and basophilic stippling of red blood cells. A bone marrow test may also be done, and Prussian blue staining can reveal ringed sideroblasts.

Management of sideroblastic anaemia is mainly supportive, and treatment focuses on addressing any underlying cause. Pyridoxine may also be prescribed to help manage the condition.

In summary, sideroblastic anaemia is a condition that affects the production of haem in red blood cells, leading to the accumulation of iron in the mitochondria. It can be congenital or acquired, and diagnosis involves various tests. Treatment is mainly supportive, and addressing any underlying cause is crucial.

The IgM antibody is composed of five antibodies joined together and is primarily responsible for clumping antigens. Anti-A and anti-B antibodies are typically IgM and are produced during early childhood due to exposure to environmental factors like bacteria, viruses, and food.

On the other hand, IgG is the most prevalent antibody and exists as a single antibody complex. IgD, on the other hand, is located on the surface of B-lymphocytes.

Blood product transfusion complications can be categorized into immunological, infective, and other complications. Immunological complications include acute haemolytic reactions, non-haemolytic febrile reactions, and allergic/anaphylaxis reactions. Infective complications may arise due to transmission of vCJD, although measures have been taken to minimize this risk. Other complications include transfusion-related acute lung injury (TRALI), transfusion-associated circulatory overload (TACO), hyperkalaemia, iron overload, and clotting.

Non-haemolytic febrile reactions are thought to be caused by antibodies reacting with white cell fragments in the blood product and cytokines that have leaked from the blood cell during storage. These reactions may occur in 1-2% of red cell transfusions and 10-30% of platelet transfusions. Minor allergic reactions may also occur due to foreign plasma proteins, while anaphylaxis may be caused by patients with IgA deficiency who have anti-IgA antibodies.

Acute haemolytic transfusion reaction is a serious complication that results from a mismatch of blood group (ABO) which causes massive intravascular haemolysis. Symptoms begin minutes after the transfusion is started and include a fever, abdominal and chest pain, agitation, and hypotension. Treatment should include immediate transfusion termination, generous fluid resuscitation with saline solution, and informing the lab. Complications include disseminated intravascular coagulation and renal failure.

TRALI is a rare but potentially fatal complication of blood transfusion that is characterized by the development of hypoxaemia/acute respiratory distress syndrome within 6 hours of transfusion. On the other hand, TACO is a relatively common reaction due to fluid overload resulting in pulmonary oedema. As well as features of pulmonary oedema, the patient may also be hypertensive, a key difference from patients with TRALI.

The submandibular lymph nodes are the primary drainage site for the mid-portion of the tongue. Subsequently, the lymphatic fluid will spread to the deep cervical lymph nodes.

Lymphatic Drainage of the Tongue

The lymphatic drainage of the tongue varies depending on the location of the tumour. The anterior two-thirds of the tongue have minimal communication of lymphatics across the midline, resulting in metastasis to the ipsilateral nodes being more common. On the other hand, the posterior third of the tongue has communicating networks, leading to early bilateral nodal metastases being more common in this area.

The tip of the tongue drains to the submental nodes and then to the deep cervical nodes, while the mid portion of the tongue drains to the submandibular nodes and then to the deep cervical nodes. If mid tongue tumours are laterally located, they will usually drain to the ipsilateral deep cervical nodes. However, those from more central regions may have bilateral deep cervical nodal involvement. Understanding the lymphatic drainage of the tongue is crucial in determining the spread of tumours and planning appropriate treatment.

Athletes who use EPO are at risk of developing polycythemia. Cyclists are known to frequently use EPO, which can cause localized erythema on the abdomen from repeated injections. The patient’s headaches are not migrainous as they lack associated symptoms such as aura, photophobia, or phonophobia. Renal cell carcinoma is the primary type of kidney cancer in adults and typically presents with flank pain, haematuria, and a flank mass. Other symptoms may include weight loss, night sweats, fever, and malaise.

