pace your MRCP-PACES
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2 523
*Announcement for Online Session No 89*
*28 May 2023*
DEAR DOCTORS :
MAY I HAVE YOUR ATTENTION PLEASE :
*Today we will have an online session on Zoom discussing 2 station 5 ( BCC )* regarding our preparation for MRCP PACES ( UK )
TIMINGS :
Saudia Arabia: 4 00 pm
Pakistan : 6 00 pm
Bangladesh : 7 00 pm
India : 6 30 pm
Singapore : 9 00 pm
Hong Kong : 9 00 pm
Malaysia : 9 00 pm
Egypt : 4 00 pm
Libya : 3 00 pm
Bahrain : 4 00 pm
Burma ( Myanmar ) :7 30 pm
Sudan : 3 00 pm
UAE : 5 00 pm
UK : 2 00 pm
Ireland ( Dublin ) : 2 00 pm
Afghanistan : 5 30 pm
Kenya : 4 00 pm
Germany ( Berlin ) : 3 00 pm
Nigeria : 2 00 pm
Japan ( Tokyo ) : 10 00 pm
Denmark : 3 00 pm
Qatar : 4 00 pm
Oman : 5 00 pm
Italy : 3 00 pm
Indonesia : 8 00 pm
Mauritius : 5 00 pm
Iraq : 4 00 pm
Texas Usa : 8 00 am
Kuwait : 4 00 pm
( please Google for your local time zones to avoid any inconvenience )
Zoom meeting link will be shared 5 minutes before start time.
The candidates for today's session have been selected.
GOOD LUCK.
2 523
*paceUrMRCP-PACES HALL OF FAME*
We are thankful to our respected coalleagues who have made us proud by their success in PACES MRCP ( UK ).
We believe that this number will keep on increasing
136.Dr Hanadi ( MRCPI )
135.Dr Azher ( MRCPI )
134.Dr Noman Hossain
133.Dr Abhinav Meelu
132.Dr Nurul Islam
131.Dr kadhaum ibrahem
130.Dr Inayut
129.Dr Susovan Mitra
128.Dr Bhavesh Kaswala
127.Dr Rashid Ali Khan
126.Dr Bisma
125.Dr Samiah
124.Dr Madiha Mahmood
123.Dr Ratan Kumar
122.Dr Dilfuza Usmanova
121.Dr Mohd Hafiz
120.Dr Colin Cheah
119.Dr Kuan Yau Yeh
118.Dr Satesh Ramasundram
117.Dr Calvin
116.Dr Wan Mohamad
115.Dr Aravinthan Balakrishnan
114.Dr Athirah Azizol
113.Dr Massum
112.Dr Rafa Faaria Alam
111.Dr Benojeer Akter
110.Dr Sonal Karpe
109.Dr Shahla
108.Dr Muhammad Faizal
107.Dr Aisha Sohail
106.Dr Sheetal
105.Dr Anand Kumar
104.Dr Paul
103.Dr Ehsan Ul Haq
102.Dr Amna Gardezi
101.Dr Muhammad Rahib
100.Dr Shilpa
99.Dr Nagaraj Patil
98.Dr Vincent Jose ( MRCPI )
97.Dr Hana Abdalla Adam Mohamed ( MRCPI )
96.Dr Thanuja Alahakoon
95.Dr Farehah ( MRCPI )
94.Dr Sankar Nath Jha ( MRCPI )
93.Dr Saadia Khan
92.Dr Montasir Elmobark
91.Dr Kiran
90.Dr Ai Yun Loh
89.Dr Eow
88.Dr Lim
87.Dr Lalitha
86.Dr Ashwin Mathew
85.Dr Kasthuri
84.Dr Rohit
83.Dr Sangshaptak Saha
82.Dr Hira Jamil
81.Dr Santa Subhra Chatterjee
80.Dr Shishir
79.Dr Rubeya Ahmad
78.Dr Javaria Imran
77.Dr Rishi Gopalakrishnan
76.Dr Ramandeep Kaur
75.Dr Shakeel
74.Dr Shamla
73.Dr Murtaza
72.Dr Urvashi
71.Dr Urmimala Bhattacharjee
70.Dr Jayalakshmi
69.Dr Steffin Methai Kattor
