Hello!
Number needed to treat = 1 / Absolute risk reduction
Mnemonic: TARR - Treat Absolute Risk Reduction
Number needed to harm = 1 / Attributable risk
Mnemonic: HARM - Harm Attributable Risk M
That's all
-IkaN
Sunday, April 23, 2017
The Basics : Lateral wall of Nasal cavity
Hey Awesomites
In this post, I will be talking about the anatomical structures in the lateral wall of the nasal cavity.
Saturday, April 22, 2017
Clubbing : Why it occurs.
Hi everyone !
This is a short post on why clubbing happens.
So it's simple !
It's cause people like to go out and get drunk.
Just kidding. Here goes.
This is a short post on why clubbing happens.
So it's simple !
It's cause people like to go out and get drunk.
Just kidding. Here goes.
1. What is clubbing ?
- It's the bulbous enlargement of the terminal digits and the nail bed.
- It's the bulbous enlargement of the terminal digits and the nail bed.
2. What are its causes ?
- Symmetrical clubbing can occur due to a host of causes.
- To summarize :
A. Respiratory
: Lung cancer
: Suppurative lung conditions like
- Symmetrical clubbing can occur due to a host of causes.
- To summarize :
A. Respiratory
: Lung cancer
: Suppurative lung conditions like
Bronchiectasis , lung abscess and Chronic TB.
: Pulmonary Fibrosis
B. Cardiac
- Cyanotic heart disease
- Eisenmenger Syndrome
- Infective endocarditis
: Pulmonary Fibrosis
B. Cardiac
- Cyanotic heart disease
- Eisenmenger Syndrome
- Infective endocarditis
C. GIT
- Inflammatory bowel disease
- Cirrhosis - esp Biliary
D. Endocrine
- Thyroid Acropachy
- Acromegaly
- Inflammatory bowel disease
- Cirrhosis - esp Biliary
D. Endocrine
- Thyroid Acropachy
- Acromegaly
3. Why does it occur
So I've spent a lot of time researching theories on how clubbing occurs. And let me tell you in the start itself, they're not clear on why it occurs.
But what makes sense to me , I want to share with you'll! And it was an absolute pain to find something convincing enough. So just stick with me here ;;)
But what makes sense to me , I want to share with you'll! And it was an absolute pain to find something convincing enough. So just stick with me here ;;)
So the crux of clubbing lies in vasodilation of the digital vessels causing proliferation of the tissue there in.
The most widely accepted theory right now is the megakaryocyte theory.
The most widely accepted theory right now is the megakaryocyte theory.
So in the figure above , the left side in white shows the normal course of a megakaryocyte through the blood.
In altered cardiorespiratory conditions , these large platelets either bypass the Pulmonary circulation owing to the shunting produced due to Heart defects or the lung parenchyma itself proves to be less to purify the blood of the platelets.
This causes these giant platelets to go lodge into the digital circulation causing release of cytokines like Platelet derived growth factor (PDGF) and TGF beta amongst others. These GF's cause vasodilation and in return , nail bed proliferation and collagen deposition.
IBD - especially Crohn disease seen to have thrombocytosis eventually which may aggravate the PDGF.
In cirrhosis of liver , especially biliary , pulmonary arteriovenous shunting is observed. This could result in the megakaryocyte entrapment as explained.
Another theory suggests inflammation triggers a vagal response causing Vasodilator effects. ( Neurogenic).
Other theories -
Hypoxia induced
Reduced ferritin related
Neurogenic
Humoral - various PG's and other humoral molecules.
The most widely accepted theory is the Megakaryocyte theory.
Hope this satisfied you !
Thank you.
Stay awesome.
~A.P.Burkholderia
Preparing for NEET - Part 2
Hello everyone.
So now for my part 2 post on NEET PG prep, I will provide
you with a seventh month schedule, but before that let’s talk about the pros and cons of joining
classes and how to deal with studies if you don’t join one.
Now in my earlier post I did mention that classes will help
YOU with only 20% of the entire prep that also with sustained proper attention
in the 12 hour class with proper notes and revision.
1. The biggest thing you achieve by attending class
is that the professors don’t beat around the bush, they give you point to point
details and explain the things which they know by experience that
the students are bound to screw up the most.
This is not something you can’t achieve by
your own. If you can get your hand on any
class notes, then that’s enough, just thoroughly read that book, be regular in
solving mcq’s and discuss your issues in group chats or with your study
buddies. This does take care of it plus you gain a lot more, because here you
are actively seeking answers and not being spoon fed like in classes
If you don’t have any class notes and our
reading standard books, I suggest only read the bold lines, don’t read anything
else. If you clearly don’t know anything about a particular topic then only
read it in depth.
2. Weekly test series and grand test with ranking. This
is beneficial only if you stick to the schedule, sadly I feel only 3 out of 10
students are regular at these exams. Also even if you don’t join the regular
course, you can just join the test series, which I feel is a great option .
The bad point is that sometimes students
feel torn between their own study speed, the subjects they want to study
first and the test series schedule. Sometimes the test series just overwhelms you a lot cause every week you need
to prepare for a different subject. This
has happened to me, and I feel that if I hadn’t join the test series to begin
with, maybe I wouldn’t have been so
confused as to whether what to study and what to revise.
So it’s
very important that you all know your own study patterns and your comfort. Don’t
do things just because everyone else is doing it. Chart down your schedule, and once you start
with it, stick to it. Don’t listen to people and try doing things their way,
you are your own person and you are awesome.
NOW for the study schedule. This way of prep is bold and ridiculous. Its exhausting
and It will demand that you trust the process, but it will work. It was taught
to me by one of my friend. Its esp for the ones who haven’t joined any classes.
·
This first phase is for you to grab onto all the
possible books on mcq’s you can for the last ten year mcq’s. And then you go crazy,
just solve the mcq. Don’t read the
explanations. Just solve and solve, just
reading the answers. Thats it. This whole process should take you a
month at the max of rigorous solving.
·
Take a break..chill out for a couple of days
·
Phase two. repeat the phase one, now I have tried this. And by experience I will
tell you this is when it gets tough, monotonous and downright stupid but keep
going at it. This will take you two months max.
·
Breaktime
·
Phase three is when you repeat it all over
again, but now you will see the difference. You will love solving cause now the
answers will flow out of you. Cause you have just learned 30.000 important one
liners of all the 20 subjects. This process will take you 20 days.
·
Phase four is when you read and solve your
doubts, read any damn book you want. Search for pictures, make your own picture
library.
Remember 75% mcq are repeats, so this plan is made in a way that you
learn all of those 75% first
You need to solve atleast all the mcq a minimum of five times to score a
decent rank
Your speed of solving should reach 300 questions in one hour with atleast
65- 70% right.
These above are your goals after you are done with phase four
Irrespective you choose to follow this plan or any of the tips in my part
1 post, or if you choose to modify it according to you. Remember the most important thing is
that you have to be consistent and do smart studies and not study like a dog. Have
your wits about yourself and don’t waste
your time on reading unnecessary details.
Thank you
Sakkan
Authors' diary: Homemade cheap DIY alternatives for a smartphone camera stand
This video is from the authors diary!
In this video, I show how I keep my camera stable while shooting videos of my notes / whiteboard.
I use paper cups and books as my camera stand.
In this video, I show how I keep my camera stable while shooting videos of my notes / whiteboard.
I use paper cups and books as my camera stand.
Friday, April 21, 2017
Paraneoplastic Dermatoses - Tripe Palm.
Hello everybody,
So from today onwards, I will cover a series of cutaneous manifestations of internal malignancies starting with the first one called Tripe Palm.