Polycythaemia is a condition that can be classified as relative, primary (polycythaemia rubra vera), or secondary. Relative polycythaemia can be caused by dehydration or stress, such as in Gaisbock syndrome. Primary polycythaemia rubra vera is a rare blood disorder that causes the bone marrow to produce too many red blood cells. Secondary polycythaemia can be caused by conditions such as COPD, altitude, obstructive sleep apnoea, or excessive erythropoietin production due to certain tumors or growths. To distinguish between true polycythaemia and relative polycythaemia, red cell mass studies may be used. In true polycythaemia, the total red cell mass in males is greater than 35 ml/kg and in women is greater than 32 ml/kg. Uterine fibroids may also cause polycythaemia indirectly by causing menorrhagia, but this is rarely a clinical problem.

Lymphatic Drainage of the Tongue

The lymphatic drainage of the tongue varies depending on the location of the tumour. The anterior two-thirds of the tongue have minimal communication of lymphatics across the midline, resulting in metastasis to the ipsilateral nodes being more common. On the other hand, the posterior third of the tongue has communicating networks, leading to early bilateral nodal metastases being more common in this area.

The tip of the tongue drains to the submental nodes and then to the deep cervical nodes, while the mid portion of the tongue drains to the submandibular nodes and then to the deep cervical nodes. If mid tongue tumours are laterally located, they will usually drain to the ipsilateral deep cervical nodes. However, those from more central regions may have bilateral deep cervical nodal involvement. Understanding the lymphatic drainage of the tongue is crucial in determining the spread of tumours and planning appropriate treatment.

Hb SC is a less severe variant of sickle cell disease that can be detected early through screening of children in the UK. This condition is characterized by the presence of both the sickle mutation and the HbC mutation, which results in a lysine substitution for glutamic acid on position 6 of the beta chain. While HbSC shares similarities with sickle cell disease, its symptoms are less frequent and severe. The severity of the disease can vary depending on the specific genotype, with HbAA being normal, HbAS being asymptomatic, HbSC/Sβ+ being moderately affected, and HbSS/Sβ0 being severely affected due to the absence of normal haemoglobin.

Understanding Sickle-Cell Anaemia

Sickle-cell anaemia is a genetic disorder that occurs when an abnormal haemoglobin chain, known as HbS, is synthesized due to an autosomal recessive condition. This condition is more common in people of African descent, as the heterozygous condition offers some protection against malaria. In the UK, around 10% of Afro-Caribbean individuals are carriers of HbS. Symptoms in homozygotes typically do not develop until 4-6 months when the abnormal HbSS molecules take over from fetal haemoglobin.

The pathophysiology of sickle-cell anaemia involves the substitution of the polar amino acid glutamate with the non-polar valine in each of the two beta chains (codon 6) of haemoglobin. This substitution decreases the water solubility of deoxy-Hb, causing HbS molecules to polymerize and sickle in the deoxygenated state. HbAS patients sickle at p02 2.5 – 4 kPa, while HbSS patients sickle at p02 5 – 6 kPa. Sickle cells are fragile and can cause haemolysis, block small blood vessels, and lead to infarction.

To diagnose sickle-cell anaemia, haemoglobin electrophoresis is the definitive test. It is essential to understand the pathophysiology and symptoms of sickle-cell anaemia to provide appropriate care and management for affected individuals.

HPV Infection and Cervical Cancer

Human papillomavirus (HPV) infection is the primary risk factor for cervical cancer, with subtypes 16, 18, and 33 being the most carcinogenic. Other common subtypes, such as 6 and 11, are associated with genital warts but are not carcinogenic. When endocervical cells become infected with HPV, they may undergo changes that lead to the development of koilocytes. These cells have distinct characteristics, including an enlarged nucleus, irregular nuclear membrane contour, hyperchromasia (darker staining of the nucleus), and a perinuclear halo. These changes are important diagnostic markers for cervical cancer and can be detected through Pap smears or other screening methods. Early detection and treatment of HPV infection and cervical cancer can greatly improve outcomes and reduce the risk of complications.

Vincristine inhibits the formation of microtubules, which are essential for separating chromosomes during cell division. This mechanism is also shared by paclitaxel, a member of the taxane family. Alkylating agents, such as cyclophosphamide, disrupt the double helix of DNA by adding an alkyl group to guanine bases. Methotrexate inhibits dihydrofolate reductase, an enzyme that supports folate in DNA synthesis. Pyrimidine antagonists, like cytarabine, prevent the use of pyrimidines in DNA synthesis.