68.Dr Yew
67.Dr Cyrin
66.Dr Farhat Nazneen
65.Dr Meenal
64.Dr Adil
63.Dr Umar Iftikhar
62.Dr Sohail ( MRCPI )
61.Dr Amarnath duraikannan
60.Dr Maha
59.Dr Samar
58.Dr Sidra German
57.Dr Mahmood Akhtar
56.Dr Muhammad Hashim
55.Dr Manmohan
54.Dr Pooja
53.Dr Haithem Alghebra ( MRCPI )
52.Dr Amna
51.Dr Nandhakumar
50.Dr Ew Ju Vern
49.Dr Mohamed Muslim
48.Dr Jerry John
47.Dr Majid Iqbal
46.Dr Phoebe
45.Dr Aimi N Zainudin
44.Dr Tahseen Azim
43.Dr Samina
42.Dr Suzi
41.Dr Samia
40.Dr Tan
39.Dr Kalpesh Kondalkar
38.Dr Sunil Abhishek
37.Dr Faiz Mashood ( MRCPI )
36.Dr Sharalaa Engatramana
35.Dr Prasad ( MRCPI )
34.Dr Kalyan Nath ( MRCPI )
33.Dr Reshma Thalikan
32.Dr Aneesa Shahul
31.Dr Arooj
30.Dr Esraa Soliman
29.Dr Amitave Chatterjee
28.Dr Malik Dilaver
27.Dr Ravi
26.Dr Priya
25.Dr Mujtaba Waris
24.Dr Shaheen Noman
23.Dr Apoorv Tiwari
22.Dr Niaz
21.Dr Janaki
20.Dr Lavanya Devi Palaniswamy
19.Dr Waqas
18.Dr Sadaf Hammad
17.Dr Osama Abdelaziz
16.Dr Rajeev Sharma
15.Dr Nehal Kunjomoidu
14.Dr Steffy
13.Dr Mustafizur Rahman (MRCPI)
12.Dr Vareeja Kasibian
11.Dr Niya Jamaludheen
10.Dr Farook Abdelgioum
9.Dr Kamran Ali
8.Dr Anik Rahman
7.Dr Manoj Dodiyah
6.Dr Madhusha
5.Dr Komal Zahid
4.Dr Hina Shaikh
3.Dr Sameer Abdus Samad
2.Dr Saurabh Gaba
1.Dr Rithik Mohan
2 523
*paceUrMRCP-Part 2 WRITTEN SUCCESS STORIES*
We are thankful to our respected coalleagues who have made us proud by their success in MRCP ( UK ) Part 2 WRITTEN
We believe that this number will keep on increasing
56.Dr Ayesha Kamran
55.Dr Sabiha Nusrat
54.Dr Ashif Istiak
53.Dr Kerolos Wagdy
52.Dr Ahmed mohamed
51.Dr Aqsa Khan
50.Dr Nabil
49.Dr Usman
48.Dr Hina Ali
47.Dr Abdul Wahab
46.Dr rabia islam abbasi
45.Dr Farina
44.Dr Ihsanullah
43.Dr Kunza tarar
42.Dr Jeevan Kumar
41.Dr Sowndhariya VA
40. Dr Hina Umar
39.Dr Berkas Khadidja
38.Dr Kiran
37.Dr Warda ( not in the group before )
36.Dr Shaista Qamar
35.Dr Nasir
34.Dr Ahmed Sayed Hamada
33.Dr Shafiq ul Islam
32.Dr Jawaria Shuja
31.Dr May
30.Dr Aliyah Abdalla
29.Dr Ashraf Jafrani
28.Dr Muhammad Sher Ali
27.Dr Mumtaz ahmad
26.25.Dr Yousaf
24..Dr Salman Afridi
23.Dr Zaheer
22.Dr Mohammad Sohail
21. Dr Raed Khan
20.Dr Maria Syed
19.Dr Divya
18.Dr Cindy Heaster
17.Dr Hira Aftab
16.Dr Sajjad Ali
15.Dr John Wesley
14.Dr Ehdaa Mohammed
13.Dr Khorshed Alam
12.Dr Mohammed Abu Noman
11.Dr Alashima Rabie
10.Dr Karmel Omer
9.Dr Ghena
8.Dr Muhammad Zaheer Ahmed
7.Dr Sumaiya
6.Dr Amer Mazher Sethi
5.Dr Ashiru Sikirat Yetunde
4.Dr Sadaf Fatima
3.Dr Inas Abdullah
2.Dr Mehwish Usman
1.Dr Najwan
2 523
*paceUrMRCP-Part 1 SUCCESS STORIES*