(Image courtesy-Google)
(The palmar ridges are accentuated and resemble to the stomach mucosa of a ruminant-tripe.)
(The palmar ridges are accentuated and resemble to the stomach mucosa of a ruminant-tripe.)
Tripe palm (also known as acanthosis palmaris and acquired pachydermatoglyphia) is a velvety thickening of the palms with a ridged or rugose appearance.
The term is derived from its resemblance to the stomach mucosa of ruminants (tripe).
It is associated with gastric or lung cancer.
In some cases, tripe palm is the initial presenting feature of the underlying malignancy.
Improvement of tripe palm occurrs in one-third of patients after beginning treatment for malignancy.
Hope it was helpful.
Let's learn Together!
-Medha.
-Medha.
Nail Changes in Medicine : A Summary
Hi everyone. Just a list of changes you can see in the nails in different systemic Diseases. So let's get nailed ;)
1. Clubbing -
Loss of angle between the nail and the nail fold - More soft and bulbous nail.
Typically indicates Cardio Pulmonary function disturbance :
--> Cardiac conditions like Cyanotic heart disease, Infective endocarditis and Atrial myxoma.
--> Respiratory conditions :
Neoplastic like CA lung ( Esp. Squamous cell CA) , Mesothelioma.
Infective like Bronchiectasis , Abscess , Empyema.
(Non cardiorespiratory causes = Inflammatory bowel disease, Biliary Cirrhois.
Thyroid Acropachy , Acromegaly. )
2. Koilonychia -
Spoon shaped nails.
Strongly indicative of Iron Deficiency anemia or Fungal nail infection.
3. Onycholysis -
Destruction of nail.
Seen in Psoriasis , Hyperthyroid and Fungal nail infection.
4. Chronic Paronychia -
Inflammation of nail fold. May have swollen nail and discharge with throbbing pain. May occur due to frequent nail biting.
5. Cyanosis -
Can be looked for in nail bed. We have a post on this already.
6. Beau line -
Transverse furrows from temporary arrest of nail growth due to increased stress.
Nails grow at 0.1 mm/d , so furrow distance from the cuticle can be used to time the attack. Can be seen in Malaria , Typhus , Rheumatic fever , Kawasaki.
7. Mees line -
White transverse bands in Arsenic poisoning / Renal failure.
8. Muerhcke's line -
White parallel lines without furrowing on the nail.
Seen in Hypoalbuminemia.
9. Terry's nails -
Proximal portion of nail is white / pink , tip is reddish brown.
Seen in cirrhosis , CRF
10. Splinter hemorrhage -
Longitudinal Hemorrhage streaks under the nail seen in Infective endocarditis.
What a fun way to get nailed down 😂 Happy studying !
Stay awesome.
~ A.P.Burkholderia.
Drug Induced Edema : Mnemonic
Hi everyone. Here's a short post highlighting drugs causing edema.
Remember : SWOLLEN
S - Steroids
W (V) - Vasodilator drugs
O - Oral Hypoglycemic drug - Glitazones
L - CycLosporine
L
E - Endocrine - Growth Hormone
N - NSAIDs
1. Steroids -
Due to the Mineralocorticoid action of reabsorbing the Sodium from the kidneys, they act as volume expanders.
2. Vasodilator drugs -
Especially CCB's like Amlodipine are known to cause this. Other Vasodilator drugs used for hypertension can also cause edema like Alpha Methyl dopa, Hydralazine, etc
3. Oral Hypoglycemic drug : Glitazones -
The Glitazones act on the PPAR gamma receptors. These receptors are also present in the kidneys and vascular system. They somehow modulate the kidneys to reabsorb Na+ and also act on the level of blood vessels via PPAR receptors.
This is one of the reasons why they are c/i in Heart failure and Liver cirrhosis ( as they cause fluid overload).
4. Cyclosporine -
Reduces the GFR , thus more fluid retention.
5. Growth hormone. I don't understand why. Do tell me if you find out !
6. NSAIDs -
NSAIDs inhibit PG synthesis in kidneys causing renal vasoconstriction and this reducing the GFR.
This causes excess fluid accumulation eventually causing edema.
That's all!
Happy studying. Stay awesome. :)
~ A.P.Burkholderia
Adult ADHD : A Clinical Overview
Hey Awesomites
Attention - Deficit Hyperactivity Disorder ( ADHD ) is a mental health disorder that usually occurs in childhood and continues into adulthood. The symptoms in adults may not be as clear as in children. In India, there are more than 10 million cases of adult ADHD per year.
In adults, the symptoms of hyperactivity may decrease, but the characteristic features of decreased attention span, mood swings, impulsive behavior, difficulty in communication and language skills, restlessness may still continue to appear.
Now lets talk about the signs. The WHO has lately released a set of six questions to test the adults for signs of ADHD - Adult Self - Report Scale Screener (ASRS) is a self - screening questionnaire that you can use to determine if you might have ADHD. The answers to these questions predict the people suffering from this disorder and is a simple way of screening :
1. How often do you have difficulty in concentrating on what the other person is saying to you, directly as well as indirectly ?
2. How often do you leave your seat when you are in a group or meetings in which you are expected to remain seated?
3. How often do you have difficulty in unwinding and relaxing when you have time to yourself ?
4. When you are in a conversation, how often do you find yourself finishing sentences of the people you are talking to before they can finish them themselves?
5. How often do you put things off until the last minute?
6. How often do you depend on others to keep your life in order and attend to details?
- The answers to these set of questions can be 'never', 'rarely', 'sometimes', 'often', or 'very often'.
- If the answer to four of the six questions is 'sometimes', 'often' or 'very often' , the person may be considered to have ADHD!
Note that this is a simple way of screening the people for signs of ADHD, and not the diagnostic criteria.
Thats all
- Jaskunwar Singh
Attention - Deficit Hyperactivity Disorder ( ADHD ) is a mental health disorder that usually occurs in childhood and continues into adulthood. The symptoms in adults may not be as clear as in children. In India, there are more than 10 million cases of adult ADHD per year.
In adults, the symptoms of hyperactivity may decrease, but the characteristic features of decreased attention span, mood swings, impulsive behavior, difficulty in communication and language skills, restlessness may still continue to appear.
Now lets talk about the signs. The WHO has lately released a set of six questions to test the adults for signs of ADHD - Adult Self - Report Scale Screener (ASRS) is a self - screening questionnaire that you can use to determine if you might have ADHD. The answers to these questions predict the people suffering from this disorder and is a simple way of screening :
1. How often do you have difficulty in concentrating on what the other person is saying to you, directly as well as indirectly ?
2. How often do you leave your seat when you are in a group or meetings in which you are expected to remain seated?
3. How often do you have difficulty in unwinding and relaxing when you have time to yourself ?
4. When you are in a conversation, how often do you find yourself finishing sentences of the people you are talking to before they can finish them themselves?
5. How often do you put things off until the last minute?
6. How often do you depend on others to keep your life in order and attend to details?
- The answers to these set of questions can be 'never', 'rarely', 'sometimes', 'often', or 'very often'.
- If the answer to four of the six questions is 'sometimes', 'often' or 'very often' , the person may be considered to have ADHD!
Note that this is a simple way of screening the people for signs of ADHD, and not the diagnostic criteria.
Thats all
- Jaskunwar Singh
Thursday, April 20, 2017
Croup mnemonic
If croup crops up in the exam, here are some high yield points you should know:
Croup CROPS!
Corticosteroids
Racemic epinephrine
Oxygen
Parainfluenza virus
Seal barking cough
Stridor
Subglottic stenosis
Steeple sign
#TLDR
Parainfluenza virus type 1 is the most common cause of croup.