Cytotoxic agents are drugs that are used to kill cancer cells. There are several types of cytotoxic agents, each with their own mechanism of action and potential adverse effects. Alkylating agents, such as cyclophosphamide, work by causing cross-linking in DNA. However, they can also cause haemorrhagic cystitis, myelosuppression, and transitional cell carcinoma. Cytotoxic antibiotics, like bleomycin and anthracyclines, degrade preformed DNA and stabilize DNA-topoisomerase II complex, respectively. However, they can also cause lung fibrosis and cardiomyopathy. Antimetabolites, such as methotrexate and fluorouracil, inhibit dihydrofolate reductase and thymidylate synthesis, respectively. However, they can also cause myelosuppression, mucositis, and liver or lung fibrosis. Drugs that act on microtubules, like vincristine and docetaxel, inhibit the formation of microtubules and prevent microtubule depolymerisation & disassembly, respectively. However, they can also cause peripheral neuropathy, myelosuppression, and paralytic ileus. Topoisomerase inhibitors, like irinotecan, inhibit topoisomerase I, which prevents relaxation of supercoiled DNA. However, they can also cause myelosuppression. Other cytotoxic drugs, such as cisplatin and hydroxyurea, cause cross-linking in DNA and inhibit ribonucleotide reductase, respectively. However, they can also cause ototoxicity, peripheral neuropathy, hypomagnesaemia, and myelosuppression.

Venous Ulceration and the Importance of Identifying Arterial Disease

Venous ulcerations are a common type of ulcer that affects the lower extremities. The underlying cause of venous congestion, which can promote ulceration, is venous insufficiency. The treatment for venous ulceration involves controlling oedema, treating any infection, and compression. However, compressive dressings or devices should not be applied if the arterial circulation is impaired. Therefore, it is crucial to identify any arterial disease, and the ankle-brachial pressure index is a simple way of doing this. If indicated, one may progress to a lower limb arteriogram.

It is important to note that there is no clinical sign of infection, and although a bacterial swab would help to rule out pathogens within the ulcer, arterial insufficiency is the more important issue. If there is a clinical suspicion of DVT, then duplex (or rarely a venogram) is indicated to decide on the indication for anticoagulation. By identifying arterial disease, healthcare professionals can ensure that appropriate treatment is provided and avoid potential complications from compressive dressings or devices.

Understanding Sickle-Cell Anaemia

Sickle-cell anaemia is a genetic disorder that occurs when an abnormal haemoglobin chain, known as HbS, is synthesized due to an autosomal recessive condition. This condition is more common in people of African descent, as the heterozygous condition offers some protection against malaria. In the UK, around 10% of Afro-Caribbean individuals are carriers of HbS. Symptoms in homozygotes typically do not develop until 4-6 months when the abnormal HbSS molecules take over from fetal haemoglobin.

The pathophysiology of sickle-cell anaemia involves the substitution of the polar amino acid glutamate with the non-polar valine in each of the two beta chains (codon 6) of haemoglobin. This substitution decreases the water solubility of deoxy-Hb, causing HbS molecules to polymerize and sickle in the deoxygenated state. HbAS patients sickle at p02 2.5 – 4 kPa, while HbSS patients sickle at p02 5 – 6 kPa. Sickle cells are fragile and can cause haemolysis, block small blood vessels, and lead to infarction.

To diagnose sickle-cell anaemia, haemoglobin electrophoresis is the definitive test. It is essential to understand the pathophysiology and symptoms of sickle-cell anaemia to provide appropriate care and management for affected individuals.

Understanding Chronic Myeloid Leukaemia and its Management

Chronic myeloid leukaemia (CML) is a type of cancer that affects the blood and bone marrow. It is characterized by the presence of the Philadelphia chromosome in more than 95% of patients. This chromosome is formed due to a translocation between chromosomes 9 and 22, resulting in the fusion of the ABL proto-oncogene and the BCR gene. The resulting BCR-ABL gene produces a fusion protein that has excessive tyrosine kinase activity.