We are thankful to our respected coalleagues who have made us proud by their success in MRCP ( UK ) Part 1
We believe that this number will keep on increasing
53.Dr Stalin P John Benz
52.Dr MM Mohamed Sufad
51.Dr Aqsa Nizamani
50.Dr Kanta
49.Dr Munmun Nipa
48.Dr Suleman khan
47.Dr Sana Rafique
46.Dr Ali
45.Dr Izza
44.Dr Kerolos Wagdy
43.Dr Bushra
42.Dr Mubaraq Mustapha
41.Dr Bajrang Kumawat
40.Dr Iffat
39.Hotchand
38.Dr Banan Rasool
37.Dr Shilpi Shukla
36.Dr Usman
35.Dr Hasseeb
34.Dr Meena
33.Dr Ahmad
32. Dr Bushra Hossain
31.Dr.Mahwish Mustafa
30.Dr.Mehak Lakhani
29.Dr Nabil
28.Dr Zakia Zulfiqar
27.Dr Laxmikant Chavan ( MRCPI )
26.Dr Hussain Baloch
25.Dr Jeevan Kumar
24.Dr Muhammad Usman Majeed
23.Dr Muhammad Shoaib Niazi
22.Dr Ahmed Abdelakher
21.Dr Sowndhariya
20.Dr Fatema
19.Dr Asifa
18.Dr Shabbir Ahmed
17.Dr Kiran
16.Dr Cindy Heaster
15.Dr Harshini
14.Dr Shiasta Qamar
13.Dr Jay Dev
12.Dr Nasir
11.Dr Jamila Noor
10.Dr Aparajita Day
9.Dr Haleem Baksh
8.Dr Salman
7.Dr Rabia
6.Dr Manjunath
5.Dr Barkas Khadija
4.Dr Afsana
3.Dr Imran
2.Dr Anam Qadeer
1.Dr Joyce Phua
2 523
*Announcement for Online Session No 89*
*28 May 2023*
DEAR DOCTORS :
MAY I HAVE YOUR ATTENTION PLEASE :
*Tomorrow we will have an online session on Zoom discussing 2 station 5 ( BCC )* regarding our preparation for MRCP PACES ( UK )
TIMINGS :
Saudia Arabia: 4 00 pm
Pakistan : 6 00 pm
Bangladesh : 7 00 pm
India : 6 30 pm
Singapore : 9 00 pm
Hong Kong : 9 00 pm
Malaysia : 9 00 pm
Egypt : 4 00 pm
Libya : 3 00 pm
Bahrain : 4 00 pm
Burma ( Myanmar ) :7 30 pm
Sudan : 3 00 pm
UAE : 5 00 pm
UK : 2 00 pm
Ireland ( Dublin ) : 2 00 pm
Afghanistan : 5 30 pm
Kenya : 4 00 pm
Germany ( Berlin ) : 3 00 pm
Nigeria : 2 00 pm
Japan ( Tokyo ) : 10 00 pm
Denmark : 3 00 pm
Qatar : 4 00 pm
Oman : 5 00 pm
Italy : 3 00 pm
Indonesia : 8 00 pm
Mauritius : 5 00 pm
Iraq : 4 00 pm
Texas Usa : 8 00 am
Kuwait : 4 00 pm
( please Google for your local time zones to avoid any inconvenience )
Zoom meeting link will be shared 5 minutes before start time.
Interested candidate may send a personal message to take the case
GOOD LUCK.
2 523
*👉 IMPORTANT 673 👈*
*Some info about heart sounds*
The 2nd heart sound ( S2) Represents aortic ( A2 )and pulmonary valve ( P2) closure.
The most important abnormality of A2 is softening in aortic stenosis.
• A2 is said to be loud in tachycardia, hypertension, and transposition, but this is
probably not a useful clinical entity.
• P2 is loud in pulmonary hypertension and soft in pulmonary stenosis.
• Splitting of S2 in inspiration is normal and is mainly due to the variation of right heart venous return with respiration, delaying the pulmonary component.