The onset of symptoms in laryngotracheitis is gradual, beginning with nasal irritation, congestion, and coryza. Fever, hoarseness, barking cough, and stridor usually develop during the next 12 to 48 hours.
In children with croup, a posterior-anterior chest radiograph demonstrates subglottic narrowing, commonly called the "steeple sign"
Children with croup are treated with dexamethasone, nebulized epinephrine and humidified oxygen depending on severity.
Remember, intubation is rarely required in croup, so think of other etiologies if the patient needs intubation.
That's all!
-IkaN
Edge of an ulcer : An overview
Hello
An overview on how edge of an ulcer appears with characteristic identification features depending on the underlying causes: (SPURE)
Sloping edge - Venous ulcer, also seen in traumatic cases. It is red - purplish in color and consists of new healing epithelium. ( spreading type )
Punched out edge - Arterial and Neuropathic ulcer. Edges are punched out at right angles. ( non spreading type )
Undermined edge - Decubitus and Tuberculous ulcer. It spreads rapidly to destroy the surrounding tissue !!
Rolling back - Basal cell Ca. It is characterised by raised, pearly white beaded edge with central necrotic tissue.
Everted edge - Squamous cell Ca. It is a rapidly growing invasive ulcer with heaped up and everted edges.
Thats all
Hope this helps :)
- Jaskunwar Singh
An overview on how edge of an ulcer appears with characteristic identification features depending on the underlying causes: (SPURE)
Sloping edge - Venous ulcer, also seen in traumatic cases. It is red - purplish in color and consists of new healing epithelium. ( spreading type )
Punched out edge - Arterial and Neuropathic ulcer. Edges are punched out at right angles. ( non spreading type )
Undermined edge - Decubitus and Tuberculous ulcer. It spreads rapidly to destroy the surrounding tissue !!
Rolling back - Basal cell Ca. It is characterised by raised, pearly white beaded edge with central necrotic tissue.
Everted edge - Squamous cell Ca. It is a rapidly growing invasive ulcer with heaped up and everted edges.
Thats all
Hope this helps :)
- Jaskunwar Singh
Submission: Direction of growing end of bone, opposite to direction of nutrient artery
submitted by: Mayank Kesharwani
Upper limb joints types mnemonic
Hey Awesomites
From proximal to distal, the joints and its types are:
Shoulder joint - Ball and socket type
Elbow joint - Hinge joint
Radio carpal ( wrist ) joint - Ellipsoidal and biaxial type
Carpo metacarpal joint - Saddle joint
Metacarpo phalyngeal joint - Ellipsoidal ( condylar ) joint
Interphalyngeal joint - Hinge joint
Mnemonic to remember the types, from proximal to distal : BaSu ( Ball and Socket ) writes Hindi ( hinge ) in elliptics ( Ellipsoidal ) but is sadly (Saddle ) condemned ( Condylar ) without hinges .
Thats all
- Jaskunwar Singh
Submission ( notes and mnemonic ) by Mayank Kesharwani - ( PS: This is a Hindi Urdu mnemonic )
Bhaiya Hum ESE Hain
Bhaiya - Ball and Socket joint
Hum - Hinge joint
E - Ellipsoidal
S - Saddle
E - Ellipsoidal
Hain - Hinge
Thanks Mayank for sharing :)
From proximal to distal, the joints and its types are:
Shoulder joint - Ball and socket type
Elbow joint - Hinge joint
Radio carpal ( wrist ) joint - Ellipsoidal and biaxial type
Carpo metacarpal joint - Saddle joint
Metacarpo phalyngeal joint - Ellipsoidal ( condylar ) joint
Interphalyngeal joint - Hinge joint
Mnemonic to remember the types, from proximal to distal : BaSu ( Ball and Socket ) writes Hindi ( hinge ) in elliptics ( Ellipsoidal ) but is sadly (Saddle ) condemned ( Condylar ) without hinges .
Thats all
- Jaskunwar Singh
Submission ( notes and mnemonic ) by Mayank Kesharwani - ( PS: This is a Hindi Urdu mnemonic )
Bhaiya Hum ESE Hain
Bhaiya - Ball and Socket joint
Hum - Hinge joint
E - Ellipsoidal
S - Saddle
E - Ellipsoidal
Hain - Hinge
Thanks Mayank for sharing :)
Submissions : Tonsillar Bed mnemonic
Hello
Tonsillar bed mnemonic ( from within outwards ) :
P(b) S S B(p)
Tonsillar bed mnemonic ( from within outwards ) :
P(b) S S B(p)
Pharyngo Basilar fascia
Superior constrictor
Styloglossus
Bucco pharngeal fascia
Superior constrictor
Styloglossus
Bucco pharngeal fascia
- Submitted by Mayank Kesharwani
Submissions : Important vertebral levels
Hello
Important vertebral levels for bifurcations:
- Common carotid artery bifurcation - C4 vertebra
- Tracheal bifurcation - T4 ( may ascend or descend upto two vertebrae higher or lower with breathing )
- Abdominal Aorta bifurcation - L4
Important vertebral levels for formations:
- Cricoid cartilage- C5- C6
- Thoracic duct crosses right to left - T5 ( and enters left IJV )
- Inferior Vena Cava formation - L5 ( from two common iliac veins )
Submitted by Mayank Kesharwani
Important vertebral levels for bifurcations:
- Common carotid artery bifurcation - C4 vertebra
- Tracheal bifurcation - T4 ( may ascend or descend upto two vertebrae higher or lower with breathing )
- Abdominal Aorta bifurcation - L4
Important vertebral levels for formations:
- Cricoid cartilage- C5- C6
- Thoracic duct crosses right to left - T5 ( and enters left IJV )
- Inferior Vena Cava formation - L5 ( from two common iliac veins )
Submitted by Mayank Kesharwani
Submissions: Rolando fracture mnemonic
Hello
TATA truck ROLLS on wheels
The shape of this fracrure is T- shaped or Y ( bent- T ) shaped, which resembles the sign of the Tata motors truck, and Roll is for "Rolando fracture"
Mnemonic submitted by Mayank Kesharwani
Diagram by Jaskunwar Singh
Bartonella henselae and Pasteurella multocida infection mnemonic
Hello!
Sometimes I confuse the clinical manifestations of these two cat related diseases - Cat scratch disease caused by Bartonella henselae and Pasteurella multocida infection caused by cat bites.
I probably wouldn't have confused these two in my step 1 days, but the older you get, the more confusing rare diseases become,
Sooo... Mnemonic!
Sometimes I confuse the clinical manifestations of these two cat related diseases - Cat scratch disease caused by Bartonella henselae and Pasteurella multocida infection caused by cat bites.
I probably wouldn't have confused these two in my step 1 days, but the older you get, the more confusing rare diseases become,
Sooo... Mnemonic!
Preparing for NEET: Part 1
Hello folks,
This is a common post requested as to how to prepare for NEET PG exams.
And as to whether joining classes is really required to get a decent rank.
So today I will share with you a study schedule told to me by my professor. Which takes around 7 month hardcore prep.
Now for a general approach to it
1. Classes are not essential. Classes add only 20% to the entire PG prep of yours.. That's with like max optimum attention and taking down notes vigorously.
2. Don't read standard books. The competition is so high, that the publishers end up increasing the number of pages. Just to make the book more appealing. Reading those books is a waste of your time cause they repeat the explanations over and over again with unnecessary details which will make you take a month atleast to finish a subject like obstetrics.