CML typically affects individuals between the ages of 60-70 years and presents with symptoms such as anaemia, weight loss, sweating, and splenomegaly. The condition is also associated with an increase in granulocytes at different stages of maturation and thrombocytosis. In some cases, CML may undergo blast transformation, leading to acute myeloid leukaemia (AML) or acute lymphoblastic leukaemia (ALL).

The management of CML involves various treatment options, including imatinib, which is considered the first-line treatment. Imatinib is an inhibitor of the tyrosine kinase associated with the BCR-ABL defect and has a very high response rate in chronic phase CML. Other treatment options include hydroxyurea, interferon-alpha, and allogenic bone marrow transplant. With proper management, individuals with CML can lead a normal life.

FFP is frozen shortly after collection due to the temperature sensitivity of factors V and VIII.

Blood Products and Cell Saver Devices

Blood products are essential in various medical procedures, especially in cases where patients require transfusions due to anaemia or bleeding. Packed red cells, platelet-rich plasma, platelet concentrate, fresh frozen plasma, and cryoprecipitate are some of the commonly used whole blood fractions. Fresh frozen plasma is usually administered to patients with clotting deficiencies, while cryoprecipitate is a rich source of Factor VIII and fibrinogen. Cross-matching is necessary for all blood products, and cell saver devices are used to collect and re-infuse a patient’s own blood lost during surgery.

Cell saver devices come in two types, those that wash the blood cells before re-infusion and those that do not. The former is more expensive and complicated to operate but reduces the risk of re-infusing contaminated blood. The latter avoids the use of donor blood and may be acceptable to Jehovah’s witnesses. However, it is contraindicated in malignant diseases due to the risk of facilitating disease dissemination.

In some surgical patients, the use of warfarin can pose specific problems and may require the use of specialised blood products. Warfarin reversal can be achieved through the administration of vitamin K, fresh frozen plasma, or human prothrombin complex. Fresh frozen plasma is used less commonly now as a first-line warfarin reversal, and human prothrombin complex is preferred due to its rapid action. However, it should be given with vitamin K as factor 6 has a short half-life.

The primary route of coagulation is the extrinsic pathway, which is inhibited by heparin’s ability to prevent the activation of factors 2, 9, 10, and 11. The convergence of both pathways occurs during the activation of factor 10. Fibrinogen is transformed into fibrin by thrombin. Plasminogen is converted to plasmin during fibrinolysis, which breaks down fibrin.

The Coagulation Cascade: Two Pathways to Fibrin Formation

The coagulation cascade is a complex process that leads to the formation of a blood clot. There are two pathways that can lead to fibrin formation: the intrinsic pathway and the extrinsic pathway. The intrinsic pathway involves components that are already present in the blood and has a minor role in clotting. It is initiated by subendothelial damage, such as collagen, which leads to the formation of the primary complex on collagen by high-molecular-weight kininogen (HMWK), prekallikrein, and Factor 12. This complex activates Factor 11, which in turn activates Factor 9. Factor 9, along with its co-factor Factor 8a, forms the tenase complex, which activates Factor 10.

The extrinsic pathway, on the other hand, requires tissue factor released by damaged tissue. This pathway is initiated by tissue damage, which leads to the binding of Factor 7 to tissue factor. This complex activates Factor 9, which works with Factor 8 to activate Factor 10. Both pathways converge at the common pathway, where activated Factor 10 causes the conversion of prothrombin to thrombin. Thrombin hydrolyses fibrinogen peptide bonds to form fibrin and also activates factor 8 to form links between fibrin molecules.

Finally, fibrinolysis occurs, which is the process of clot resorption. Plasminogen is converted to plasmin to facilitate this process. It is important to note that certain factors are involved in both pathways, such as Factor 10, and that some factors are vitamin K dependent, such as Factors 2, 7, 9, and 10. The intrinsic pathway can be assessed by measuring the activated partial thromboplastin time (APTT), while the extrinsic pathway can be assessed by measuring the prothrombin time (PT).