• Wide splitting occurs in right bundle branch block (BBB), pulmonary stenosis, deep inspiration, mitral regurgitation, and VSD.
• Wide fixed splitting occurs in atrial septal defect (ASD).
• Reversed splitting (ie A2 following P2, with splitting increasing on expiration) occurs in left bundle branch block, aortic stenosis, PDA (patent ductus arteriosus), and right ventricular pacing.
• A single S2 occurs in Fallot’s tetralogy, severe aortic or pulmonary stenosis, pulmonary atresia, Eisenmenger’s syndrome, large VSD, or hypertension.
NB: splitting and P2 are heard best in the pulmonary area.
Good luck.
2 523
*👉 IMPORTANT 672 👈*
Please note that
Elderly patients with BPH might be taking alpha 1 blockers which may cause postural (orthostatic) hypotension, a common case of dizziness in elderly patients in exams.
examples (tamsulosin, prazocin)
Good Luck.
2 523
*👉 IMPORTANT 671 👈*
*Brief management summary for Ankylosing Spondylitis*
The following is partly based on the 2010 EULAR guidelines :
encourage regular exercise such as swimming
NSAIDs are the first-line treatment
physiotherapy
the disease-modifying drugs which are used to treat rheumatoid arthritis (such as sulphasalazine) are only really useful if there is peripheral joint involvement
the 2010 EULAR guidelines suggest: 'Anti-TNF therapy should be given to patients with persistently high disease activity despite conventional treatments'
research is ongoing to see whether anti-TNF therapies such as etanercept and adalimumab should be used earlier in the course of the disease
Good Luck
2 523
*👉 IMPORTANT 670 👈*
*Few Investigations for Ankylosing Spondylitis*
Inflammatory markers (ESR, CRP) are typically raised although normal levels do not exclude ankylosing spondylitis.
HLA-B27 is of little use in making the diagnosis as it is positive in:
90% of patients with ankylosing spondylitis
10% of normal patients
Plain x-ray of the sacroiliac joints is the most useful investigation in establishing the diagnosis. Radiographs may be normal early in disease, later changes include:
sacroiliitis: subchondral erosions, sclerosis
squaring of lumbar vertebrae
'bamboo spine' (late & uncommon)
syndesmophytes: due to ossification of outer fibers of annulus fibrosus
chest x-ray: apical fibrosis
If the x-ray is negative for sacroiliac joint involvement in ankylosing spondylitis but suspicion for AS remains high, the next step in the evaluation should be obtaining an MRI. Signs of early inflammation involving sacroiliac joints (bone marrow oedema) confirm the diagnosis of AS and prompt further treatment.
Spirometry may show a restrictive defect due to a combination of pulmonary fibrosis, kyphosis and ankylosis of the costovertebral joints.
Good Luck.
2 523
*👉 IMPORTANT 669 👈*
*Referral criteria for ankylosong spondylitis*
NICE advise:
all patients with suspected ankylosing spondylitis should be referred to a specialist
'Do not rule out the possibility that a person has spondyloarthritis solely on the presence or absence of any individual sign, symptom or test result.'
Good Luck
2 523
*👉 IMPORTANT 668 👈*
*Few clinical features of Ankylosing spondylitis*
*Introduction*
Ankylosing spondylitis is a HLA-B27 associated spondyloarthropathy. It typically presents in males (sex ratio 3:1) aged 20-30 years old.
*Clinical features*
*Features*
typically a young man who presents with lower back pain and stiffness of insidious onset
stiffness is usually worse in the morning and improves with exercise
the patient may experience pain at night which improves on getting up
*Clinical examination*
reduced lateral flexion
reduced forward flexion - Schober's test - a line is drawn 10 cm above and 5 cm below the back dimples (dimples of Venus). The distance between the two lines should increase by more than 5 cm when the patient bends as far forward as possible
reduced chest expansion
Other features - the 'A's
Apical fibrosis
Anterior uveitis
Aortic regurgitation
Achilles tendonitis
AV node block
Amyloidosis
and cauda equina syndrome
peripheral arthritis (25%, more common if female
Good Luck
2 523
*👉 IMPORTANT 667 👈*
*Few complications of ITP*
Complications of treatment are related to side effects of specific drugs used for treatment of ITP. A referral to local haematology department is desirable to weigh up the risks and benefits of choosing a particular modality of treatment against the risks of bleeding. I.e. if platelet counts are stable and above a certain acceptable threshold (depending on hospital guidelines, i.e. >50 and asymptomatic), it may be reasonable to continue monitoring.