The only decent book I found was modit khanna for medicine, like the initial pages of high yield notes and the questions and not the explanations. Don't read the explanations unless the answer is not known to you through the high yeild section.
3. Try getting your hands on class notes. Be it DAMS, Bhatia or IAMS. They are all amazing and to the point. And that's what is needed.
4. Get the NEET PG question booklet, by Arvind Arora. A minimum of last five years questions of NEET is a must to solve.
5. Never sit with a pen and a paper or a marker during your first read for any subject. You will end up marking the whole book and write unnecessary notes and wasting a lot of precious time. Save it for your second and third read or when you are confident enough that you know the flow of the subject and now just need to focus on details.
6. While reading if you have any doubts make a point to jot it down and find answers before sleeping or at the end of the week. But do solve them. Cause at the end just before exams these are the doubts that trouble you the most.
7. You need to score only a 75% aggregate to score a decent rank. Like to be in the top 3000. That is very much possible with a 7 month smart prep. For the the fight in between the top 3000 see the next para
8. Imagine yourself after a 24hr emergency duty, back to back and just next day you have to write theory paper of your uni exam.That's a near about situation of how mind stressed you are before neet.
Like it's 20 subjects..and you need to shift your focus from ophthalmology to psm in a matter of seconds. If you can't do that and if you waste your time even like an extra 5 mins on one question then you will be compromising the tail questions and that's when the stress gets to you. You keep looking at the timer and boom you black out.
A solution to this is you need to train your brain to deal with this situation. I have an aggregate of tips from medicowesome authors to deal with this.
- Solve the grand test. Just don't stick to one subject solving be as varied as possible. Like your best shot is solving 100 random questions every day doesn't matter if you know only 5subjects out of the 20, you only need to train your brain to deal with it.
- Solve the questions after an on call or after a very stressful day, give yourself the taste of it. So that your brain will be able to switch attentions during exams.
I feel the battle between the top 3000 rankers all comes down to who switched their attention between questions the fastest. The knowledge is the same it all matters that whether you were able to use it to your best or not.
9. Follow medicowesome :D
A bit cheeky but seriously it helps. Every now and then try reading the various posts. It will help you to condition your brain to all the subjects piece by piece.
10. A lot of questions are photo based. Try making your own picture library like jot down the things of pics you want to search for and look for it at the end of the day or the week end.
11. We don't promote apps and stuff but I would seriously advice downloading the pg prep app from Google play. It has stats to show your progress, daily exams, a 55 thousand question bank, photo questions, subject wise and grand test questions. It is amazing. Go ahead download it if you haven't and stick to it.
12. Have a way to destress yourself during the prep. Like be it running , movie, at a cafe or a novel.
Pg prep is a monotonous dumb thing to do , let's not lie to our selves -_-
You need to keep your engine at a steady pace so that you are able to fast track during the last month before your exam.
Like I personally read manga :D
Weekly updates were my solace and paradise. That's the way I treated myself after I had completed my schedule for the week.
I will upload a seven month prep schedule in part 2.
- Sakkan
Wednesday, April 19, 2017
Myopic Shift : Explanation
Hi everyone ! So this is a short post on the Second Sight or the Myopic Shift seen in Cataract.
So in people who have a hypermetropic / presbyopic power , tend to experience a reduction in their refractive errors when Cataract starts to develop. This is called Myopic Shift or Second sight.
This occurs most commonly in nuclear cataracts. Now why this occurs is , the lens in early stages of Cataract undergoes sclerosis. That increases the Power of the lens ( this increases the refractive index).
Thus it makes the lens slightly more Powerful , or Convex. Due to this it acts as a correction for Hyperopia/ Presbyopia (Where the error was due to a weaker lens. )
This transient Myopic nature of the eye is called the Myopic Shift.
It does go away when the Cataract progresses as the sclerosis begins to reduce refractive surface in the lens.
Hope this helped! Stay awesome !
Happy Studying :)
~ A.P.Burkholderia
Infants of Diabetic Mothers (IDM) : A clinical overview
Hello
With the prevalence of insulin - dependent diabetes mellitus and maternal hyperglycemia, serious consequences to the ingrowing foetus may occur during its organogenesis. Lets have a quick review of the clinical problems in the infants of diabetic mothers ( IDM ) with some lame mnemonics :p -
GENERAL BUILT :
- Macrosomia ( birth weight >4,000 gm ) resulting in difficult labor and complications such as traumatic asphyxia, shoulder dystocia, BP injury, etc.
- Large for gestational age
CONGENITAL ANOMALIES :-
1. CARDIOVASCULAR - mnemonic : CASTeD
- Cyanotic heart disease
- Asymmetric septal hypertrophy ( resulating in small LV )
- Septal defects ( VSD, ASD )
- Transposition of blood vessels
- Decreased cardiac output ( due to perinatal asphyxia and metabolic acidosis )
- Cyanotic heart disease
- Asymmetric septal hypertrophy ( resulating in small LV )
- Septal defects ( VSD, ASD )
- Transposition of blood vessels
- Decreased cardiac output ( due to perinatal asphyxia and metabolic acidosis )
2. SKELETAL AND CNS -
- Caudal regression syndrome
- Mental retardation
- Caudal regression syndrome
- Mental retardation
3. NEURAL TUBE DEFECTS - mnemonic : HAM
- Holoprosencephaly
- Anencephaly
- Meningomyelocoele
4. RENAL and GENITOURINARY - mnemonic : HURT
- Hydronephrosis
- Urethral dysplasia
- Renal agenesis
- Thrombosis of renal vein
( patient presents with flank mass, intermittent hematuria, and thrombocytopenia )
5. GASTROINTESTINAL - mnemonic : GAS
- Gastrointestinal obstruction ( due to duodenal atresia )
- Anorectal malformations
- Small left colon syndrome
7. METABOLIC changes -
- Hyperbilirubinemia ( due to polycythemia )
- Hypoglycemia occurs 30 - 90 mins post delivery which may take several days to resolve. Rebound hypoglycemia may occur in response to rapid, large boluses of glucose ( 10-15 mg/kg/min ).
- Hypocalcemia ( levels <7 mg/dL ) occurs within hours to days after birth due to a delay in PTH synthesis after birth, often accompanied with Hypomagnesemia.
Thats all
Hope this helps :)
- Jaskunwar Singh
Mnemonico diagnostico : Risk approach to Antenatal cases
Hello
'High - risk' antenatal cases contribute to 70 - 80% of perinatal morbidity and mortality rates. The screening and diagnostic tests to evaluate and identify such cases is a must so as to provide special care to the mother - child duo. Risk approach for antenatal cases according to WHO includes : ( mnemonic - RISK APPROACH )
'High - risk' antenatal cases contribute to 70 - 80% of perinatal morbidity and mortality rates. The screening and diagnostic tests to evaluate and identify such cases is a must so as to provide special care to the mother - child duo. Risk approach for antenatal cases according to WHO includes : ( mnemonic - RISK APPROACH )
Tuesday, April 18, 2017
Prader-Willi syndrome and Angelman syndrome mnemonic
Hello! Let me start with the mnemonic and then I'll explain these syndromes in detail.
Type 1 RTA pathophysiology, notes and mnemonic
Hello! This post is on type 1 renal tubular acidosis.
What causes Type 1 RTA?
Defective H+ ion secretion in the distal tubule.
Impairment in H+ ions secretion result in an inability to acidify the pH beyond 5.5 (Used in the diagnosis of type 1 RTA)
The plasma bicarbonate is significantly reduced and may fall below 10 meq/L.
These patients tend to have urinary K+ wasting and hypokalemia (thought to be due to increased potassium secretion by distal tubular cells in the setting of diminished H+ ion secretion.)