The Development of Haematopoiesis in the Foetus

The development of haematopoiesis in the foetus is a complex process that involves several organs. Initially, the yolk sac is the primary site of haematopoiesis until around two months gestation when the liver takes over. The liver remains the most important site of haematopoiesis until about month seven when the bone marrow becomes the predominant site throughout life.

After the age of 20, haematopoiesis occurs mainly in the proximal bones, with production in the distal lone bones decreasing. However, in certain disease states such as β-thalassaemia, haematopoiesis can occur outside of the bone marrow, known as extra-medullary haematopoiesis. the development of haematopoiesis in the foetus is important for identifying potential abnormalities and diseases that may arise during this process.

Oxygen Transport and Factors Affecting Haemoglobin Saturation

Oxygen transport in the body is mainly carried out by erythrocytes, with only 1% of oxygen being transported as a solution due to its limited solubility. The amount of oxygen transported depends on the concentration of haemoglobin and its degree of saturation. Haemoglobin is a globular protein composed of four subunits, with two alpha and two beta subunits forming globin. Haem, which surrounds an iron atom in its ferrous state, can form two additional bonds with oxygen and a polypeptide chain. The oxygenation of haemoglobin is a reversible reaction, and the molecular shape of haemoglobin facilitates the binding of subsequent oxygen molecules.

The oxygen dissociation curve describes the relationship between the percentage of saturated haemoglobin and partial pressure of oxygen in the blood, and it is not affected by haemoglobin concentration. The curve can be shifted to the right or left by various factors. Chronic anaemia, for example, causes an increase in 2,3 DPG levels, which shifts the curve to the right, resulting in lower oxygen delivery. The Haldane effect causes a shift to the left, resulting in decreased oxygen delivery to tissues, while the Bohr effect causes a shift to the right, resulting in enhanced oxygen delivery to tissues. Factors that shift the curve to the left include low levels of H+, pCO2, 2,3-DPG, and temperature, as well as the presence of HbF, methaemoglobin, and carboxyhaemoglobin. Factors that shift the curve to the right include raised levels of H+, pCO2, and 2,3-DPG, as well as increased temperature.

Understanding the coagulation cascade is crucial, but it’s also important to know the substances that the body secretes to maintain normal blood vessel function and prevent excessive clotting. In primary haemostasis, the formation of a platelet plug is a critical step, and several substances in the blood vessels work against platelet activation to keep the blood flowing smoothly.

Prostacyclin, which is produced from arachidonic acid, inhibits platelet activation. Nitric oxide prevents platelet adhesion to the vessel wall and also dilates blood vessels to increase blood flow. Endothelial ADPase inhibits ADP, which is a platelet activator.

Fibrinogen, a large and soluble compound, is the precursor to fibrin, which forms an insoluble mesh to trap blood cells and platelets within a clot. This is the final step of the coagulation cascade, and the clot is further strengthened by fibrin-stabilising factor. Thromboxane, produced by activated platelets, increases platelet activation and constricts blood vessels, making it another thrombotic agent. Aggregated platelets produce ADP, which further enhances platelet aggregation.

The Coagulation Cascade: Two Pathways to Fibrin Formation

The coagulation cascade is a complex process that leads to the formation of a blood clot. There are two pathways that can lead to fibrin formation: the intrinsic pathway and the extrinsic pathway. The intrinsic pathway involves components that are already present in the blood and has a minor role in clotting. It is initiated by subendothelial damage, such as collagen, which leads to the formation of the primary complex on collagen by high-molecular-weight kininogen (HMWK), prekallikrein, and Factor 12. This complex activates Factor 11, which in turn activates Factor 9. Factor 9, along with its co-factor Factor 8a, forms the tenase complex, which activates Factor 10.

The extrinsic pathway, on the other hand, requires tissue factor released by damaged tissue. This pathway is initiated by tissue damage, which leads to the binding of Factor 7 to tissue factor. This complex activates Factor 9, which works with Factor 8 to activate Factor 10. Both pathways converge at the common pathway, where activated Factor 10 causes the conversion of prothrombin to thrombin. Thrombin hydrolyses fibrinogen peptide bonds to form fibrin and also activates factor 8 to form links between fibrin molecules.