Patients who received splenectomy require long term prophylactic penicillin V and pneumococcal/meningococcal vaccines.
Most patients with ITP do not have severe bleeding. In a review of adult ITP cases in Oklahoma over a 10 year period, 83% patients were managed on an outpatient bases. Indications for inpatient management of ITP include:
Large bleeding;
Haemodynamic compromise;
Intracranial haemorrhage;
Platelet count of less than < 30.
Inadequate response to conventional therapy agents.
Good Luck
2 523
*👉 IMPORTANT 666 👈*
*Some treatment options for ITP*
ITP at first presentation should be referred to and managed by haematologists.
The requirement for treatment varies between patient to patient; as such, clinical status is a key determinant for these considerations - i.e. asymptomatic, bleeding or planned surgical/dental procedures.
Treatment is only given to those patients that absolutely require it, hence decreasing the risks of adverse effects such as infection as a result of immunosuppression. Below are the recommendations as according to British society of haematology.
First line treatment for ITP is oral prednisone at 1mg/kg daily with proton pump inhibitors . This is given over a period of 2 - 4 weeks and weaned off a few weeks after. Most patients respond to this treatment within a week of commencing steroids.
Pooled normal human immunoglobulin (IVIG) is also listed as first line treatment. Intravenous immunoglobulin is administered at 1g/kg. The mechanism of action is unknown but it was thought that one way is by blocking the Fc receptor of macrophages.
Splenectomy had been used for many years, long before steroids were used. It is now second line for ITP in steroid refractory cases. It works by avoiding platelet destruction by removing the spleen.
Other immunomodulatory drugs such as rituximab, cyclophosphamide and dapsone have also been used to treat ITP. Romiplostim works by activating the thrombopoietin receptor and stimulating JAK2, thus it stimulates platelet production. It has been approved by NICE as an option for ITP. Indications for usage include:
ITP is refractory to standard active treatments and rescue therapies or
Patients have severe disease and a high risk of bleeding that needs frequent courses of rescue therapies.
Additionally it is important to avoid drugs which make bleeding worse. It is important to avoid antiplatelet drugs such as aspirin and clopidogrel.
In cases of severe bleeding, it is important to treat promptly with transfusion of platelets, IVIG, tranexamic acids and initiate major haemorrhage protocol. Although transfusion of platelets may not improve platelet count, it has been shown to be effective at relieving the symptoms in acutely severe bleeding.
Good Luck
2 523
👉 IMPORTANT 665 👈
*Some investigations for ITP*
There are a number of investigations to be considered in patients presenting with bleeding and in those with incidental findings of thrombocytopenia. There is no single blood marker for ITP. Rather it is a diagnosis of exclusion. Minimum investigations to be done if thrombocytopenia is found include:
Firstly, full blood count and blood film need to be requested. This would demonstrate isolated decrease in platelet counts, with normal counts in all other cell lineages. Additionally, there should be no evidence of fragments on the film.
Secondly, a virology screen including HIV, EBV, hepatitis screen.
Further investigations to be considered, as guided by history and examination findings:
Clotting screen including PT and APTT, especially in those with severe bleeding.
Thyroid function tests
Malarial screen
Myeloma screen.
Immunological tests including ANA is considered especially if coexisting rheumatological features are present.
Imaging including CT may be useful if there is a high index of suspicion for cancer.
Bone marrow biopsy is no longer a standard investigation for ITP. If there are blood count abnormalities such as anaemia, leucopenia or other unexplained haematological findings, a bone marrow biopsy is warranted. In cases where ITP is not responsive to treatment and there is a high clinical suspicion for MDS, bone marrow biopsy should be carried out.
Good Luck
2 523
👉 IMPORTANT 664 👈
Few differential diagnosis for ITP
ITP is a diagnosis of exclusion. Thrombocytopenia can be caused by increased destruction of platelets, and/or reduced production of platelets.
Important differential diagnoses to consider include:
Non-immunological causes of increased destruction of platelets include disseminated intravascular coagulation (DIC) i.e. in the setting of sepsis or malignancy.