What type of RTA is associated with an enhanced chance if nephrolithiasis?
Distal or type 1 RTA can cause nephrocalcinosis / calcium oxalate kidney stones.
Mnemonic: ONE predisposes to stONEs
Pathophysiology: Hypercalciuria, hyperphosphatemia, nephrolithiasis (calcium phosphate stones) and nephrocalcinosis are frequently associated with untreated type 1 RTA. The hypercalciuria is thought to be due to:
1) increased calcium phosphate release from bone as a result of bone buffering of excess acid and
2) reduction in tubular calcium reabsorption secondary to chronic acidosis.
The hypercalciuria, alkaline urine, and reduced excretion of citrate in the urine (which normally prevents calcium crystallization) promote the precipitation of calcium phosphate and stone formation.
Which conditions are associated with type 1 RTA?
diStal RTA is associated with the 3 S's:
Sjogren's
SLE
Sickle cell anemia
Treatment: Bicarbonate administration
That's all!
-IkaN
Defective H+ ion secretion in the distal tubule.
Impairment in H+ ions secretion result in an inability to acidify the pH beyond 5.5 (Used in the diagnosis of type 1 RTA)
The plasma bicarbonate is significantly reduced and may fall below 10 meq/L.
These patients tend to have urinary K+ wasting and hypokalemia (thought to be due to increased potassium secretion by distal tubular cells in the setting of diminished H+ ion secretion.)
What type of RTA is associated with an enhanced chance if nephrolithiasis?
Distal or type 1 RTA can cause nephrocalcinosis / calcium oxalate kidney stones.
Mnemonic: ONE predisposes to stONEs
Pathophysiology: Hypercalciuria, hyperphosphatemia, nephrolithiasis (calcium phosphate stones) and nephrocalcinosis are frequently associated with untreated type 1 RTA. The hypercalciuria is thought to be due to:
1) increased calcium phosphate release from bone as a result of bone buffering of excess acid and
2) reduction in tubular calcium reabsorption secondary to chronic acidosis.
The hypercalciuria, alkaline urine, and reduced excretion of citrate in the urine (which normally prevents calcium crystallization) promote the precipitation of calcium phosphate and stone formation.
Which conditions are associated with type 1 RTA?
diStal RTA is associated with the 3 S's:
Sjogren's
SLE
Sickle cell anemia
Treatment: Bicarbonate administration
That's all!
-IkaN
Monday, April 17, 2017
Mnemonico diagnostico : Vitamin D deficient Rickets
Hey Awesomites
The clinical features specific for Rickets due to vitamin D deficiency are : Vit D BHP RICKETS
V - Visceroptosis ( due to ligament laxity )
D - DEXA scan / low bone Density
B - Bossing of skull
H - Harrison's groove
P - Ping pong ball sensation
R - Rachitic rosary
I - Iron deficiency and other anemias
C - Coxa vara
K - Kyphosis
E - Eruption of teeth ( delayed )
T - Thoracolumbar ( Lordosis )
S - Sternum and ribs protrusion ( Pigeon chest )
Thats all
- Jaskunwar Singh
The clinical features specific for Rickets due to vitamin D deficiency are : Vit D BHP RICKETS
V - Visceroptosis ( due to ligament laxity )
D - DEXA scan / low bone Density
B - Bossing of skull
H - Harrison's groove
P - Ping pong ball sensation
R - Rachitic rosary
I - Iron deficiency and other anemias
C - Coxa vara
K - Kyphosis
E - Eruption of teeth ( delayed )
T - Thoracolumbar ( Lordosis )
S - Sternum and ribs protrusion ( Pigeon chest )
Thats all
- Jaskunwar Singh
Sunday, April 16, 2017
Difference between Duodenal and Gastric Ulcer
Hello everyone, let’s talk about the ever confusing difference between Duodenal and Gastric Ulcer. Both the ulcers are a type of Peptic Ulcer which occurs due the action of acid resulting in the damage of alimentary mucosa. The main cause for both of them could be infection with H. pylori or intake of NSAIDs.
Mnemonico diagnostico : Klinefelter's syndrome
Hey Awesomites
Criteria for diagnosis of Klinefelter's syndrome in males mnemonic : KLINEFELTER
K - (K) Cryptorchidism
L - Leydig cells hypertrophy
I - Increased gonadotrophins
N - Negative/ Positive chromatism (aberrations)
E - Elongated legs
F - Failure of secondary sexual characters
E - Eunuchoidism
L - Late pubic hair
T - Testicular failure
E - Erectile dysfunction / Elbow deformities
R - Retardation (mental)
Thats all
- Jaskunwar Singh
Criteria for diagnosis of Klinefelter's syndrome in males mnemonic : KLINEFELTER
K - (K) Cryptorchidism
L - Leydig cells hypertrophy
I - Increased gonadotrophins
N - Negative/ Positive chromatism (aberrations)
E - Elongated legs
F - Failure of secondary sexual characters
E - Eunuchoidism
L - Late pubic hair
T - Testicular failure
E - Erectile dysfunction / Elbow deformities
R - Retardation (mental)
Thats all
- Jaskunwar Singh
Non Contraceptive uses of the Condom
Hi everyone. So we know what we use a condom for generally :p
But there are a few non Contraceptive uses for this magical device that prevents babies :').
So here goes -
1. Prevention of STD's.
2. Can be used in Balloon Tamponade to control PPH.
3. Used to cover the USG probe inserted into the female tract.
4. Can be used as a mould for the vagina during Vulvoplasty.
5. Women with Anti Sperm antibodies during the initial phase. (Controversial).
So that's about it.
We know no 5 more reasons to use condoms !
Go get em ; )
Happy studying.
Stay awesome.
~ A.P.Burkholderia
How to remember Hepatitis B is associated with membranous glomerulonephritis
Writing this post because I confused it with focal segmental glomerulonephritis yesterday.
Hepatitis B is associated with membranous glomerulonephritis.
Mnemonic: Happy memory - Heppy membory - Hepatitis B Membranous nephropathy :D
That's all!
-IkaN
Bromocriptine : Utility Review
Hi everyone ! Here's a brief review on the drug Bromocriptine which happens to be one of my favorite drugs. So here goes.
- Bromocriptine is a Dopaminergic agonist , specifically acting on the D2 Receptors.
- It is a very widely used drug , with various and multi systemic uses.
Uses :
1. Parkinson's disease.
- Bromocriptine and other D2 agonists like Rotigotine , Ropinirole and Pramipexole can be used to treat Parkinsonism.
- They act by providing a sort of replacement for the depleted dopamine in the circuits of the basal ganglia.
- They are quite effective , especially in case of L Dopa resistance , or deterioration of symptoms when on L dopa.
2. Neuroleptic Malignant Syndrome.
- NMS is perhaps caused by D2 blockade due to drugs like Haloperidol and Fluphenazine.
- Thus it makes sense if you give this D2 agonist to treat this disorder.
3. Hyperprolactinemia.
- Dopamine acts as a Prolactin Inhibitory Factor (PIF) at the Hypthalamo-Pituitary level.
- In cases of Hyperprolactinemia where there is gynecomastia and galactorrhea, giving D2 agonists counteracts the elevated prolactin levels.
- Thus it's useful in Anti psychotic/ Metoclopramide induced Hyperprolactinemia.
- Can be used in Ovulation induction due to elevated prolactin by a Pituitary adenoma.
4. Diabetes Mellitus.
- Bromocriptine modulates the Dopaminergic discharge at the Hypothalamus level.
- This modulates the circadian rhythm and resets the abnormal metabolic drive of the Hypothalamus and reduces the insulin resistance.