Finally, fibrinolysis occurs, which is the process of clot resorption. Plasminogen is converted to plasmin to facilitate this process. It is important to note that certain factors are involved in both pathways, such as Factor 10, and that some factors are vitamin K dependent, such as Factors 2, 7, 9, and 10. The intrinsic pathway can be assessed by measuring the activated partial thromboplastin time (APTT), while the extrinsic pathway can be assessed by measuring the prothrombin time (PT).

Exposure to nitrosamine increases the likelihood of developing oesophageal and gastric cancer. Nitrosamine is commonly added to processed meats like bacon, ham, sausages, and hot dogs, making frequent consumption of these foods a risk factor for these types of cancer. Nitrosamine is also present in tobacco smoke. On the other hand, flavonoids, which are abundant in plants, have been linked to a decreased risk of gastric cancer. Acrylamide is present in starchy foods, while fluoride is used in water and toothpaste to prevent tooth decay.

Understanding Carcinogens and Their Link to Cancer

Carcinogens are substances that have the potential to cause cancer. These substances can be found in various forms, including chemicals, radiation, and viruses. Aflatoxin, which is produced by Aspergillus, is a carcinogen that can cause liver cancer. Aniline dyes, on the other hand, can lead to bladder cancer, while asbestos is known to cause mesothelioma and bronchial carcinoma. Nitrosamines are another type of carcinogen that can cause oesophageal and gastric cancer, while vinyl chloride can lead to hepatic angiosarcoma.

It is important to understand the link between carcinogens and cancer, as exposure to these substances can increase the risk of developing the disease. By identifying and avoiding potential carcinogens, individuals can take steps to reduce their risk of cancer. Additionally, researchers continue to study the effects of various substances on the body, in order to better understand the mechanisms behind cancer development and to develop new treatments and prevention strategies. With continued research and education, it is possible to reduce the impact of carcinogens on human health.

There are five potential disease phenotypes of alpha thalassaemia based on the number of faulty or missing globin alleles in a patient’s genotype. These include silent carrier (alpha(+) heterozygous) for one missing allele, alpha thalassaemia trait: alpha(0) heterozygous for two missing alleles, alpha thalassaemia trait: alpha(+) homozygous for two missing alleles, haemoglobin H disease for three missing alleles, and (–/–) for four missing alleles.

Understanding Alpha-Thalassaemia

Alpha-thalassaemia is a genetic disorder that results from a deficiency of alpha chains in haemoglobin. The condition is caused by a mutation in the alpha-globulin genes located on chromosome 16. The severity of the disease depends on the number of alpha globulin alleles affected. If one or two alleles are affected, the blood picture would be hypochromic and microcytic, but the haemoglobin level would typically be normal. However, if three alleles are affected, it results in a hypochromic microcytic anaemia with splenomegaly, which is known as Hb H disease. In the case of all four alleles being affected, which is known as homozygote, it can lead to death in utero, also known as hydrops fetalis or Bart’s hydrops. Understanding the different levels of severity of alpha-thalassaemia is crucial in diagnosing and managing the condition.

Cytarabine is a medication used in chemotherapy to treat acute myeloid leukaemia (AML). It works by interfering with DNA synthesis during the S-phase of the cell cycle and inhibiting DNA polymerase.

Allopurinol is a medication that inhibits xanthine oxidase, which prevents the production of uric acid. It is commonly used to treat gout, but can also be used to prevent hyperuricaemia in high-grade lymphoma and leukaemia before chemotherapy treatment.

Methotrexate works by inhibiting dihydrofolate reductase and thymidylate synthesis. It is used to treat rheumatoid arthritis and various types of cancer.

Ondansetron is an anti-emetic medication that is used to prevent nausea during chemotherapy treatment. It works by selectively blocking serotonin receptors (5-HT3) in the chemoreceptor trigger zone (CTZ) of the medulla.