Pregnancy and its complications such as HELLP syndrome can also cause thrombocytopenia.
Chronic liver disease and hypersplenism is associated with thrombocytopenia.
Thrombotic thrombocytopenic purpura (TTP) is life-threatening disease which presents with thrombocytopenia but can result in multi-organ failure, cardiac complications, strokes and other thrombotic events. The hallmark for DIC and TTP is the presence of fragments on the blood film.
Additionally, drugs such as heparin may result in thrombocytopenia, known as heparin-induced thrombocytopenia or HIT.
Immunomodulatory drugs such as gold, alemtuzumab and more recently immunotherapy agents such as nivolumab and pembrolizumab have been associated with ITP.
Thrombocytopenia may be the first sign in well patients with underlying viral infections such as HIV or hepatitis.
Many haematological malignancies can result in thrombocytopenia such as leukaemia, lymphoma, myelofibrosis, myelodysplasia and myeloma. Therefore it is important to take a careful history, as patients with these diseases often present with constitutional symptoms.
Finally, rheumatological diseases such as SLE and rheumatoid arthritis can present with thrombocytopenia.
Good Luck
2 523
👉 *IMPORTANT 663* 👈
*Some info about clinical presentation of idiopathic thrombocytopenic purpara ( ITP )*
Approximately 1/3 of patients are asymptomatic and have incidental discovery on blood test.
Approximately 2/3 of patients have bleeding. Commonly patients with ITP present to their doctors with petechiae , small red dots on the skin. Purpura , formed by petechiae joined together, can also occur.
Mild epistaxis is common. Continuous epistaxis requiring nasal packing or cauterisation may pose greater risks of bleeding.
In women, patients with ITP may have prolonged and heavy menstrual cycles.
Very rarely, nonetheless the most importantly, ITP can present with intracranial bleeding; this occurs in 1.4% of the cases.
Severe non-intracranial bleeds such as large gastrointestinal bleed occur in 9.6% of the cases.
Patients with ITP can present as generally unwell, i.e. feeling lethargic.
Occasionally, patients with ITP may present with strokes and TIA, often referred to as paradoxical thrombotic events in ITP.
Good Luck
2 523
👉 *IMPORTANT 662* 👈
*Some info about pathophysiology of idiopathic thrombocytopenic purpara ( ITP )*
ITP is an autoimmune disorder. In ITP abnormal immune system leads to destruction of own platelets . Although the precise mechanism for ITP is not completely understood, there have been several widely accepted theories:
In ITP, autoantibodies are produced by the patient's B cells, principally of IgG. These target against platelet membrane glycoproteins GPIIb/IIIa.
These platelets with autoantibodies are then engulfed by macrophages and degraded in the spleen.
The bone marrow compensates by producing megakaryocytes (precursor to platelets).
Purpura occurs as a result of increased permeability in capillary due to low platelets.
In some cases, it is thought that viral infections can precede development of ITP. Antibodies against viral antigens cross react with normal antigens on platelet surfaces thus producing molecular mimicry.
Good Luck
2 523
👉 *IMPORTANT 661* 👈
*Some info about aetiology of idiopathic thrombocytopenic purpara ( ITP )*
It is thought that ITP is an autoimmune disorder resulting in antibodies produced to target against individual’s own platelets, leading to thrombocytopenia.
This in turn results in petechiae and in rarer cases more severe bleeding.
Furthermore, ITP can be primary or secondary. Primary ITP occurs when there is isolated thrombocytopenia is found with no co-existing conditions. Secondary ITP is associated with co-existing conditions. These include:
Rheumatological diseases
CLL
Lymphoma
Viral infections
Various pharmacological agents
Good Luck
2 523
👉 *IMPORTANT 660* 👈
*Important points in the management of sarcoidosis*
*Indications for steroids*
patients with chest x-ray stage 2 or 3 disease who have moderate to severe or progressive symptoms. Patients with asymptomatic and stable stage 2 or 3 disease who have only mildly abnormal lung function do not require treatment
hypercalcaemia
eye, heart or neuro involvement
Prognosis
*Factors associated with poor prognosis*
insidious onset, symptoms > 6 months
absence of erythema nodosum
extrapulmonary manifestations: e.g. lupus pernio, splenomegaly
CXR: stage III-IV features
black people
Good Luck
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