- The specific Quick Release formulation is used for this indication.
- It may be used in conjunction with Insulin and does not cause hypoglycemia.
- It cannot however be used for DKA
5. Acromegaly.
- Inhibits the excess Growth Hormone secretion by acting at the Hypothalamus level.
Hope this helped !
Happy studying and stay awesome!
~ A.P.Burkholderia
Neuroleptic Malignant Syndrome : A Crisp Overview
Hi everyone ! So I recently saw a patient who possibly had Neuroleptic malignant syndrome. So I though I would do a post on it !
1. The Syndrome -
NMS is an idiosyncratic reaction to Anti psychotic drugs. It causes a host of symptoms like Rigidity , Hyperpyrexia and altered consciousness.
2. The Etiology -
- All Antipsychotic drugs can cause NMS. But most commonly implicated are Haloperidol, Fluphenazine and Chlorpromazine.
- Especially at risk are those taking Depot preparations.
- Even lithium in high doses can precipitate this.
- Atypical Antipsychotic drugs have a lower propensity to cause this.
3. The Pathophysiology -
- Although largely speculative , the cause is said to be the dopaminergic blockade by the anti psychotic drugs.
- Blockade of D2 in Hypothalamus is responsible for the Behavioral and Temperature changes.
- Blockade of D2 in the basal ganglia ( nigro striatal pathway) causes the Rigidity.
- increased muscular activity can cause muscle break down.
4. The Clinical Features -
- generally within 4-10 days after starting the Antipsychotic drug. But can even occur years later.
- Hyperthermia ( Hypothalamus is conked off )
- Lead pipe Rigidity ( Basal ganglia are screwed)
- Altered mental state - delirious.
- Sweating/ Diaphoresis ( compensation for high temp)
- Tachycardia
- Dyspnea
- Urinary incontinence
- Dysphagia
- Pallor.
Symptoms develop over a period of 24-72 hours.
5. Tests -
- Creatine Phosphokinase (CPK MM) is raised
- Leukocytosis
- Low Iron
- Deranged LFT and LDH
( Can be used to differentiate from serotonin syndrome)
- Diagnosis requires Hyperthermia + Rigidity + 2 other features ( including riased leukocytes and CK MM)
6. Management -
- ABCD
- Ventilatory support if needed
- stop Antipsychotic drugs.
- Anti pyrectics . Ice packs. Cooling blankets.
- BDZ
- Specific -->
Dantrolene - Muscle relaxant and Hyperthermia management. 400 mg/D.
- Bromocriptine - D2 agonist.
- ECT may be needed.
Hope this was helpful ! Happy studying and Stay awesome.
~ A.P.Burkholderia
Reversible Causes of Dementia : Mnemonic
Hi everyone ! This is a short post on causes of dementia that can be corrected. This is very important as most causes other than these have no available treatment ! (One Reversible cause of dementia is the Demeantor's kiss ;;) Treat using Expectro Patronum)
So the medically treatable causes include the following.
Remember : ABCD2E
- Alcoholism
- Vitamin B deficiency - Thiamine / Niacin /B12
- CNS infections - HIV , Chronic Meningoencephalitis , Whipple Disease, Neurosyphilis.
- Depression
- Drug induced
- Endocrine - Thyroid disturbances
Let's look at how these can be corrected medically.
- A = Alcohol abuse. May be a result of Alcoholic delirium/ Wernicke-Korsakoff syndrome. So the management would include giving Thiamine to the patient , and alcohol withdrawal using Disulfiram ans other anti craving drugs like Ondansetron, Acamprosate, Topiramate and Naltrexone.
- Vitamin B Deficiency = Thiamine deficiency we've seen above.
Niacin Deficiency causes 3 D's - Diarrhea , Dermatitis and Dementia. So treat that using Niacin.
B12 Deficiency and possibly folic acid can also cause Dementia.
- CNS Infections = They cause transient cognitive changes that are reversible on treating the disease.
- Depression = may cause depressive pseudodementia or even true dementia. (pseudo dementia = no confabulation or impaired recent memory)
- Drug induced = Chronic use of drugs like BDZ , Opiates and TCA's.
- Endocrine = Hypothyroidism is notorious to cause Dementia.
~~~~~~~~~~~~~~~~~~~~~~~
The surgically correctable causes are below.
Remember = T2 H2
- Tumors (esp frontal lobe tumors )
- Trauma (Subdural Hematoma)
- Normal Pressure Hydrocephalus (NPH)
- Hydrocephalus
- Tumors are resected surgically.
- For the hydrocephalus group , ventriculo peritoneal shunting is performed.
- NPH = Triad of symptoms showing Gait disturbances , Urinary incontinence and Dementia. (GUD)
Hope this post helped you and didn't leave you too demented. ! If it did, have some chocolate like Lupin would offer ;;)
Happy studying.
Stay awesome.
~ A.P.Burkholderia
Saturday, April 15, 2017
Fact of the day: Nightmares are a warning for serious mental problems
Hello
Not one or two, but frequent nightmares are major caveats for underlying serious mental problems. Rapid Eye Movement sleep disorder is a rare disorder that causes the person to act violently during dreamy state. This may be a warning sign for major neurologic disorders like Parkinson's and neurodegenerative diseases like Alzheimer's !!
Night owls are more likely to have frequent sleep and mood disturbances than the early sleepers. Evidences suggest people suffering from nightmares and related sleep disorders are more likely to have suicidal tendencies than those not, in addition to other contributing factors.
- Jaskunwar Singh
Not one or two, but frequent nightmares are major caveats for underlying serious mental problems. Rapid Eye Movement sleep disorder is a rare disorder that causes the person to act violently during dreamy state. This may be a warning sign for major neurologic disorders like Parkinson's and neurodegenerative diseases like Alzheimer's !!
Night owls are more likely to have frequent sleep and mood disturbances than the early sleepers. Evidences suggest people suffering from nightmares and related sleep disorders are more likely to have suicidal tendencies than those not, in addition to other contributing factors.
- Jaskunwar Singh
Friday, April 14, 2017
Drugs causing hyperkalemia mnemonic
Hello!
I modified the K BANK mnemonic and added more to it to cover a few more drugs.
The mnemonic for drugs causing hyperkalemia is: K BANK Digs, cycles, sucks, self help (Sulf hep!)
K - Potassium sparing diuretics (Obviously!)
B - Non selective beta blockers
A - ACEI, ARBs
N - NSAIDs
K - Potassium supplements
Digs - Digoxin
Cycles - Cyclosporine
Sucks - Succinylcholine
Sulf - Sulfonamides, Trimethoprim
Hep - Heparin
That's all!
-IkaN
Direct acting cholinomimetic agonist mnemonic
Hi everyone,
Here's the mnemonic for direct acting cholinomimetic drugs: ABC VPN
Nerve fibres : A clinico-physiological approach.
Hello everyone. So I've not been active at all lately , cause Final Year ! Pretty depressing 🙄. Anyway. Here's a post about the nerves and what we need to know for clinical application!
Nerves
So Erlanger and Gasser classified the nerves into A, B and C based on Myelination and size.
So you have :
A
(Which has Alpha , Beta , Gamma , Delta fibres )
B
C
Out of these , the first 3 :
A - Alpha , Beta , Gamma = Large fibres which are largely Myelinated.
And next 3 :
A - Delta , B , C = Small fibres which are not Myelinated as much.
How I remember these fibres is as per evolutionary significance.
The least Myelinated fibres , which are the smallest are the ones all living creatures need. As we progress from C to B to A , we continue to gather more and more well developed and specialised fibres.