Cytotoxic agents are drugs that are used to kill cancer cells. There are several types of cytotoxic agents, each with their own mechanism of action and potential adverse effects. Alkylating agents, such as cyclophosphamide, work by causing cross-linking in DNA. However, they can also cause haemorrhagic cystitis, myelosuppression, and transitional cell carcinoma. Cytotoxic antibiotics, like bleomycin and anthracyclines, degrade preformed DNA and stabilize DNA-topoisomerase II complex, respectively. However, they can also cause lung fibrosis and cardiomyopathy. Antimetabolites, such as methotrexate and fluorouracil, inhibit dihydrofolate reductase and thymidylate synthesis, respectively. However, they can also cause myelosuppression, mucositis, and liver or lung fibrosis. Drugs that act on microtubules, like vincristine and docetaxel, inhibit the formation of microtubules and prevent microtubule depolymerisation & disassembly, respectively. However, they can also cause peripheral neuropathy, myelosuppression, and paralytic ileus. Topoisomerase inhibitors, like irinotecan, inhibit topoisomerase I, which prevents relaxation of supercoiled DNA. However, they can also cause myelosuppression. Other cytotoxic drugs, such as cisplatin and hydroxyurea, cause cross-linking in DNA and inhibit ribonucleotide reductase, respectively. However, they can also cause ototoxicity, peripheral neuropathy, hypomagnesaemia, and myelosuppression.

Free haemoglobin is bound by haptoglobin.

Copper is bound by ceruloplasmin.

Stored iron in the body is in the form of ferritin.

Free heme molecules are bound by hemopexin.

Laboratory Findings in Haematological Disease

Haptoglobin is a laboratory test that measures the level of a protein that binds to free haemoglobin. A decrease in haptoglobin levels is often associated with intravascular haemolysis, a condition where red blood cells are destroyed within blood vessels. On the other hand, an increase in mean corpuscular haemoglobin concentration (MCHC) is commonly seen in hereditary spherocytosis and autoimmune haemolytic anemia. In contrast, a decrease in MCHC is often observed in microcytic anaemia, which is commonly caused by iron deficiency. It is important to note that autoimmune haemolytic anemia is often associated with spherocytosis. These laboratory findings are commonly tested in haematological disease exams.

A helpful mnemonic for remembering transfusion reactions is Got a bad unit. Each letter represents a potential complication:

G – Graft vs. Host disease
O – Overload
T – Thrombocytopenia
A – Alloimmunization
B – Blood pressure unstable
A – Acute hemolytic reaction
D – Delayed hemolytic reaction
U – Urticaria
N – Neutrophilia
I – Infection
T – Transfusion-associated lung injury

Graft vs. Host disease occurs when the patient’s own lymphocytes are similar to the donor’s lymphocytes, causing severe complications. Thrombocytopenia may occur a few days after transfusion and may resolve on its own. Patients with IGA antibodies require IgA deficient blood transfusions.

Blood product transfusion complications can be categorized into immunological, infective, and other complications. Immunological complications include acute haemolytic reactions, non-haemolytic febrile reactions, and allergic/anaphylaxis reactions. Infective complications may arise due to transmission of vCJD, although measures have been taken to minimize this risk. Other complications include transfusion-related acute lung injury (TRALI), transfusion-associated circulatory overload (TACO), hyperkalaemia, iron overload, and clotting.

Non-haemolytic febrile reactions are thought to be caused by antibodies reacting with white cell fragments in the blood product and cytokines that have leaked from the blood cell during storage. These reactions may occur in 1-2% of red cell transfusions and 10-30% of platelet transfusions. Minor allergic reactions may also occur due to foreign plasma proteins, while anaphylaxis may be caused by patients with IgA deficiency who have anti-IgA antibodies.

Acute haemolytic transfusion reaction is a serious complication that results from a mismatch of blood group (ABO) which causes massive intravascular haemolysis. Symptoms begin minutes after the transfusion is started and include a fever, abdominal and chest pain, agitation, and hypotension. Treatment should include immediate transfusion termination, generous fluid resuscitation with saline solution, and informing the lab. Complications include disseminated intravascular coagulation and renal failure.

TRALI is a rare but potentially fatal complication of blood transfusion that is characterized by the development of hypoxaemia/acute respiratory distress syndrome within 6 hours of transfusion. On the other hand, TACO is a relatively common reaction due to fluid overload resulting in pulmonary oedema. As well as features of pulmonary oedema, the patient may also be hypertensive, a key difference from patients with TRALI.