C -
The smallest fibres.
Least Myelinated.
Most basic fibres and most primitive from an evolutionary stand point !
Control sensations of Dull Pain and Temperature (Heat)
B -
Small fibres.
Low Myelination.
Next most Basic Instinct - Urination.
Controls your Autonomic nervous system.
Remember- B = Bladder
A Delta -
Moderately Small fibres.
Lower Myelination than other A fibres.
Responsible for sensation of Sharp pain and Temperature ( Cold )
Thus to summarize the small fibres -
We have C , B and A Delta.
Out of these
C and A Delta control Pain and Temperature
( where C controls Dull pain and Heat ; A Delta controls Sharp pain and Cold )
And B controls Bladder /ANS.
(How to remember A Delta vs C.
C is more primitive. Hence controls Dull pain. Sharp pain is a little more specialized and hence is controlled by the relatively more modern fibre - the A Delta)
Coming to the large fibres.
We progress from A gamma to A beta to A alpha.
A Gamma :
Large but smaller then Alpha and beta.
Myelinated but not as much as alpha and beta.
Responsible for muscle tone.
Remember : A Gamma = Gamma motor neuron which is responsible for tone.
A Beta :
Very large.
Well Myelinated.
Responsible for modern sensations like Fine touch, Pressure and Vibration.
A Alpha :
Largest.
Most Myelinated.
Responsible for Muscle Contraction and Most modern sense - Proprioception.
It's the Bomb of the fibres hence responsible for muscle contraction.
Thus , demyelinating diseases like Guillian Barre syndrome and CIDP would affect the fibres that are used to being Myelinated.
So your presentation in these diseases would generally involve loss of:
A Alpha - Motor + Proprioception
A Beta - Modern sensations of fine touch and vibration.
A Gamma - Tone
And Axonal Polyneuropathic Diseases like Metabolic or Post infectious ones would involve loss and abnormalities of -
A Delta - Sharp Pain and Cold
B - ANS
C - Dull pain and Heat.
Hope this was helpful !
Happy studying !
Stay awesome.
~ A.P. Burkholderia
Case control study vs Cohort study mnemonic
Super short post :)
Case control study - Start with an outcome and go back in time to study the risk factor.
Simplified: Case (Diseased) vs Control (No disease)
Cohort study - Start with risk factor and see who developed the disease and who did not.
Mnemonic: cOhOrt has two O's.
One O has an R (cohORt), which means one group has the risk factor.
Other O does not have an R (cOhort), which means the other group does not have the risk factor.
Compare the two to see who gets the disease.
How to remember that case control studies measure odds ratio and cohort studies measure relative risk:
You take surgical "cases" to the "OR" (Operating room)
Case control study - Odds Ratio
cohoRRRRRRt measures Relative Risk.
kthxbye!
-IkaN
Case control study - Start with an outcome and go back in time to study the risk factor.
Simplified: Case (Diseased) vs Control (No disease)
Cohort study - Start with risk factor and see who developed the disease and who did not.
Mnemonic: cOhOrt has two O's.
One O has an R (cohORt), which means one group has the risk factor.
Other O does not have an R (cOhort), which means the other group does not have the risk factor.
Compare the two to see who gets the disease.
How to remember that case control studies measure odds ratio and cohort studies measure relative risk:
You take surgical "cases" to the "OR" (Operating room)
Case control study - Odds Ratio
cohoRRRRRRt measures Relative Risk.
kthxbye!
-IkaN
Abdominal Pain in Pregnancy
Hey guys
In this post I will mention the most common and must-know causes of abdominal pain in pregnancy which is a very common complaint during gestation. I will also mention certain salient points which will be helpful in the differential diagnosis.
1. Implantation Bleeding. There is a mild abdominal pain 6-12 days after conception along with a small amount of vaginal bleeding called spotting. Be careful so as not to confuse this bleeding with the menstrual bleeding.
2. Ectopic Pregnancy. This is the leading cause of first trimester mortality of the foetus. If there is a serum HCG level more than 2400 mIU/ml (The discriminatory zone is 1500-2400mIU/ml) and on USG there is no gestational sac in the uterus, then you should strongly suspect this. The most common sites are Tubal, Ovarian, Interstitial, Cervical.
3. Spontaneous Abortion. It is common in the early pregnanacy( upto 20 weeks) and is divided into 4 stages: Threatened, Inevitable, Incomplete, Complete. If there is vaginal bleeding without cervical dilatation or any change in cervical consistency, then it is Threatened abortion, if the cervix is dilated, it is Inevitable; if some products of conception are discharged per vaginally, it is incomplete abortion.
4. Abruptio Placentae. It is due to premature separation of placenta from its implantation site causing vaginal bleeding and pain due to uterine cramps caused by myometrial irritation. In some cases there is no vaginal bleeding, and we call those Concealed abruption. If the abruption is large enough to cause uteroplacental insufficiency the fetus is at risk. And the mother is at risk of haemorrhagic shock.
5. Ovarian Cyst
6. Ovarian Torsion
7. Appendicitis
8. Uterine leiomyomas (Fibroids)
9. HELLP Syndrome. Haemolysis, Elevated liver enzymes, Low platelets syndrome is a complication of Preeclampsia characterized by nausea, vomiting and right upper quadrant pain and tenderness. If this condition has progressed, there is risk of seizures and in the worst case hepatic rupture causing hypovolemic shock and severe pain. Peripheral blood smear will show schistocytes and low platelets.
10. Cholelithiasis. This condition will have characteristic biliary colic, i.e., intermittent right upper quadrant pain associated with nausea and vomiting.
11. Cholecystitis.
12. UTI. There will be suprapubic pain with dysuria, frequency and urgency.
13. Urolithiasis.
14. Round Ligament Pain. Enlargement of uterus during pregnancy leads to traction in the round ligament which pulls on the nearby nerve fibres causing sharp pain; such a pain can also be caused by round ligament spasm or cramps. This pain is usually present on the right side because of the dextro-deviation of the uterus and managed by acetaminophen and exercise.
That's all!
-VM
Ischial Spines - Important Obstetric Landmark.
Hello There!
So let's enlist few important points in relation to the ischial spines.
Ischial spines can be generally be palpated at about a finger-length into the vagina, at 4 & 8o'clock.
They are felt as bony prominences and their palpation may cause a little discomfort to the patient.
These spines serve as a landmark for:
1) Engagement of Fetal Head.(Most commonly used for determining the Fetal Station during labor.
Ischial spines are considered as Station0)
2) Internal Rotation of the fetal head.
3) Pudendal Nerve Block.
4) External os.
5) Obstetric Curve (J shaped) takes forward curve at this level.
6) Insertion of levator Ani.
7) Plane of least pelvic dimension.
8) Ring pessary is kept at the level of ischial spines.
These are the few things I know about at the level of the Ischial spines.
Do let me know some additional points you know of, to add to the list.
Let's learn Together!
-Medha.
Thursday, April 13, 2017
Umbilical Cord Knots.
Hello everybody!
Recently during my Ob-Gyn internship while delivering the placenta, the Umbilical cord that I held, was very lumpy bumpy. Little knowing about the reason at that moment, I came home found out the reason.
Let's see how the Umbilical cord can get knotty sometimes.
So there are two types of knots seen in the cord.
1)True Umbilical Knots
2)False Umbilical Knots.
True Knots :
These are noted after delivery.
The umbilical vessels, are protected by the thick myxomatous Wharton jelly, and can rarely be occluded completely. The jelly protects the vessels and the fetal blood supply, as there is only flattening or dissipation of Wharton jelly when a Knot is formed.
Due to the knot some amount of venous congestion distal to it and some partially or completely occlusive vascular thrombi may also be observed.
A true knot is formed when a loop of cord slips over the infant’s head or shoulders during delivery.
If the knot is pulled tightly it can cause fetal demise due to restriction of the circulation in the cord.
The True Knots can occur due to:
1)A long cord,
2)Large amounts of amniotic fluid
3)A small infant,
4)An overactive fetus
5)As a result of external version.
(All the above causes lead to increased fetal movements in utero)
However the fetal mortality rate associated with true knots is low.
False Knots:
In the cord the blood vessels are longer than the cord and are often folded on themselves producing nodulations on the surface of the cord. These nodulations are lumps and bumps I saw!
These have been termed as false knots.
So guys the next time you see a lumpy bumpy cord, unlike me, you now know the reason.
That's all, on the Umbilical cord and it's knots.
Let's learn Together!
-Medha.
Laryngomalacia vs tracheomalacia mnemonic
Laryngomalacia casuses inspiratory stridor.
Tracheomalacia causes expiratory stridor.
Tracheomalacia causes expiratory stridor.
Terson Syndrome.
Hello everybody!
In this post let's quickly learn about Terson Syndrome.
So what is it?
This Syndrome is a combination of intraocular and subarachnoid haemorrhage secondary to aneurysmal rupture, most commonly arising from the anterior communicating artery.
Terson Syndrome along with other bleeding disorders is included amongst the Systemic causes of vitreous hemorrhage!
Intraocular haemorrhage is also seen to occur with:
1)Subdural haematoma
2)Acute elevation of intracranial pressure
The mechanism of intraocular bleeding:
There is increase in cavernous sinus pressure due to the subarachnoid/subdural hemorrhage leading to stasis in the retinal veins. This stasis in the retinal veins leads to increased intraluminal pressure in the veins making them susceptible to bleed.
The haemorrhage is often Bilateral.
Typically intraretinal and/or preretinal. With this hemorrhage there is a possibility of it leaking in the vitreous.
The vitreous haemorrhage usually resolves in a few months and the long-term, the visual prognosis is good.
I hope you guys found it useful. Do let me know about some neuro-opthalmology syndromes you know about.
Let's learn Together!
-Medha.
Innate Cellular Anti-retroviral Mechanisms
This post will focus on the mechanism by which a cell fights against HIV, mainly by interfering with its life cycle. There are only 3 such mechanisms discovered and elucidated till date.
As it says on the post, these are innate mechanisms most of which are upregulated by Interferons (alpha and gamma).The adaptive immune system is mostly ineffective against retroviruses. How? Earlier the most accepted hypothesis was that this is because of error-prone Reverse trancriptase which makes a lot of errors while forming the proviral ds DNA, hence causing hypermutations(mainly G to A) resuting in change in the viral antigenic domains. This is true for both HIV and HBV.
1. APOBEC3G: The full form is Apolipoprotein B mRNA editing enzyme and catalytic polypeptide like 3g which you will easily forget and you should. It is basically a cytidine deaminase which acts on the negative cDNA strand and converts dC into dU; hence converting G into A in the positive strand. These hypermutations ultimately lead to failure of viral replication by unknown processes. So the latest most accepted hypothesis explaining the G to A hypermutations in virion DNA is this. This is more effective against HBV than HIV, guess why? Its because HIV-1 has Vif (Viral Infectivity Factor) that inactivates APOBEC3G.
2. TRIM5: This is the reason why Rhesus monkeys are innately resistant to HIV. Its an awesome protein in my opinion. What it does is as soon as the viral nucleocapsid enters the cell, it forms a cage around it and cause it to "uncoat" prematurely hence inactivating the reverse transcriptase and other enzymes present within the capsid. Then it performs a Kamikaze!
It ubiquitinates itself (auto-ubiquitination); hence causing its own proteasomal degradation and destroying the viral proteins in the process as collateral damage.
3. Tetherin: Now this is a case of Stockholm Syndrome! Tetherin are proteins that tethers or chains the virion to the cell membrane, hence preventing its release from the cell. The cell is not letting the virus leave her. So that when the cell dies either by apoptosis or inflammatory processes, the virions die with it. <3
Unfortunately however cool these may appear, these are mostly ineffective and hence the standard microbiology textbooks choose to ignore these proteins. Hopefully in future, drugs will be designed to make them more effective. :)
That's all!
-VM
Cerebellum and Motor learning!
Hello everybody!
Let's today learn about cerebellum and how amazing it is.
So all of us know that walking, swimming or typing needs conscious effort while being learnt for the first time, but after learning, one can continue these activities mechanically without having to think about them.
After learning, the responsibility for these activities seems to shift more and more to the cerebellum leaving the cerebral cortex free for other tasks.
That is why a child who is learning to walk has to put all his mind into it. Any distraction may make him fall. But as adults we can multitask along with walking.
Let's see how this happens.
There is evidence that cerebellar circuits can undergo functional changes as a result of experience.
The climbing fibres play an important role in this process. (bring information only from the inferior olivary nuclei, and establish excitatory synapses with Purkinje cells)
In a new situation, the climbing fibre activity is high, and it tends to reduce mossy fibre activity.
(Mossy fiber excitation not only stimulates Specific Purkinge cells but also inhibits the neighbouring Purkinge Cells.)
On repeated exposure to stimulus while learning, the mossy fibre response gets stabilized at the low level without an increase in the climbing fibre activity and the Cerebellar efferents perform the function semiautonomously on stabilized afferent input.
Thus Cerebellar learning may spare the cerebral cortex in the learnt movements.
I hope this was informative.
Let's learn together!
-Medha.
Drug: Evolocumab
This post will be on Evolocumab, a monoclonal antibody drug recently approved by FDA for use in refractory cases of Primary Hyperlipidemia and Homozygous(Not used in heterozygous) Familial Hypercholesterolemia alongwith Statins and appropriate diet and lifestyle modifications.
Mechanism of Action:
As you know, LDL-Cholesterol is the bad cholesterol which is cleared by hepatocytes via surface LDL-receptors. These receptors are catabolized in hepatocytes by the enzyme proprotein convertase subtilisin/kexin subtype 9, fondly called PCSK9.
This enzyme is inhibited by Evolocumab, hence decreasing the intracellular clearance of LDL-R, thereby increasing the clearance of LDL-C from the body.
And Statins also help in raising the expression of LDL-R in hepatocytes by inhibiting HMG-CoA Reductase, hence decreasing cholesterol synthesis forcing the hepatocyte to extract more cholesterol from the blood.
The most common adverse effect is Nasopharyngitis which is easily manageable. And the black box warning is Hypersensitivity Reaction.
Look out for new drugs and ever-changing treatment and management guidelines and try to stay updated! :)
-VM
As you know, LDL-Cholesterol is the bad cholesterol which is cleared by hepatocytes via surface LDL-receptors. These receptors are catabolized in hepatocytes by the enzyme proprotein convertase subtilisin/kexin subtype 9, fondly called PCSK9.
This enzyme is inhibited by Evolocumab, hence decreasing the intracellular clearance of LDL-R, thereby increasing the clearance of LDL-C from the body.
And Statins also help in raising the expression of LDL-R in hepatocytes by inhibiting HMG-CoA Reductase, hence decreasing cholesterol synthesis forcing the hepatocyte to extract more cholesterol from the blood.
The most common adverse effect is Nasopharyngitis which is easily manageable. And the black box warning is Hypersensitivity Reaction.
Look out for new drugs and ever-changing treatment and management guidelines and try to stay updated! :)
-VM
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